Your search keyword '"Gabriel Miltenberger"' showing total 100 results

1. Genetic risk variants in New Yorkers of Puerto Rican and Dominican Republic heritage with Parkinson’s disease

Author

Gabriel Miltenberger-Miltenyi, Roberto A. Ortega, Aloysius Domingo, Rachita Yadav, Ayumi Nishiyama, Deborah Raymond, Viktoriya Katsnelson, Nikita Urval, Matthew Swan, Vicki Shanker, Joan Miravite, Ruth H. Walker, Susan B. Bressman, Laurie J. Ozelius, José C. Cabassa, and Rachel Saunders-Pullman

Subjects

Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract There is a paucity of genetic characterization in people with Parkinson’s disease (PD) of Latino and Afro-Caribbean descent. Screening LRRK2 and GBA variants in 32 New Yorkers of Puerto Rican ethnicity with PD and in 119 non-Hispanic-non-Jewish European PD cases revealed that Puerto Rican participants were more likely to harbor the LRRK2-p.G2019S variant (15.6% vs. 4.2%, respectively). Additionally, whole exome sequencing of twelve Puerto Rican and Dominican PD participants was performed as an exploratory study.

Published

2023

2. Left ventricular noncompaction associated with a pathogenic mutation in the MYH7 gene: Known mutation, different phenotype

Author

Margarida Oliveira, Olga Azevedo, Bebiana Faria, Pedro von Hafe, Geraldo Dias, Ricardo Faria, Victor Sanfins, Mário Lourenço, Gabriel Miltenberger-Miltenyi, and António Lourenço

Subjects

Não compactação ventricular esquerda, Cardiomiopatia, Gene MYH7, Heterogeneidade genética, Mutação sarcomérica, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Left ventricular noncompaction (LVNC) is a genetically heterogeneous cardiomyopathy, with familial and sporadic forms, but genetic testing only identifies a pathogenic mutation in a minority of cases. The main complications are heart failure, embolism and dysrhythmias. Herein we report a familial case of LVNC associated with a mutation in the MYH7 gene and review the literature regarding controversies in LVNC. A 50-year-old woman was referred to the cardiology clinic for palpitations. She underwent echocardiography and cardiac magnetic resonance imaging that revealed mild left ventricular systolic dysfunction and LVNC criteria. She had several episodes of non-sustained ventricular tachycardia and received an implantable cardioverter-defibrillator (ICD). Genetic testing revealed the c.1003G>C (p.Ala335Pro) mutation in the MYH7 gene. Familial screening showed clear genotype-phenotype cosegregation, which provided strong evidence for the pathogenic role of this mutation. To the best of our knowledge, this is the first report of LVNC associated with the p.Ala335Pro mutation in the MYH7 gene. This mutation has been described in hypertrophic cardiomyopathy, suggesting that the same pathogenic sarcomere mutation may be associated with different cardiomyopathies. This case also highlights the current difficulties regarding decisions on ICD implantation for primary prevention of sudden cardiac death in LVNC. Resumo: A não compactação do ventrículo esquerdo (LVNC) é uma cardiomiopatia geneticamente heterogénea, com formas familiares e esporádicas descritas. No entanto, o estudo genético permite identificar uma mutação patogénica numa minoria de casos. Neste trabalho, reportamos um caso familiar de não compactação do ventrículo esquerdo associada a uma mutação no gene MYH7 e apresentamos uma revisão das principais controvérsias na LVNC.Mulher de 50 anos, referenciada para a consulta de cardiologia por palpitações. O ecocardiograma transtorácico e a ressonância magnética cardíaca revelaram a presença de disfunção ventricular esquerda ligeira e de critérios de LVNC. Após documentação de episódios de taquicardia ventricular não sustentada foi implantado um cardiodesfibrilhador implantável (CDI). O teste genético revelou a presença da mutação c.1003G>C (p.Ala335Pro) no gene MYH7. O rastreio familiar mostrou uma clara segregação genótipo-fenótipo, o que suporta a patogenicidade desta mutação.Este é o primeiro caso de LVNC em associação com a mutação p.Ala335Pro no gene MYH7. Esta mutação já se encontrava previamente descrita em casos de cardiomiopatia hipertrófica, o que suporta que a mesma mutação sarcomérica pode expressar-se com diferentes fenótipos. Este caso destaca ainda as dificuldades atuais no que concerne à estratificação do risco arrítmico nos doentes com LVNC, mais concretamente para decisão de implantação de CDI em prevenção primária.

Published

2022

3. Early neurotransmitters changes in prodromal frontotemporal dementia: A GENFI study

Author

Enrico Premi, Marta Pengo, Irene Mattioli, Valentina Cantoni, Juergen Dukart, Roberto Gasparotti, Emanuele Buratti, Alessandro Padovani, Martina Bocchetta, Emily G. Todd, Arabella Bouzigues, David M. Cash, Rhian S. Convery, Lucy L. Russell, Phoebe Foster, David L. Thomas, John C. van Swieten, Lize C. Jiskoot, Harro Seelaar, Daniela Galimberti, Raquel Sanchez-Valle, Robert Laforce, Jr, Fermin Moreno, Matthis Synofzik, Caroline Graff, Mario Masellis, Maria Carmela Tartaglia, James B. Rowe, Kamen A. Tsvetanov, Rik Vandenberghe, Elizabeth Finger, Pietro Tiraboschi, Alexandre de Mendonça, Isabel Santana, Chris R. Butler, Simon Ducharme, Alexander Gerhard, Johannes Levin, Markus Otto, Sandro Sorbi, Isabelle Le Ber, Florence Pasquier, Jonathan D. Rohrer, Barbara Borroni, Aitana Sogorb Esteve, Carolin Heller, Caroline V. Greaves, Henrik Zetterberg, Imogen J. Swift, Kiran Samra, Rachelle Shafei, Carolyn Timberlake, Thomas Cope, Timothy Rittman, Andrea Arighi, Chiara Fenoglio, Elio Scarpini, Giorgio Fumagalli, Vittoria Borracci, Giacomina Rossi, Giorgio Giaccone, Giuseppe Di Fede, Paola Caroppo, Sara Prioni, Veronica Redaelli, David Tang-Wai, Ekaterina Rogaeva, Miguel Castelo-Branco, Morris Freedman, Ron Keren, Sandra Black, Sara Mitchell, Christen Shoesmith, Robart Bartha, Rosa Rademakers, Jackie Poos, Janne M. Papma, Lucia Giannini, Rick van Minkelen, Yolande Pijnenburg, Benedetta Nacmias, Camilla Ferrari, Cristina Polito, Gemma Lombardi, Valentina Bessi, Michele Veldsman, Christin Andersson, Hakan Thonberg, Linn Öijerstedt, Vesna Jelic, Paul Thompson, Tobias Langheinrich, Albert Lladó, Anna Antonell, Jaume Olives, Mircea Balasa, Nuria Bargalló, Sergi Borrego-Ecija, Ana Verdelho, Carolina Maruta, Catarina B. Ferreira, Gabriel Miltenberger, Frederico Simões do Couto, Alazne Gabilondo, Ana Gorostidi, Jorge Villanua, Marta Cañada, Mikel Tainta, Miren Zulaica, Myriam Barandiaran, Patricia Alves, Benjamin Bender, Carlo Wilke, Lisa Graf, Annick Vogels, Mathieu Vandenbulcke, Philip Van Damme, Rose Bruffaerts, Koen Poesen, Pedro Rosa-Neto, Serge Gauthier, Agnès Camuzat, Alexis Brice, Anne Bertrand, Aurélie Funkiewiez, Daisy Rinaldi, Dario Saracino, Olivier Colliot, Sabrina Sayah, Catharina Prix, Elisabeth Wlasich, Olivia Wagemann, Sandra Loosli, Sonja Schönecker, Tobias Hoegen, Jolina Lombardi, Sarah Anderl-Straub, Adeline Rollin, Gregory Kuchcinski, Maxime Bertoux, Thibaud Lebouvier, Vincent Deramecourt, Beatriz Santiago, Diana Duro, Maria João Leitão, Maria Rosario Almeida, Miguel Tábuas-Pereira, and Sónia Afonso

Subjects

Frontotemporal dementia, Frontotemporal lobar degeneration, Genes, Magnetic resonance imaging, Positron emission tomography, Neurotransmitters, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Background: Neurotransmitters deficits in Frontotemporal Dementia (FTD) are still poorly understood. Better knowledge of neurotransmitters impairment, especially in prodromal disease stages, might tailor symptomatic treatment approaches. Methods: In the present study, we applied JuSpace toolbox, which allowed for cross-modal correlation of Magnetic Resonance Imaging (MRI)-based measures with nuclear imaging derived estimates covering various neurotransmitter systems including dopaminergic, serotonergic, noradrenergic, GABAergic and glutamatergic neurotransmission.We included 392 mutation carriers (157 GRN, 164 C9orf72, 71 MAPT), together with 276 non-carrier cognitively healthy controls (HC). We tested if the spatial patterns of grey matter volume (GMV) alterations in mutation carriers (relative to HC) are correlated with specific neurotransmitter systems in prodromal (CDR® plus NACC FTLD = 0.5) and in symptomatic (CDR® plus NACC FTLD≥1) FTD. Results: In prodromal stages of C9orf72 disease, voxel-based brain changes were significantly associated with spatial distribution of dopamine and acetylcholine pathways; in prodromal MAPT disease with dopamine and serotonin pathways, while in prodromal GRN disease no significant findings were reported (p

Published

2023

4. Screening for Fabry disease in patients with left ventricular noncompaction

Author

Olga Azevedo, Nuno Marques, Nuno Craveiro, Ana Rita Pereira, Hugo Antunes, Liliana Reis, Rui Azevedo Guerreiro, Rui Pontes dos Santos, Gabriel Miltenberger-Miltenyi, Nuno Sousa, and Damião Cunha

Subjects

Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Introduction and Aim: It is unclear whether left ventricular noncompaction (LVNC) is a distinct cardiomyopathy or a morphologic manifestation of different cardiomyopathies. We previously reported a case of LVNC in a Fabry disease (FD) patient, but it remains to be clarified whether LVNC is a cardiac manifestation of FD, a coincidental finding or an overdiagnosis, which has major therapeutic implications. This study aims to determine the prevalence of FD among patients with LVNC. Methods: We performed a retrospective study including all patients diagnosed with LVNC in eight hospital centers. Diagnosis of LVNC was based on at least one echocardiographic or cardiac magnetic resonance criterion. FD screening was performed by combined enzyme and genetic testing. Results: The study included 78 patients diagnosed with LVNC based on the Jenni (84.6%), Stöllberger (46.2%), Chin (21.8%), Petersen (83.8%) and Jacquier (16.2%) criteria. Left ventricular systolic dysfunction was present in 48.7%. Heart failure was found in 60.3%, ventricular dysrhythmias in 21.6% and embolic events in 11.5%. FD screening found no additional cases among patients with LVNC, besides the previously described case. Conclusion: No additional FD cases were found among patients with LVNC, which argues against the hypothesis that LVNC is a cardiac manifestation of FD. Resumo: Introdução e objetivo: Não está esclarecido se a não compactação do ventrículo esquerdo (NCVE) é uma miocardiopatia distinta ou uma manifestação morfológica de várias miocardiopatias. Nós reportamos previamente um caso de NCVE num doente com doença de Fabry (DF), mas permanece por esclarecer se a NCVE é uma manifestação cardíaca de DF, um achado coincidente ou um sobrediagnóstico, o que tem importantes implicações terapêuticas. Este estudo pretende determinar a prevalência de DF em doentes com NCVE. Métodos: Estudo retrospetivo incluindo todos os doentes diagnosticados com NCVE em oito centros hospitalares. O diagnóstico de NCVE foi baseado em pelo menos um dos critérios de ecocardiografia ou ressonância cardíaca. O rastreio de DF foi realizado por teste enzimático e genético. Resultados: O estudo incluiu 78 doentes diagnosticados com NCVE com base nos critérios de Jenni (84,6%), Stöllberger (46,2%), Chin (21,8%), Petersen (83,8%) e Jacquier (16,2%). A disfunção sistólica do VE estava presente em 48,7%. A insuficiência cardíaca foi encontrada em 60,3%, as disritmias ventriculares em 21,6% e os eventos embólicos em 11,5%. O rastreio de DF não encontrou casos adicionais nos doentes com NCVE, para além do caso previamente descrito. Conclusão: Não foram encontrados casos adicionais de DF nos doentes com NCVE, o que argumenta contra a hipótese de a NCVE ser uma manifestação cardíaca de DF. Keywords: Fabry disease, Noncompaction, Hypertrabeculation, Cardiomyopathy, Screening, Palavras-chave: Doença de Fabry, Não compactação, Hipertrabeculação, Cardiomiopatia, Rastreio

Published

2019

5. Teste genético post mortem, o diagnóstico clínico não se esgota com a morte do doente

Author

Sílvia Ribeiro, Luís Coelho, Katerina Puentes, Gabriel Miltenberger‐Miltenyi, Bebiana Faria, Lucy Calvo, João Primo, Víctor Sanfins, and António Lourenço

Subjects

Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Resumo: Em até um terço dos casos de morte súbita, a autópsia médico‐legal é «branca», estando já contemplada nas recomendações internacionais a possibilidade da realização de autópsia molecular. A importância do teste genético post mortem prende‐se com a identificação de doenças hereditárias, frequentemente doenças com padrão de transmissão autossómico dominante, sendo possível, através de consulta e rastreio de parentes, identificar elementos na família com a doença, não raramente portadores assintomáticos de uma mutação, havendo espaço para alterar o curso de vida dos mesmos. Os autores apresentam três casos clínicos que reforçam o quão importante é o estudo genético post mortem, assim como o estudo familiar e a integração dos dados numa consulta de cardiologia, seja arritmologia, consulta de doença coronária ou miocardiopatias, dependendo da patologia específica, podendo modificar o curso da doença em muitos parentes. Abstract: In up to one‐third of cases of sudden death, the medico‐legal autopsy finding is inconclusive, and the option to perform a molecular autopsy is covered in international guidelines. The importance of postmortem genetic testing lies in its ability to identify hereditary diseases, often those with an autosomal dominant transmission pattern, and, through consultations and screening of relatives, to identify family members with a pathogenic mutation, who are often asymptomatic, providing an opportunity to change the course of their lives. The authors present three clinical cases that highlight the importance of postmortem genetic studies and family studies, as well as the integration of the data obtained in a cardiology consultation, which may be for arrhythmology, coronary disease or cardiomyopathy, depending on the specific condition. This could modify the course of the disease in many relatives. Palavras‐chave: Autópsia, Teste genético post mortem, Canalopatias, Síndrome de Brugada, Keywords: Autopsy, Postmortem genetic testing, Channelopathies, Brugada syndrome

Published

2019

6. Pathologic expansion in the C9orf72 gene is associated with accelerated decline of respiratory function and decreased survival in amyotrophic lateral sclerosis

Author

Gabriel Miltenberger-Miltenyi, Vasco A. Conceição, Marta Gromicho, Ana Catarina Pronto-Laborinho, Susana Pinto, and Mamede de Carvalho

Subjects

Medicine

Abstract

AbstractIntroduction Respiratory insufficiency is the main cause of death in amyotrophic lateral sclerosis (ALS). As the C9orf72 repeat expansion represents the most common genetic risk factor for this disease, we studied whether C9orf72 modulates respiratory function and survival.Methods Demographic and clinical data, and C9orf72 status were collected from 372 ALS patients followed in our centre. Multiple regressions controlling for the C9orf72 expansion, diagnosis delay, region of onset, age, gender, and comorbid frontotemporal dementia were performed to evaluate the functional and respiratory status of the patients at baseline and during disease progression – assessed using the global ALSFRS-R score and its respiratory subscore, and the predicted forced vital capacity (%FVC). A Cox regression controlling for the same variables was carried out to analyse survival.Results At baseline, 32/372 (8.60%) patients carried the C9orf72 repeat expansion. We found that the C9orf72 mutation is an independent risk factor for a faster %FVC decline (p = .001) and shorter survival (p = .002).Conclusions In ALS patients with C9orf72 expansion, shorter survival probably derives from faster respiratory function decline. This finding may indicate a new pathogenic mechanism of C9orf72 in ALS.

Published

2021

7. Disease-related cortical thinning in presymptomatic granulin mutation carriers

Author

Sergi Borrego-Écija, Roser Sala-Llonch, John van Swieten, Barbara Borroni, Fermín Moreno, Mario Masellis, Carmela Tartaglia, Caroline Graff, Daniela Galimberti, Robert Laforce, Jr, James B Rowe, Elizabeth Finger, Rik Vandenberghe, Fabrizio Tagliavini, Alexandre de Mendonça, Isabel Santana, Matthis Synofzik, Simon Ducharme, Johannes Levin, Adrian Danek, Alex Gerhard, Markus Otto, Chris Butler, Giovanni Frisoni, Sandro Sorbi, Carolin Heller, Martina Bocchetta, David M Cash, Rhian S Convery, Katrina M Moore, Jonathan D Rohrer, Raquel Sanchez-Valle, Martin N. Rossor, Nick C. Fox, Ione O.C. Woollacott, Rachelle Shafei, Caroline Greaves, Mollie Neason, Rita Guerreiro, Jose Bras, David L. Thomas, Jennifer Nicholas, Simon Mead, Lieke Meeter, Jessica Panman, Janne Papma, Rick van Minkelen, Yolande Pijnenburg, Begoña Indakoetxea, Alazne Gabilondo, Mikel TaintaMD, Maria de Arriba, Ana Gorostidi, Miren Zulaica, Jorge Villanua, Zigor Diaz, Jaume Olives, Albert Lladó, Mircea Balasa, Anna Antonell, Nuria Bargallo, Enrico Premi, Maura Cosseddu, Stefano Gazzina, Alessandro Padovani, Roberto Gasparotti, Silvana Archetti, Sandra Black, Sara Mitchell, Ekaterina Rogaeva, Morris Freedman, Ron Keren, David Tang-Wai, Linn Öijerstedt, Christin Andersson, Vesna Jelic, Hakan Thonberg, Andrea Arighi, Chiara Fenoglio, Elio Scarpini MD, Giorgio Fumagalli, Thomas Cope, Carolyn Timberlake, Timothy Rittman, Christen Shoesmith, Robart Bartha, Rosa Rademakers, Carlo Wilke, Benjamin Bender, Rose Bruffaerts, Philip Vandamme, Mathieu Vandenbulcke, Carolina Maruta, Catarina B. Ferreira, Gabriel Miltenberger, Ana Verdelho, Sónia Afonso, Ricardo Taipa, Paola Caroppo, Giuseppe Di Fede, Giorgio Giaccone, Sara Prioni, Veronica Redaelli, Giacomina Rossi, Pietro Tiraboschi, Diana Duro, Maria Rosario Almeida, Miguel Castelo-Branco, Maria João Leitão, Miguel Tabuas-Pereira, Beatriz Santiago, Serge Gauthier, Pedro Rosa-Neto, Michele Veldsman, Toby Flanagan, Catharina Prix, Tobias Hoegen, Elisabeth Wlasich, Sandra Loosli, Sonja Schonecker, Elisa Semler, and Sarah Anderl-Straub

Subjects

Frontotemporal dementia, Cortical thickness, GRN, Presymptomatic, Genetic mutations, Computer applications to medicine. Medical informatics, R858-859.7, Neurology. Diseases of the nervous system, RC346-429

Abstract

Mutations in the granulin gene (GRN) cause familial frontotemporal dementia. Understanding the structural brain changes in presymptomatic GRN carriers would enforce the use of neuroimaging biomarkers for early diagnosis and monitoring. We studied 100 presymptomatic GRN mutation carriers and 94 noncarriers from the Genetic Frontotemporal dementia initiative (GENFI), with MRI structural images. We analyzed 3T MRI structural images using the FreeSurfer pipeline to calculate the whole brain cortical thickness (CTh) for each subject. We also perform a vertex-wise general linear model to assess differences between groups in the relationship between CTh and diverse covariables as gender, age, the estimated years to onset and education. We also explored differences according to TMEM106B genotype, a possible disease modifier. Whole brain CTh did not differ between carriers and noncarriers. Both groups showed age-related cortical thinning. The group-by-age interaction analysis showed that this age-related cortical thinning was significantly greater in GRN carriers in the left superior frontal cortex. TMEM106B did not significantly influence the age-related cortical thinning. Our results validate and expand previous findings suggesting an increased CTh loss associated with age and estimated proximity to symptoms onset in GRN carriers, even before the disease onset.

Published

2021

8. Differential early subcortical involvement in genetic FTD within the GENFI cohort

Author

Martina Bocchetta, Emily G. Todd, Georgia Peakman, David M. Cash, Rhian S. Convery, Lucy L. Russell, David L. Thomas, Juan Eugenio Iglesias, John C. van Swieten, Lize C. Jiskoot, Harro Seelaar, Barbara Borroni, Daniela Galimberti, Raquel Sanchez-Valle, Robert Laforce, Fermin Moreno, Matthis Synofzik, Caroline Graff, Mario Masellis, Maria Carmela Tartaglia, James B. Rowe, Rik Vandenberghe, Elizabeth Finger, Fabrizio Tagliavini, Alexandre de Mendonça, Isabel Santana, Chris R. Butler, Simon Ducharme, Alexander Gerhard, Adrian Danek, Johannes Levin, Markus Otto, Sandro Sorbi, Isabelle Le Ber, Florence Pasquier, Jonathan D. Rohrer, Sónia Afonso, Maria Rosario Almeida, Sarah Anderl-Straub, Christin Andersson, Anna Antonell, Silvana Archetti, Andrea Arighi, Mircea Balasa, Myriam Barandiaran, Nuria Bargalló, Robart Bartha, Benjamin Bender, Alberto Benussi, Maxime Bertoux, Anne Bertrand, Valentina Bessi, Sandra Black, Sergi Borrego-Ecija, Jose Bras, Alexis Brice, Rose Bruffaerts, Agnès Camuzat, Marta Cañada, Valentina Cantoni, Paola Caroppo, Miguel Castelo-Branco, Olivier Colliot, Thomas Cope, Vincent Deramecourt, María de Arriba, Giuseppe Di Fede, Alina Díez, Diana Duro, Chiara Fenoglio, Camilla Ferrari, Catarina B. Ferreira, Nick Fox, Morris Freedman, Giorgio Fumagalli, Aurélie Funkiewiez, Alazne Gabilondo, Roberto Gasparotti, Serge Gauthier, Stefano Gazzina, Giorgio Giaccone, Ana Gorostidi, Caroline Greaves, Rita Guerreiro, Carolin Heller, Tobias Hoegen, Begoña Indakoetxea, Vesna Jelic, Hans-Otto Karnath, Ron Keren, Gregory Kuchcinski, Tobias Langheinrich, Thibaud Lebouvier, Maria João Leitão, Albert Lladó, Gemma Lombardi, Sandra Loosli, Carolina Maruta, Simon Mead, Lieke Meeter, Gabriel Miltenberger, Rick van Minkelen, Sara Mitchell, Katrina Moore, Benedetta Nacmias, Annabel Nelson, Jennifer Nicholas, Linn Öijerstedt, Jaume Olives, Sebastien Ourselin, Alessandro Padovani, Jessica Panman, Janne M. Papma, Yolande Pijnenburg, Cristina Polito, Enrico Premi, Sara Prioni, Catharina Prix, Rosa Rademakers, Veronica Redaelli, Daisy Rinaldi, Tim Rittman, Ekaterina Rogaeva, Adeline Rollin, Pedro Rosa-Neto, Giacomina Rossi, Martin Rossor, Beatriz Santiago, Dario Saracino, Sabrina Sayah, Elio Scarpini, Sonja Schönecker, Elisa Semler, Rachelle Shafei, Christen Shoesmith, Imogen Swift, Miguel Tábuas-Pereira, Mikel Tainta, Ricardo Taipa, David Tang-Wai, Paul Thompson, Hakan Thonberg, Carolyn Timberlake, Pietro Tiraboschi, Philip Van Damme, Mathieu Vandenbulcke, Michele Veldsman, Ana Verdelho, Jorge Villanua, Jason Warren, Carlo Wilke, Ione Woollacott, Elisabeth Wlasich, Henrik Zetterberg, and Miren Zulaica

Subjects

Genetic frontotemporal dementia, MRI imaging, Brain volumetry, Presymptomatic stage, Computer applications to medicine. Medical informatics, R858-859.7, Neurology. Diseases of the nervous system, RC346-429

Abstract

Background: Studies have previously shown evidence for presymptomatic cortical atrophy in genetic FTD. Whilst initial investigations have also identified early deep grey matter volume loss, little is known about the extent of subcortical involvement, particularly within subregions, and how this differs between genetic groups. Methods: 480 mutation carriers from the Genetic FTD Initiative (GENFI) were included (198 GRN, 202 C9orf72, 80 MAPT), together with 298 non-carrier cognitively normal controls. Cortical and subcortical volumes of interest were generated using automated parcellation methods on volumetric 3 T T1-weighted MRI scans. Mutation carriers were divided into three disease stages based on their global CDR® plus NACC FTLD score: asymptomatic (0), possibly or mildly symptomatic (0.5) and fully symptomatic (1 or more). Results: In all three groups, subcortical involvement was seen at the CDR 0.5 stage prior to phenoconversion, whereas in the C9orf72 and MAPT mutation carriers there was also involvement at the CDR 0 stage. In the C9orf72 expansion carriers the earliest volume changes were in thalamic subnuclei (particularly pulvinar and lateral geniculate, 9–10%) cerebellum (lobules VIIa-Crus II and VIIIb, 2–3%), hippocampus (particularly presubiculum and CA1, 2–3%), amygdala (all subregions, 2–6%) and hypothalamus (superior tuberal region, 1%). In MAPT mutation carriers changes were seen at CDR 0 in the hippocampus (subiculum, presubiculum and tail, 3–4%) and amygdala (accessory basal and superficial nuclei, 2–4%). GRN mutation carriers showed subcortical differences at CDR 0.5 in the presubiculum of the hippocampus (8%). Conclusions: C9orf72 expansion carriers show the earliest and most widespread changes including the thalamus, basal ganglia and medial temporal lobe. By investigating individual subregions, changes can also be seen at CDR 0 in MAPT mutation carriers within the limbic system. Our results suggest that subcortical brain volumes may be used as markers of neurodegeneration even prior to the onset of prodromal symptoms.

Published

2021

9. Natural history of the late-onset phenotype of Fabry disease due to the p.F113L mutation

Author

Olga Azevedo, Miguel F. Gago, Gabriel Miltenberger-Miltenyi, Ana Raquel Robles, Maria Antónia Costa, Olga Pereira, Ana Teresa Vide, Gonçalo Castelo Branco, Sónia Simões, Maria José Guimarães, Ana Salgado, Nuno Sousa, and Damião Cunha

Subjects

Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Background: The common GLA gene mutation p.F113L causes late-onset phenotype of Fabry disease (FD) with predominant cardiac manifestations. A founder effect of FD due to this mutation was found in the Portuguese region of Guimarães. Our study aims to deepen the knowledge on the natural history of this late-onset variant. Methods: 203 consecutive adult Fabry patients with p.F113L mutation (79 males; mean age 46 ± 18 years), from this region, were submitted at baseline to a predefined diagnostic protocol. The occurrence of FD manifestations was analyzed in each decade of age in both genders. Results: In males, left ventricular hypertrophy (40.2%) and late gadolinium enhancement (21.4%) arose over 30 years; heart failure (HF) (21.9%), ventricular tachycardia (8.9%) and conduction disorders over 40 years; and bifascicular (13.1%) and complete atrioventricular blocks (5.9%) beyond 50 years of age. Cardiac manifestations occurred more commonly and 1–2 decades earlier in males; their frequency increased with age. Septum and posterior wall thickness, LV mass, QRS interval duration and pro-BNP levels increased with age in both genders. Mean survival free from HF (64 ± 1 vs. 76 ± 2 years) and pacemaker (71 ± 2 vs. 86 ± 1 years) was higher in females (p

Published

2020

10. Correction: Gene Expression Differences in Peripheral Blood of Parkinson's Disease Patients with Distinct Progression Profiles.

Author

Raquel Pinho, Leonor C Guedes, Lilach Soreq, Patrícia P Lobo, Tiago Mestre, Miguel Coelho, Mário M Rosa, Nilza Gonçalves, Pauline Wales, Tiago Mendes, Ellen Gerhardt, Christiane Fahlbusch, Vincenzo Bonifati, Michael Bonin, Gabriel Miltenberger-Miltényi, Fran Borovecki, Hermona Soreq, Joaquim J Ferreira, and Tiago F Outeiro

Subjects

Medicine, Science

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0157852.].

Published

2017

11. Sarcomeric hypertrophic cardiomyopathy: Genetic profile in a Portuguese population

Author

Dulce Brito, Gabriel Miltenberger-Miltenyi, Sónia Vale Pereira, Doroteia Silva, António Nunes Diogo, and Hugo Madeira

Subjects

Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Background: Sarcomeric hypertrophic cardiomyopathy has heterogeneous phenotypic expressions, of which sudden cardiac death is the most feared. A genetic diagnosis is essential to identify subjects at risk in each family. The spectrum of disease-causing mutations in the Portuguese population is unknown. Methods: Seventy-seven unrelated probands with hypertrophic cardiomyopathy were systematically screened for mutations by PCR and sequencing of five sarcomeric genes: MYBPC3, MYH7, TNNT2, TNNI3 and MYL2. Familial cosegregation analysis was performed in most patients. Results: Thirty-four different mutations were identified in 41 (53%) index patients, 71% with familial hypertrophic cardiomyopathy. The most frequently involved gene was MYBPC3 (66%) with 22 different mutations (8 novel) in 27 patients, followed by MYH7 (22%), TNNT2 (12%) and TNNI3 (2.6%). In three patients (7%), two mutations were found in MYBPC3 and/or MYH7. Additionally, 276 relatives were screened, leading to the identification of a mean of three other affected relatives for each pedigree with the familial form of the disease. Conclusions: Disease-associated mutations were identified mostly in familial hypertrophic cardiomyopathy, corroborating the idea that rarely studied genes may be implicated in sporadic forms. Private mutations are the rule, MYBPC3 being the most commonly involved gene. Mutations in MYBPC3 and MYH7 accounted for most cases of sarcomere-related disease. Multiple mutations in these genes may occur, which highlights the importance of screening both. The detection of novel mutations strongly suggests that all coding regions should be systematically screened. Genotyping in hypertrophic cardiomyopathy enables a more precise diagnosis of the disease, with implications for risk stratification and genetic counseling. Resumo: Introdução: A miocardiopatia hipertrófica sarcomérica (MH) tem expressão fenotípica heterogénea, sendo a morte súbita cardíaca a mais temida. O diagnóstico genético é fundamental para identificar os indivíduos em risco em cada família. O perfil genético da doença é desconhecido na população portuguesa. População e métodos: Estudaram-se geneticamente 77 doentes-índice com MH, não-relacionados, pesquisando-se, por PCR e sequenciação, mutações nos genes MYBPC3, MYH7, TNNT2, TNNI3 e MYL2. Efetuou-se análise de co-segregação familiar na maioria dos doentes. Resultados: Identificaram-se 34 mutações diferentes em 41 doentes-índice (53%), 71% com MH familiar. O gene mais frequentemente envolvido foi o MYBPC3 (66%), identificando-se 22 mutações diferentes (8 novas) em 27 doentes-índice. Seguiram-se os genes MYH7 (22%), TNNT2 (12%) e TNNI3 (2,6%). Em 3 doentes (7%) identificaram-se 2 mutações nos genes MYBPC3 e/ou MYH7. Estudaram-se também 276 familiares detetando-se, em média, mais 3 indivíduos em risco, em cada pedigree com MH familiar. Conclusões: Foram identificadas mutações associadas a MH maioritariamente na doença familiar, reforçando a ideia corrente de as formas esporádicas estarem associadas a genes raramente estudados. A maioria das mutações é privada de cada família. O gene MYBPC3 é o mais frequentemente afetado. As mutações neste gene e no gene MYH7 são responsáveis pela maioria das situações de MH. Podem existir mutações múltiplas nestes genes, sendo mandatório o seu rastreio. A identificação de mutações novas aconselha a rastrear sistematicamente todas as regiões codificadoras. O estudo genético na MH permite um diagnóstico mais preciso da doença, determinante para a estratificação do risco e para o aconselhamento genético. Keywords: Sarcomeric hypertrophic cardiomyopathy, Mutations, Sarcomeric genes, Prevalence, Risk stratification, Palavras-chave: Miocardiopatia hipertrófica sarcomérica, Mutações, Genes sarcoméricos, Prevalência, Estratificação do risco

Published

2012

12. Gene Expression Differences in Peripheral Blood of Parkinson's Disease Patients with Distinct Progression Profiles.

Author

Raquel Pinho, Leonor C Guedes, Lilach Soreq, Patrícia P Lobo, Tiago Mestre, Miguel Coelho, Mário M Rosa, Nilza Gonçalves, Pauline Wales, Tiago Mendes, Ellen Gerhardt, Christiane Fahlbusch, Vincenzo Bonifati, Michael Bonin, Gabriel Miltenberger-Miltényi, Fran Borovecki, Hermona Soreq, Joaquim J Ferreira, and Tiago F Outeiro

Subjects

Medicine, Science

Abstract

The prognosis of neurodegenerative disorders is clinically challenging due to the inexistence of established biomarkers for predicting disease progression. Here, we performed an exploratory cross-sectional, case-control study aimed at determining whether gene expression differences in peripheral blood may be used as a signature of Parkinson's disease (PD) progression, thereby shedding light into potential molecular mechanisms underlying disease development. We compared transcriptional profiles in the blood from 34 PD patients who developed postural instability within ten years with those of 33 patients who did not develop postural instability within this time frame. Our study identified >200 differentially expressed genes between the two groups. The expression of several of the genes identified was previously found deregulated in animal models of PD and in PD patients. Relevant genes were selected for validation by real-time PCR in a subset of patients. The genes validated were linked to nucleic acid metabolism, mitochondria, immune response and intracellular-transport. Interestingly, we also found deregulation of these genes in a dopaminergic cell model of PD, a simple paradigm that can now be used to further dissect the role of these molecular players on dopaminergic cell loss. Altogether, our study provides preliminary evidence that expression changes in specific groups of genes and pathways, detected in peripheral blood samples, may be correlated with differential PD progression. Our exploratory study suggests that peripheral gene expression profiling may prove valuable for assisting in prediction of PD prognosis, and identifies novel culprits possibly involved in dopaminergic cell death. Given the exploratory nature of our study, further investigations using independent, well-characterized cohorts will be essential in order to validate our candidates as predictors of PD prognosis and to definitively confirm the value of gene expression analysis in aiding patient stratification and therapeutic intervention.

Published

2016

13. Cardiac Anderson-Fabry disease: Lessons from a 25-year-follow up

Author

Dulce Brito, Gabriel Miltenberger–Miltenyi, Oana Moldovan, Carmen Navarro, and Hugo Costa Madeira

Subjects

Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Sarcomeric hypertrophic cardiomyopathy (HCM) is the most common genetic cause of unexplained left ventricular hypertrophy and has no specific treatment. Anderson-Fabry disease (AFD) is rare and usually multisystemic, but occasionally expresses clinically as a predominantly cardiac phenotype mimicking HCM. We describe an illustrative case of a patient followed regularly for 25 years with a diagnosis of familial HCM and no identified sarcomeric mutations. Next-generation sequencing analysis identified a novel pathogenic mutation in the GLA gene, leading to a diagnosis of previously unknown multisystemic AFD, with consequent implications for the patient's treatment and prognosis and familial screening. Resumo: A miocardiopatia hipertrófica sarcomérica é a causa genética mais comum da hipertrofia ventricular esquerda inexplicada e não tem tratamento específico. A doença de Anderson-Fabry é rara, geralmente multissistémica mas, ocasionalmente, pode expressar-se clinicamente com um fenótipo predominantemente cardíaco, imitando miocardiopatia hipertrófica. Os autores descrevem o caso ilustrativo de uma doente seguida regularmente durante 25 anos com o diagnóstico de miocardiopatia hipertrófica familiar, sem mutação sarcomérica identificada. A utilização da análise de sequenciação de nova geração identificou uma mutação patogénica nova no gene GLA, aclarando o diagnóstico oculto de doença de Anderson-Fabry multissistémica, com as consequentes implicações terapêuticas, prognósticas e na investigação familiar. Keywords: Hypertrophic cardiomyopathy, Anderson-Fabry disease, Next-generation sequencing, Palavras-chave: Miocardiopatia hipertrófica, Doença de Anderson-Fabry, Sequenciação de nova geração

Published

2014

14. Impaired proteostasis contributes to renal tubular dysgenesis.

Author

Rita Machado de Oliveira, Zrinka Marijanovic, Filipe Carvalho, Gabriel Miltenberger Miltényi, Joana Estevão Matos, Sandra Tenreiro, Sónia Oliveira, Francisco Javier Enguita, Rosário Stone, and Tiago Fleming Outeiro

Subjects

Medicine, Science

Abstract

Protein conformational disorders are associated with the appearance, persistence, accumulation, and misprocessing of aberrant proteins in the cell. The etiology of renal tubular dysgenesis (RTD) is linked to mutations in the angiotensin-converting enzyme (ACE). Here, we report the identification of a novel ACE mutation (Q1069R) in an RTD patient. ACE Q1069R is found sequestered in the endoplasmic reticulum and is also subject to increased proteasomal degradation, preventing its transport to the cell surface and extracellular fluids. Modulation of cellular proteostasis by temperature shift causes an extension in the processing time and trafficking of ACE Q1069R resulting in partial rescue of the protein processing defect and an increase in plasma membrane levels. In addition, we found that temperature shifting causes the ACE Q1069R protein to be secreted in an active state, suggesting that the mutation does not affect the enzyme's catalytic properties.

Published

2011

15. Novel mutation in the KCNH2 gene associated with long QT syndrome

Author

Doroteia Silva, Gabriel Miltenberger-Miltenyi, Maria José Correia, and António Nunes Diogo

Subjects

Diseases of the circulatory (Cardiovascular) system, RC666-701

Published

2013

16. Rare Association of two Genetic Causes of Sudden Death in a Young Survivor

Author

Dulce Brito, Andreia Magalhães, Nuno Cortez-Dias, and Gabriel Miltenberger-Miltenyi

Subjects

Death, Sudden Cardiac, Cardiomyopathy, Hypertrophic, Familial, Adolescent, Brugada Syndrome, Diseases of the circulatory (Cardiovascular) system, RC666-701

17. A data-driven disease progression model of fluid biomarkers in genetic frontotemporal dementia

Author

Ione O.C. Woollacott, Cristina Polito, Philip Van Damme, Mathieu Vandenbulcke, Rose Bruffaerts, Diana Duro, Chiara Fenoglio, David M. Cash, Maria Rosário Almeida, Sonja Schönecker, C. Ferreira, Sónia Afonso, Matthis Synofzik, Sara Prioni, Marta Cañada, Mikel Tainta, Miguel Tábuas-Pereira, Christin Andersson, Caroline Graff, Miguel Castelo-Branco, Enrico Premi, Håkan Thonberg, Fabrizio Tagliavini, Rachelle Shafei, Benjamin Bender, Ana Gorostidi, Maria João Leitão, Jennifer M. Nicholas, Elise G.P. Dopper, Silvana Archetti, Esther E. Bron, Ana Verdelho, Ron Keren, Isabel Santana, Christen Shoesmith, Pietro Tiraboschi, Sergi Borrego-Écija, Michela Pievani, Sandro Sorbi, Rick van Minkelen, Hans-Otto Karnath, Albert Lladó, Caroline V. Greaves, Jaume Olives, Alessandro Padovani, Miren Zulaica, Giuliano Binetti, Martin Rosser, Pedro Rosa-Neto, Vesna Jelic, Alexander Gerhard, Rosa Rademakers, Sandra E. Black, Wiro J. Niessen, Tobias Hoegen, Rhian S Convery, Janne M. Papma, Maria Carmela Tartaglia, Emily Todd, Adrian Danek, Rita Guerreiro, Robart Bartha, Linn Öijerstedt, Giuseppe Di Fede, Sebastien Ourselin, Núria Bargalló, James B. Rowe, Christopher C Butler, Giorgio G. Fumagalli, Valentina Bessi, Alberto Benussi, Nick C. Fox, Beatriz Santiago, Ekaterina Rogaeva, Alazne Gabilondo, Giacomina Rossi, Mircea Balasa, David L. Thomas, Benedetta Nacmias, Veronica Redaelli, Anna Antonell, Vikram Venkatraghavan, Jonathan D. Rohrer, Jackie M. Poos, Yolande A.L. Pijnenburg, Lieke H.H. Meeter, Carlo Wilke, Sandra V. Loosli, Elio Scarpini, Tobias Langheinrich, Alina Díez, Elisa Semler, Elizabeth Finger, Begoña Indakoetxea, Jessica L. Panman, Carolyn Timberlake, Gemma Lombardi, Luisa Benussi, Morris Freedman, Barbara Borroni, Ricardo Taipa, Johannes Levin, Thomas E. Cope, Paul M. Thompson, Giorgio Giaccone, Valentina Cantoni, Arabella Bouzigues, Jose Bras, Serge Gauthier, Andrea Arighi, Stefan Klein, Fermin Moreno, Markus Otto, Georgia Peakman, Emma L. van der Ende, David F. Tang-Wai, Sarah Anderl-Straub, Jason D. Warren, Alexandre de Mendonça, Camilla Ferrari, Elisabeth Wlasich, Catharina Prix, Michele Veldsman, Raquel Sánchez-Valle, Sara Mitchell, Carolina Maruta, Robert Laforce, Paola Caroppo, Jorge Villanua, Imogen J Swift, Harro Seelaar, Henrik Zetterberg, Simon Mead, Simon Ducharme, Myriam Barandiaran, Katrina M. Moore, John C. van Swieten, Gabriel Miltenberger, Mario Masellis, Timothy Rittman, Lize C. Jiskoot, Daniela Galimberti, Rik Vandenberghe, Carolin Heller, Stefano Gazzina, Aitana Sogorb-Esteve, Roberto Gasparotti, Martina Bocchetta, Neurology, Amsterdam Neuroscience - Neurodegeneration, Repositório da Universidade de Lisboa, Radiology & Nuclear Medicine, and Neurosurgery

Subjects

Oncology, medicine.medical_specialty, Medizin, tau Proteins, Disease, medicine.disease_cause, frontotemporal dementia, biomarker, disease progression model, event-based modelling, neurofilament light chain, Biomarkers, C9orf72 Protein, Complement C1q, Cross-Sectional Studies, Disease Progression, Glial Fibrillary Acidic Protein, Humans, Longitudinal Studies, Mutation, Frontotemporal Dementia, diagnosis [Frontotemporal Dementia], Settore BIO/13 - Biologia Applicata, C9orf72, Internal medicine, Medicine, ddc:610, genetics [C9orf72 Protein], genetics [Frontotemporal Dementia], business.industry, medicine.disease, Astrogliosis, genetics [tau Proteins], Cohort, Biomarker (medicine), Neurology (clinical), Sample collection, business, Frontotemporal dementia

Abstract

© The Author(s) (2021). Published by Oxford University Press on behalf of the Guarantors of Brain. This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/ by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com, Several CSF and blood biomarkers for genetic frontotemporal dementia have been proposed, including those reflecting neuroaxonal loss (neurofilament light chain and phosphorylated neurofilament heavy chain), synapse dysfunction [neuronal pentraxin 2 (NPTX2)], astrogliosis (glial fibrillary acidic protein) and complement activation (C1q, C3b). Determining the sequence in which biomarkers become abnormal over the course of disease could facilitate disease staging and help identify mutation carriers with prodromal or early-stage frontotemporal dementia, which is especially important as pharmaceutical trials emerge. We aimed to model the sequence of biomarker abnormalities in presymptomatic and symptomatic genetic frontotemporal dementia using cross-sectional data from the Genetic Frontotemporal dementia Initiative (GENFI), a longitudinal cohort study. Two-hundred and seventy-five presymptomatic and 127 symptomatic carriers of mutations in GRN, C9orf72 or MAPT, as well as 247 non-carriers, were selected from the GENFI cohort based on availability of one or more of the aforementioned biomarkers. Nine presymptomatic carriers developed symptoms within 18 months of sample collection ('converters'). Sequences of biomarker abnormalities were modelled for the entire group using discriminative event-based modelling (DEBM) and for each genetic subgroup using co-initialized DEBM. These models estimate probabilistic biomarker abnormalities in a data-driven way and do not rely on previous diagnostic information or biomarker cut-off points. Using cross-validation, subjects were subsequently assigned a disease stage based on their position along the disease progression timeline. CSF NPTX2 was the first biomarker to become abnormal, followed by blood and CSF neurofilament light chain, blood phosphorylated neurofilament heavy chain, blood glial fibrillary acidic protein and finally CSF C3b and C1q. Biomarker orderings did not differ significantly between genetic subgroups, but more uncertainty was noted in the C9orf72 and MAPT groups than for GRN. Estimated disease stages could distinguish symptomatic from presymptomatic carriers and non-carriers with areas under the curve of 0.84 (95% confidence interval 0.80-0.89) and 0.90 (0.86-0.94) respectively. The areas under the curve to distinguish converters from non-converting presymptomatic carriers was 0.85 (0.75-0.95). Our data-driven model of genetic frontotemporal dementia revealed that NPTX2 and neurofilament light chain are the earliest to change among the selected biomarkers. Further research should investigate their utility as candidate selection tools for pharmaceutical trials. The model's ability to accurately estimate individual disease stages could improve patient stratification and track the efficacy of therapeutic interventions., This study was supported in the Netherlands by two Memorabel grants from Deltaplan Dementie (The Netherlands Organisation for Health Research and Development and Alzheimer Nederland; grant numbers 733050813,733050103 and 733050513), the Bluefield Project to Cure Frontotemporal Dementia, the Dioraphte foundation (grant number 1402 1300), the European Joint Programme—Neurodegenerative Disease Research and the Netherlands Organisation for Health Research and Development (PreFrontALS: 733051042, RiMod-FTD: 733051024); V.V. and S.K. have received funding from the European Union’s Horizon 2020 research and innovation programme under grant agreement no. 666992 (EuroPOND). E.B. was supported by the Hartstichting (PPP Allowance, 2018B011); in Belgium by the Mady Browaeys Fonds voor Onderzoek naar Frontotemporale Degeneratie; in the UK by the MRC UK GENFI grant (MR/M023664/1); J.D.R. is supported by an MRC Clinician Scientist Fellowship (MR/M008525/1) and has received funding from the NIHR Rare Disease Translational Research Collaboration (BRC149/NS/MH); I.J.S. is supported by the Alzheimer’s Association; J.B.R. is supported by the Wellcome Trust (103838); in Spain by the Fundació Marató de TV3 (20143810 to R.S.V.); in Germany by the Deutsche Forschungsgemeinschaft (DFG, German Research Foundation) under Germany’s Excellence Strategy within the framework of the Munich Cluster for Systems Neurology (EXC 2145 SyNergy—ID 390857198) and by grant 779357 ‘Solve-RD’ from the Horizon 2020 Research and Innovation Programme (to MS); in Sweden by grants from the Swedish FTD Initiative funded by the Schörling Foundation, grants from JPND PreFrontALS Swedish Research Council (VR) 529–2014-7504, Swedish Research Council (VR) 2015–02926, Swedish Research Council (VR) 2018–02754, Swedish Brain Foundation, Swedish Alzheimer Foundation, Stockholm County Council ALF, Swedish Demensfonden, Stohnes foundation, Gamla Tjänarinnor, Karolinska Institutet Doctoral Funding and StratNeuro. H.Z. is a Wallenberg Scholar.

Published

2022

18. Serum Phospholipid Profile Changes in Gaucher Disease and Parkinson’s Disease

Author

Laura López de Frutos, Francisco Almeida, Jessica Murillo-Saich, Vasco A. Conceição, Monica Guma, Oswald Queheberger, Pilar Giraldo, and Gabriel Miltenberger-Miltenyi

Subjects

Sphingolipids, 1-Deoxynojirimycin, Gaucher Disease, Parkinson’s disease, Gaucher disease, plasma phospholipids, GBA1, miglustat, dopamine agonist, Phosphatidylethanolamines, Organic Chemistry, Plasmalogens, Parkinson Disease, Phosphatidylglycerols, General Medicine, Phosphatidylserines, Catalysis, Computer Science Applications, Inorganic Chemistry, Dopamine Agonists, Mutation, Phosphatidylcholines, Humans, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Biomarkers

Abstract

Alterations in the levels of serum sphingolipids and phospholipids have been reported in Gaucher disease and in Parkinson’s disease, suggesting a potential role of these lipids as biomarkers. This project’s objective is to detect novel associations and novel candidate biomarkers in the largest Spanish Gaucher and Parkinson diseases of the Iberian Peninsula. For that, 278 participants were included: 100 sporadic Parkinson’s patients, 70 Gaucher patients, 15 GBA1-mutation-carrier Parkinson’s patients and 93 controls. A serum lipidomics array including 10 phospholipid groups, 368 species, was performed using high-performance liquid chromatography–mass spectrometry. Lipid levels were compared between groups via multiple-regression analyses controlling for clinical and demographic parameters. Additionally, lipid levels were compared within the Gaucher and Parkinson’s groups controlling for medication and/or disease severity. Results were controlled for robustness by filtering of non-detectable lipid values. There was an increase in the levels of phosphatidylcholine, with a simultaneous decrease in lyso-phosphatidylcholine, in the Gaucher, Parkinson’s and GBA1-mutation-carrier Parkinson’s patients vs. controls. Phosphatidylethanolamine, lyso- and plasmalogen-phosphatidylethanolamine were also increased in Gaucher and Parkinson’s. Gaucher patients also showed an increase in lyso-phosphatidylserine and phosphatidylglycerol. While in the Gaucher and Parkinson’s groups, velaglucerase alpha and dopamine agonists, respectively, showed positive associations with the lipid changes, miglustat treatment in Gaucher patients normalized the altered phosphatidylcholine/lyso-phosphatidylcholine ratio. In conclusion, Gaucher and Parkinson’s patients showed changes in various serum phospholipid levels when compared with healthy controls, further supporting the role of such lipids in disease development and, possibly, as putative biomarkers. This hypothesis was reinforced by the normalizing effect of miglustat, and by controlling for data robustness, even though the limited number of participants, especially in the sub-distribution by treatment groups in GD requires validation in a larger number of patients.

Published

2022

19. Interaction between VPS13A and the XK scramblase is required to prevent VPS13A disease in humans

Author

Jae-Sook Park, Yiying Hu, Nancy. M. Hollingsworth, Gabriel Miltenberger-Miltenyi, and Aaron M. Neiman

Abstract

VPS13 family proteins form conduits between the membranes of different organelles through which lipids are transferred. In humans there are four VPS13 paralogs each of which is required to prevent a different inherited disorder. VPS13 proteins contain multiple conserved domains. The VAB domain binds to adaptor proteins to recruit VPS13 to specific membrane contact sites. This work demonstrates the importance of a different domain in VPS13A in preventing VPS13A disease (chorea-acanthocytosis). The Pleckstrin Homology (PH) domain at the C-terminus of VPS13A is required to form a complex with the XK scramblase and for proper localization of VPS13A within the cell. Mutations in the interaction surface between VPS13A and XK predicted by Alphafold modeling disrupt complex formation and colocalization of the two proteins. Mutant VPS13A alleles found in patients with VPS13A disease truncate the PH domain. The phenotypic similarities between VPS13A disease and McLeod syndrome caused by mutations in XK argue that loss of VPS13A-XK complex is the basis of both diseases.Summary StatementVPS13A disease and McLeod syndrome are related disorders caused by mutation of the VPS13A and XK genes, respectively. A pathologic VPS13A mutation disrupts binding of the VPS13A and XK proteins, suggesting a common basis of both diseases.

Published

2022

20. Interaction between VPS13A and the XK scramblase is important for VPS13A function in humans

Author

Jae-Sook Park, Yiying Hu, Nancy M. Hollingsworth, Gabriel Miltenberger-Miltenyi, and Aaron M. Neiman

Subjects

complications [Neuroacanthocytosis], VPS13A protein, human, PH domain, Vesicular Transport Proteins, genetics [Mutation], Cell Biology, VPS13A, Lipid transport, Neuro-acanthocytosis syndromes, genetics [Vesicular Transport Proteins], metabolism [Neuroacanthocytosis], ddc:570, Mitochondrial Membranes, Mutation, metabolism [Mitochondrial Membranes], metabolism [Vesicular Transport Proteins], Humans, genetics [Neuroacanthocytosis], XK, Neurodegeneration, Neuroacanthocytosis

Abstract

VPS13 family proteins form conduits between the membranes of different organelles through which lipids are transferred. In humans, there are four VPS13 paralogs, and mutations in the genes encoding each of them are associated with different inherited disorders. VPS13 proteins contain multiple conserved domains. The Vps13 adaptor-binding (VAB) domain binds to adaptor proteins that recruit VPS13 to specific membrane contact sites. This work demonstrates the importance of a different domain in VPS13A function. The pleckstrin homology (PH) domain at the C-terminal region of VPS13A is required to form a complex with the XK scramblase and for the co-localization of VPS13A with XK within the cell. Alphafold modeling was used to predict an interaction surface between VPS13A and XK. Mutations in this region disrupt both complex formation and co-localization of the two proteins. Mutant VPS13A alleles found in patients with VPS13A disease truncate the PH domain. The phenotypic similarities between VPS13A disease and McLeod syndrome caused by mutations in VPS13A and XK, respectively, argue that loss of the VPS13A–XK complex is the basis of both diseases.

Published

2022

21. A panel of CSF proteins separates genetic frontotemporal dementia from presymptomatic mutation carriers

Author

Yolande A.L. Pijnenburg, Alessandro Padovani, Lieke H.H. Meeter, Rita Guerreiro, Mathieu Vandenbulcke, Rose Bruffaerts, Sonja Schönecker, Sofia Bergström, Florence Pasquier, Mikel Tainta, Beatriz Santiago, Roberto Gasparotti, Maria Rosário Almeida, Núria Bargalló, Abbe Ullgren, Martina Bocchetta, James B. Rowe, Pietro Tiraboschi, Robart Bartha, Rachelle Shafei, Benjamin Bender, Anna Månberg, Enrico Premi, Sergi Borrego-Écija, Sandro Sorbi, Christopher C Butler, Rick van Minkelen, Alberto Benussi, Marta Cañada, Carlo Wilke, Christin Andersson, Caroline Graff, Isabel Santana, Elisa Semler, Valentina Bessi, Miren Zulaica, Benedetta Nacmias, Tobias Langheinrich, Christen Shoesmith, Philip Van Damme, Camilla Ferrari, Martin Rosser, Pedro Rosa-Neto, Alexandre de Mendonça, Jennifer M. Nicholas, Catharina Prix, Sebastien Ourselin, Michele Veldsman, Jessica L. Panman, Håkan Thonberg, Jennie Olofsson, Paul M. Thompson, Ana Gorostidi, Andrea Arighi, Raquel Sánchez-Valle, Anna Antonell, Vesna Jelic, Ana Verdelho, Sara Mitchell, Janne M. Papma, Alina Díez, Giuliano Binetti, Rhian S Convery, Silvana Archetti, Ekaterina Rogaeva, Michela Pievani, C. Ferreira, Hans-Otto Karnath, Veronica Redaelli, Giuseppe Di Fede, Giovanni B. Frisoni, Carolina Maruta, Giacomina Rossi, Jaume Olives, Simon Ducharme, Roberta Ghidoni, Alexander Gerhard, Ron Keren, Johannes Levin, Sandra V. Loosli, Jose Bras, Isabelle Le Ber, Emily Todd, Robert Laforce, Sónia Afonso, Matthis Synofzik, Alazne Gabilondo, Elizabeth Finger, Thomas E. Cope, Paola Caroppo, Jorge Villanua, Diana Duro, Georgia Peakman, Giorgio G. Fumagalli, Serge Gauthier, Mario Masellis, Markus Otto, Caroline V. Greaves, Carolyn Timberlake, Harro Seelaar, Ione O.C. Woollacott, Sara Prioni, Jason D. Warren, Cristina Polito, Miguel Tábuas-Pereira, David F. Tang-Wai, Carmela Tartaglia, Linn Öijerstedt, Luisa Benussi, Barbara Borroni, Ricardo Taipa, Albert Lladó, Mircea Balasa, Rosa Rademakers, Lize C. Jiskoot, Miguel Castelo-Branco, Julia Remnestål, Fabrizio Tagliavini, Giorgio Giaccone, Maria João Leitão, Henrik Zetterberg, Valentina Cantoni, Daniela Galimberti, Sarah Anderl-Straub, Simon Mead, Myriam Barandiaran, Adrian Danek, Timothy Rittman, Chiara Fenoglio, Katrina M. Moore, David M. Cash, Rik Vandenberghe, Peter Nilsson, Elisabeth Wlasich, John C. van Swieten, Morris Freedman, Sandra E. Black, Carolin Heller, Stefano Gazzina, Gabriel Miltenberger, Fermin Moreno, Nick C. Fox, David L. Thomas, Jonathan D. Rohrer, Begoña Indakoetxea, Tobias Hoegen, Gemma Lombardi, Elio Scarpini, Bergström, Sofia [0000-0003-2910-4754], Apollo - University of Cambridge Repository, Neurology, Amsterdam Neuroscience - Neurodegeneration, Genetic Frontotemporal Dementia Initiative (GENFI), Jiskoot, Lize (Beitragende*r), Rowe, James B. (Beitragende*r), de Mendonça, Alexandre (Beitragende*r), Tagliavini, Fabrizio (Beitragende*r), Santana, Isabel (Beitragende*r), Le Ber, Isabelle (Beitragende*r), Levin, Johannes (Beitragende*r), Danek, Adrian (Beitragende*r), Otto, Markus (Beitragende*r), Frisoni, Giovanni (Beitragende*r), Ghidoni, Roberta (Beitragende*r), Sorbi, Sandro (Beitragende*r), Pasquier, Florence (Beitragende*r), Jelic, Vesna (Beitragende*r), Andersson, Christin (Beitragende*r), Afonso, Sónia (Beitragende*r), Almeida, Maria Rosario (Beitragende*r), Anderl-Straub, Sarah (Beitragende*r), Antonell, Anna (Beitragende*r), Archetti, Silvana (Beitragende*r), Arighi, Andrea (Beitragende*r), Balasa, Mircea (Beitragende*r), Barandiaran, Myriam (Beitragende*r), Bargalló, Nuria (Beitragende*r), Bartha, Robart (Beitragende*r), Bender, Benjamin (Beitragende*r), Benussi, Alberto (Beitragende*r), Benussi, Luisa (Beitragende*r), Bessi, Valentina (Beitragende*r), Binetti, Giuliano (Beitragende*r), Black, Sandra (Beitragende*r), Bocchetta, Martina (Beitragende*r), Borrego-Ecija, Sergi (Beitragende*r), Bras, Jose (Beitragende*r), Bruffaerts, Rose (Beitragende*r), Cañada, Marta (Beitragende*r), Cantoni, Valentina (Beitragende*r), Caroppo, Paola (Beitragende*r), Cash, David (Beitragende*r), Castelo-Branco, Miguel (Beitragende*r), Convery, Rhian (Beitragende*r), Cope, Thomas (Beitragende*r), Di Fede, Giuseppe (Beitragende*r), Díez, Alina (Beitragende*r), Duro, Diana (Beitragende*r), Fenoglio, Chiara (Beitragende*r), Ferrari, Camilla (Beitragende*r), Ferreira, Catarina B. (Beitragende*r), Fox, Nick (Beitragende*r), Freedman, Morris (Beitragende*r), Fumagalli, Giorgio (Beitragende*r), Gabilondo, Alazne (Beitragende*r), Gasparotti, Roberto (Beitragende*r), Gauthier, Serge (Beitragende*r), Gazzina, Stefano (Beitragende*r), Giaccone, Giorgio (Beitragende*r), Gorostidi, Ana (Beitragende*r), Greaves, Caroline (Beitragende*r), Guerreiro, Rita (Beitragende*r), Heller, Carolin (Beitragende*r), Hoegen, Tobias (Beitragende*r), Indakoetxea, Begoña (Beitragende*r), Karnath, Hans-Otto (Beitragende*r), Keren, Ron (Beitragende*r), Langheinrich, Tobias (Beitragende*r), Leitão, Maria João (Beitragende*r), Lladó, Albert (Beitragende*r), Lombardi, Gemma (Beitragende*r), Loosli, Sandra (Beitragende*r), Maruta, Carolina (Beitragende*r), Mead, Simon (Beitragende*r), Meeter, Lieke (Beitragende*r), Miltenberger, Gabriel (Beitragende*r), van Minkelen, Rick (Beitragende*r), Mitchell, Sara (Beitragende*r), Moore, Katrina (Beitragende*r), Nacmias, Benedetta (Beitragende*r), Nicholas, Jennifer (Beitragende*r), Olives, Jaume (Beitragende*r), Ourselin, Sebastien (Beitragende*r), Padovani, Alessandro (Beitragende*r), Panman, Jessica (Beitragende*r), Papma, Janne M. (Beitragende*r), Peakman, Georgia (Beitragende*r), Pievani, Michela (Beitragende*r), Pijnenburg, Yolande (Beitragende*r), Polito, Cristina (Beitragende*r), Premi, Enrico (Beitragende*r), Prioni, Sara (Beitragende*r), Prix, Catharina (Beitragende*r), Rademakers, Rosa (Beitragende*r), Redaelli, Veronica (Beitragende*r), Rittman, Tim (Beitragende*r), Rogaeva, Ekaterina (Beitragende*r), Rosa-Neto, Pedro (Beitragende*r), Rossi, Giacomina (Beitragende*r), Rosser, Martin (Beitragende*r), Santiago, Beatriz (Beitragende*r), Scarpini, Elio (Beitragende*r), Schönecker, Sonja (Beitragende*r), Semler, Elisa (Beitragende*r), Shafei, Rachelle (Beitragende*r), Shoesmith, Christen (Beitragende*r), Tábuas-Pereira, Miguel (Beitragende*r), Tainta, Mikel (Beitragende*r), Taipa, Ricardo (Beitragende*r), Tang-Wai, David (Beitragende*r), Thomas, David L. (Beitragende*r), Thompson, Paul (Beitragende*r), Thonberg, Håkan (Beitragende*r), Timberlake, Carolyn (Beitragende*r), Tiraboschi, Pietro (Beitragende*r), Todd, Emily (Beitragende*r), Van Damme, Philip (Beitragende*r), Vandenbulcke, Mathieu (Beitragende*r), Veldsman, Michele (Beitragende*r), Verdelho, Ana (Beitragende*r), Villanua, Jorge (Beitragende*r), Warren, Jason (Beitragende*r), Wilke, Carlo (Beitragende*r), Woollacott, Ione (Beitragende*r), Wlasich, Elisabeth (Beitragende*r), Zetterberg, Henrik (Beitragende*r), and Zulaica, Miren (Beitragende*r)

Subjects

medicine.medical_specialty, Neurology, NEFM, Medizin, genetics [Mutation], LASSO, Biology, Aquaporin 4 (AQP4), Neurosecretory protein VGF (VGF), DISEASE, genetics [Progranulins], Cellular and Molecular Neuroscience, Progranulins, CEREBROSPINAL-FLUID, C9orf72, ddc:570, medicine, CRITERIA, Humans, Neuronal pentraxin 2 (NPTX2), RC346-429, genetics [Frontotemporal Dementia], Molecular Biology, Pathological, Genetics, Science & Technology, Neurosciences, RC952-954.6, Brain, Neurofilament medium polypeptide (NEFM), medicine.disease, Molecular medicine, Cerebrospinal fluid, Aquaporin 4, Geriatrics, Suspension bead array, Frontotemporal Dementia, Mutation, Mutation (genetic algorithm), Neurosciences & Neurology, Neurology. Diseases of the nervous system, Neurology (clinical), Life Sciences & Biomedicine, Random forest, Biomarkers, Research Article, Frontotemporal dementia

Abstract

Availability of data and materials: The datasets used and/or analysed during the current study are available from the corresponding author on reasonable request. Supplementary Information: Additional file 1 of A panel of CSF proteins separates genetic frontotemporal dementia from presymptomatic mutation carriers: a GENFI study; Additional file 2 of A panel of CSF proteins separates genetic frontotemporal dementia from presymptomatic mutation carriers: a GENFI study; both files are available online at https://doi.org/10.1186/s13024-021-00499-4 Copyright © The Author(s) 2021. Background: A detailed understanding of the pathological processes involved in genetic frontotemporal dementia is critical in order to provide the patients with an optimal future treatment. Protein levels in CSF have the potential to reflect different pathophysiological processes in the brain. We aimed to identify and evaluate panels of CSF proteins with potential to separate symptomatic individuals from individuals without clinical symptoms (unaffected), as well as presymptomatic individuals from mutation non-carriers. Methods: A multiplexed antibody-based suspension bead array was used to analyse levels of 111 proteins in CSF samples from 221 individuals from families with genetic frontotemporal dementia. The data was explored using LASSO and Random forest. Results: When comparing affected individuals with unaffected individuals, 14 proteins were identified as potentially important for the separation. Among these, four were identified as most important, namely neurofilament medium polypeptide (NEFM), neuronal pentraxin 2 (NPTX2), neurosecretory protein VGF (VGF) and aquaporin 4 (AQP4). The combined profile of these four proteins successfully separated the two groups, with higher levels of NEFM and AQP4 and lower levels of NPTX2 in affected compared to unaffected individuals. VGF contributed to the models, but the levels were not significantly lower in affected individuals. Next, when comparing presymptomatic GRN and C9orf72 mutation carriers in proximity to symptom onset with mutation non-carriers, six proteins were identified with a potential to contribute to a separation, including progranulin (GRN). Conclusion: In conclusion, we have identified several proteins with the combined potential to separate affected individuals from unaffected individuals, as well as proteins with potential to contribute to the separation between presymptomatic individuals and mutation non-carriers. Further studies are needed to continue the investigation of these proteins and their potential association to the pathophysiological mechanisms in genetic FTD. This study has received support from the Swedish FTD initiative funded by the Schörling Family Foundation. This work was also funded by KTH Center for Applied Precision Medicine (KCAP) funded by the Erling-Persson Family Foundation, grants from Vetenskapsrådet Dnr 529-2014-7504, VR 2015-02926 and 2018-02754, Swedish Alzheimer Foundation, Swedish Brain Foundation, Åhlén foundation, Demensfonden, Stohnes foundation, Gamla Tjänarinnor and Stockholm County Council ALF. Furthermore, support was received by the MRC UK GENFI grant (MR/M023664/1), the Bluefield Project, the JPND GENFI-PROX grant (2019-02248), the Dioraphte Foundation [grant numbers 09-02-00]; the Association for Frontotemporal Dementias Research Grant 2009; The Netherlands Organization for Scientific Research (NWO) (grant HCMI 056-13-018); ZonMw Memorabel (Deltaplan Dementie), (project numbers 733 050 103 and 733 050 813); JPND PreFrontAls consortium (project number 733051042). JDR is supported by an MRC Clinician Scientist Fellowship (MR/M008525/1) and has received funding from the NIHR Rare Disease Translational Research Collaboration (BRC149/NS/MH). Several authors of this publication are members of the European Reference Network for Rare Neurological Diseases - Project ID No 739510. M.S. was supported by the JPND grant “GENFI-prox” (by DLR/BMBF to M. S, joint with JDR., J.vS., M.O., B.B. and C.G.). Open Access funding provided by Royal Institute of Technology.

Published

2021

22. Fabry Disease Therapy: State-of-the-Art and Current Challenges

Author

Damião Cunha, Nuno Sousa, Miguel Gago, Gabriel Miltenberger-Miltenyi, Olga Azevedo, and Universidade do Minho

Subjects

0301 basic medicine, 1-Deoxynojirimycin, pegunigalsidase alfa, Genetic enhancement, mRNA, migalastat, Review, 030105 genetics & heredity, Bioinformatics, Catalysis, Inorganic Chemistry, lcsh:Chemistry, 03 medical and health sciences, Migalastat, medicine, Humans, Substrate reduction therapy, Physical and Theoretical Chemistry, substrate reduction, Molecular Biology, lcsh:QH301-705.5, Spectroscopy, moss-derived alfa galactosidase A, fabry disease, agalsidase alfa, Science & Technology, business.industry, Organic Chemistry, General Medicine, Enzyme replacement therapy, medicine.disease, Fabry disease, gene therapy, Recombinant Proteins, 3. Good health, Computer Science Applications, AGALSIDASE BETA, Isoenzymes, Clinical trial, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, alpha-Galactosidase, agalsidase beta, business, Agalsidase alfa, enzyme replacement therapy

Abstract

Fabry disease (FD) is a lysosomal storage disorder caused by mutations of the GLA gene that lead to a deficiency of the enzymatic activity of α-galactosidase A. Available therapies for FD include enzyme replacement therapy (ERT) (agalsidase alfa and agalsidase beta) and the chaperone migalastat. Despite the large body of literature published about ERT over the years, many issues remain unresolved, such as the optimal dose, the best timing to start therapy, and the clinical impact of anti-drug antibodies. Migalastat was recently approved for FD patients with amenable GLA mutations; however, recent studies have raised concerns that “in vitro” amenability may not always reflect “in vivo” amenability, and some findings on real-life studies have contrasted with the results of the pivotal clinical trials. Moreover, both FD specific therapies present limitations, and the attempt to correct the enzymatic deficiency, either by enzyme exogenous administration or enzyme stabilization with a chaperone, has not shown to be able to fully revert FD pathology and clinical manifestations. Therefore, several new therapies are under research, including new forms of ERT, substrate reduction therapy, mRNA therapy, and gene therapy. In this review, we provide an overview of the state-of-the-art on the currently approved and emerging new therapies for adult patients with FD.

Published

2021

23. Founder effect of Fabry disease due to p.F113L mutation: Clinical profile of a late-onset phenotype

Author

Emilia Lopes, Rui Faria, Paulo Gaspar, Olga Azevedo, Alice Martins, Jorge Rodrigues, Sónia Simões, Gabriel Miltenberger-Miltenyi, Pedro Reimão, Nuno Sousa, Olga Pereira, Damião Cunha, Fátima Dias, Miguel Gago, Andreas Gal, and Maria José Guimarães

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, Cardiomyopathy, 030105 genetics & heredity, Left ventricular hypertrophy, Biochemistry, Gastroenterology, Bifascicular block, Late Onset Disorders, Cohort Studies, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Internal medicine, Genetics, Humans, Medicine, Cornea verticillata, Molecular Biology, Aged, Aged, 80 and over, Portugal, business.industry, Haplotype, Hypertrophic cardiomyopathy, Cardiomyopathy, Hypertrophic, Middle Aged, medicine.disease, Fabry disease, Founder Effect, 3. Good health, Phenotype, alpha-Galactosidase, Mutation, Fabry Disease, Female, medicine.symptom, business, 030217 neurology & neurosurgery, Founder effect

Abstract

Background Knowledge on clinical profiles of late-onset phenotypes of Fabry disease (FD) is essential to better define their natural history. Our study aims to demonstrate a founder effect of FD due to the GLA gene mutation c.337T>C (p.F113L) in the Portuguese region of Guimaraes; and to characterize the clinical profile of this late-onset phenotype in a large cohort of genetically related adult patients, living in the same region. Methods and Results FD screening was performed in 150 adult patients with hypertrophic cardiomyopathy (HCM) and found 25 Fabry patients (16.6%). The p.F113L mutation was found in 21 of them, leading to a genealogy study and haplotype analysis of the p.F113L patients. Genealogy research revealed a 12-generation family tree with a common ancestor to p.F113L patients, suggesting a founder effect that was supported by haplotype findings. Pedigree analysis was performed and 120 consecutive p.F113L patients underwent a predefined diagnostic evaluation of FD multiorgan involvement. This late-onset phenotype was characterized by common and/or potentially severe cardiac manifestations (left ventricular hypertrophy 40.8%, atrial fibrillation 5%, non-sustained ventricular tachycardia 12.5%, atrioventricular block 18.3%, bifascicular block 13.4%). Extracardiac manifestations included albuminuria>30 mg/24 h 36.1%, chronic kidney disease≥G3 7.6%, brain white matter lesions 54.4%, stroke 3.3%, sensorineural deafness 44.5%, cornea verticillata 13.9%. Plasma lyso-GB3 was undetectable in females, regardless of clinical manifestations. Conclusion A founder effect of FD due to p.F113L mutation was documented by genealogy and genetics in a Portuguese region. In this late-onset phenotype, although cardiac manifestations carry the highest prognostic impact, extracardiac involvement is common.

Published

2020

24. Social cognition impairment in genetic frontotemporal dementia within the GENFI cohort

Author

Rachelle Shafei, Benjamin Bender, Jackie M. Poos, Maria Carmela Tartaglia, Janne M. Papma, Lieke H.H. Meeter, Isabel Santana, Christen Shoesmith, Mikel Tainta, Simon Mead, Albert Lladó, Alazne Gabilondo, Emanuela Rotondo, Alexander Gerhard, Simon Ducharme, Myriam Barandiaran, Mario Masellis, Caroline V. Greaves, Jaume Olives, Rita Guerreiro, Andrea Arighi, Diana Duro NPsych, Sara Mitchell, Roberto Gasparotti, Mathieu Vandenbulcke, Tobias Langheinrich, Thomas E. Cope, Martina Bocchetta, Robart Bartha, Daid Tang-Wai, Jessica L. Panman, Maria Rosário Almeida, Christopher C Butler, Rose Bruffaerts, Núria Bargalló, Pietro Tiraboschi, Beatriz Santiago, Elisabeth Wlasich, Philip Vandamme, Giorgio Giaccone, Sergi Borrego-Écija, Sonja Schönecker, Robert Laforce, Paola Caroppo, Katrina M. Moore, Ione O.C. Woollacott, Maria de Arriba, Veronica Redaelli, Rick van Minkelen, Jorge Villanua, Sónia Afonso, Matthis Synofzik, Nick C. Fox, Jennifer M. Nicholas, David L. Thomas, James B. Rowe, Carlo Wilke, Miren Zulaica, Pedro Rosa-Neto, Jonathan D. Rohrer, Elizabeth Finger, Carolyn Timberlake, C. Ferreira, David M. Cash, Timothy Rittman, Alessandro Padovani, Barbara Borroni, Ricardo Taipa, John C. van Swieten, Sandra V. Loosli, Begoña Indakoetxea, Daniela Galimberti, Sandra E. Black, Ana Gorostidi, Vesna Jelic, Catharina Prix, Ron Keren, Y.A.L. Pijnenburg, Michele Veldsman, Rosa Rademakers, Adrian Danek, Zigor Diaz, Miguel Tábuas-Pereira, Johannes Levin, Raquel Sánchez-Valle, Jose Bras, Rhian S Convery, Silvana Archetti, Markus Otto, Miguel Castelo-Branco, Rik Vandenberghe, Anna Antonell, Fabrizio Tagliavini, Sarah Anderl-Straub, Giuseppe Di Fede, Martin N. Rossor, Carolina Maruta MPsych, Enrico Premi, Giorgio G. Fumagalli, Sara Prioni, Cristina Muscio, Maria João Leitão, Lucy L. Russell, Håkan Thonberg, Ana Verdelho, Gabriel Miltenberger, Ekaterina Rogaeva, Giacomina Rossi, Linn Öijerstedt, Christin Andersson, Caroline Graff, Serge Gauthier, Maura Cosseddu MPsych, Carolin Heller, Stefano Gazzina, Jason D. Warren, Chiara Fenoglio, Tobias Hoegen, Elio Scarpini, Morris Freedman, Fermin Moreno, Mircea Balasa, Lize C. Jiskoot, Alexandre de Mendonça, Paul Thompson, Elisa Semler, Hans-Otto Karnarth, Amsterdam Neuroscience - Neurodegeneration, Neurology, Clinical Genetics, and Repositório da Universidade de Lisboa

Subjects

Social Cognition, C9orf72, Emotion processing, Facial emotion recognition, Faux pas, Frontotemporal dementia, MAPT, Progranulin, Theory of mind, 1702 Cognitive Sciences, Medizin, Social Sciences, Audiology, DISEASE, Behavioural Neurology, genetics [Progranulins], 0302 clinical medicine, Progranulins, Psychology, genetics [Frontotemporal Dementia], Faux pa, Psychology, Experimental, NEUROANATOMY, 05 social sciences, Genetic FTD Initiative, GENFI, Experimental Psychology, MIND, Magnetic Resonance Imaging, ORBITOFRONTAL CORTEX, Neuropsychology and Physiological Psychology, Frontal lobe, Frontotemporal Dementia, Life Sciences & Biomedicine, Behavioral Sciences, medicine.medical_specialty, Cognitive Neuroscience, FRONTAL VARIANT, Experimental and Cognitive Psychology, 050105 experimental psychology, Lateralization of brain function, Temporal lobe, 03 medical and health sciences, AGE, Social cognition, mental disorders, medicine, Humans, 0501 psychology and cognitive sciences, ddc:610, genetics [C9orf72 Protein], DECLINE, Science & Technology, EMOTION RECOGNITION, C9orf72 Protein, Neurosciences, PERFORMANCE, medicine.disease, Facial emotion recognitions, 1701 Psychology, Mutation, Orbitofrontal cortex, Neurosciences & Neurology, GENDER, 1109 Neurosciences, Insula, 030217 neurology & neurosurgery

Abstract

© 2020 The Author(s). Published by Elsevier Ltd. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/)., A key symptom of frontotemporal dementia (FTD) is difficulty interacting socially with others. Social cognition problems in FTD include impaired emotion processing and theory of mind difficulties, and whilst these have been studied extensively in sporadic FTD, few studies have investigated them in familial FTD. Facial Emotion Recognition (FER) and Faux Pas (FP) recognition tests were used to study social cognition within the Genetic Frontotemporal Dementia Initiative (GENFI), a large familial FTD cohort of C9orf72, GRN, and MAPT mutation carriers. 627 participants undertook at least one of the tasks, and were separated into mutation-negative healthy controls, presymptomatic mutation carriers (split into early and late groups) and symptomatic mutation carriers. Groups were compared using a linear regression model with bootstrapping, adjusting for age, sex, education, and for the FP recognition test, language. Neural correlates of social cognition deficits were explored using a voxel-based morphometry (VBM) study. All three of the symptomatic genetic groups were impaired on both tasks with no significant difference between them. However, prior to onset, only the late presymptomatic C9orf72 mutation carriers on the FER test were impaired compared to the control group, with a subanalysis showing differences particularly in fear and sadness. The VBM analysis revealed that impaired social cognition was mainly associated with a left hemisphere predominant network of regions involving particularly the striatum, orbitofrontal cortex and insula, and to a lesser extent the inferomedial temporal lobe and other areas of the frontal lobe. In conclusion, theory of mind and emotion processing abilities are impaired in familial FTD, with early changes occurring prior to symptom onset in C9orf72 presymptomatic mutation carriers. Future work should investigate how performance changes over time, in order to gain a clearer insight into social cognitive impairment over the course of the disease.

Published

2020

25. Postmortem genetic testing: Clinical diagnosis is not ended by the patient’s death

Author

Bebiana Faria, Sílvia Ribeiro, Lucy Calvo, Gabriel Miltenberger-Miltenyi, António Lourenço, Luís Coelho, Victor Sanfins, João Primo, and Katerina Puentes

Subjects

lcsh:Diseases of the circulatory (Cardiovascular) system, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Cardiomyopathy, Autopsy, Disease, medicine.disease, Asymptomatic, Sudden death, lcsh:RC666-701, Hereditary Diseases, medicine, General Earth and Planetary Sciences, medicine.symptom, business, Intensive care medicine, General Environmental Science, Genetic testing, Brugada syndrome

Abstract

In up to one-third of cases of sudden death, the medico-legal autopsy finding is inconclusive, and the option to perform a molecular autopsy is covered in international guidelines. The importance of postmortem genetic testing lies in its ability to identify hereditary diseases, often those with an autosomal dominant transmission pattern, and, through consultations and screening of relatives, to identify family members with a pathogenic mutation, who are often asymptomatic, providing an opportunity to change the course of their lives. The authors present three clinical cases that highlight the importance of postmortem genetic studies and family studies, as well as the integration of the data obtained in a cardiology consultation, which may be for arrhythmology, coronary disease or cardiomyopathy, depending on the specific condition. This could modify the course of the disease in many relatives. Resumo: Em até um terço dos casos de morte súbita, a autópsia médico-legal é “branca”, estando já contemplada nas recomendações internacionais a possibilidade da realização de autópsia molecular. A importância do teste genético post mortem prende-se com a identificação de doenças hereditárias, frequentemente doenças com padrão de transmissão autossómico dominante, sendo possível, através de consulta e rastreio de parentes, identificar elementos na família com a doença, não raramente portadores assintomáticos de uma mutação, havendo espaço para alterar o curso de vida dos mesmos. Os autores apresentam três casos clínicos que reforçam o quão importante é o estudo genético post mortem, assim como o estudo familiar e a integração dos dados numa consulta de cardiologia, seja arritmologia, consulta de doença coronária ou miocardiopatias, dependendo da patologia específica, podendo modificar o curso da doença em muitos parentes. Keywords: Autopsy, Postmortem genetic testing, Channelopathies, Brugada syndrome, Palavras-chave: Autópsia, Teste genético post mortem, Canalopatias, Síndrome de Brugada

Published

2019

26. Natural history of the late-onset phenotype of Fabry disease due to the p.F113L mutation

Author

Ana Teresa Vide, Olga Azevedo, Maria José Guimarães, Maria Antónia Costa, Damião Cunha, Miguel Gago, Gonçalo Castelo Branco, Nuno Sousa, Ana Raquel Robles, Ana Salgado, Olga Pereira, Sónia Simões, and Gabriel Miltenberger-Miltenyi

Subjects

medicine.medical_specialty, Natural history, Late onset, Late-onset, Ventricular tachycardia, Left ventricular hypertrophy, 03 medical and health sciences, QRS complex, 0302 clinical medicine, Endocrinology, Internal medicine, Genetics, medicine, Molecular Biology, lcsh:QH301-705.5, Fabry disease, 0303 health sciences, lcsh:R5-920, business.industry, 030305 genetics & heredity, F113L, medicine.disease, Phenotype, lcsh:Biology (General), Heart failure, Cardiology, business, lcsh:Medicine (General), Cardiac, 030217 neurology & neurosurgery, Research Paper, Founder effect

Abstract

Background: The common GLA gene mutation p.F113L causes late-onset phenotype of Fabry disease (FD) with predominant cardiac manifestations. A founder effect of FD due to this mutation was found in the Portuguese region of Guimarães. Our study aims to deepen the knowledge on the natural history of this late-onset variant. Methods: 203 consecutive adult Fabry patients with p.F113L mutation (79 males; mean age 46 ± 18 years), from this region, were submitted at baseline to a predefined diagnostic protocol. The occurrence of FD manifestations was analyzed in each decade of age in both genders. Results: In males, left ventricular hypertrophy (40.2%) and late gadolinium enhancement (21.4%) arose over 30 years; heart failure (HF) (21.9%), ventricular tachycardia (8.9%) and conduction disorders over 40 years; and bifascicular (13.1%) and complete atrioventricular blocks (5.9%) beyond 50 years of age. Cardiac manifestations occurred more commonly and 1–2 decades earlier in males; their frequency increased with age. Septum and posterior wall thickness, LV mass, QRS interval duration and pro-BNP levels increased with age in both genders. Mean survival free from HF (64 ± 1 vs. 76 ± 2 years) and pacemaker (71 ± 2 vs. 86 ± 1 years) was higher in females (p

Published

2020

27. Serum lipid alterations in GBA-associated Parkinson's disease

Author

Robin B. Chan, Tiago F. Outeiro, João A. Carriço, Paulo Gaspar, Tiago Soares, Raquel Bouça Machado, Roy N. Alcalay, Joaquim J. Ferreira, Yimeng Xu, Vasco A. Conceição, Gabriel Miltenberger-Miltenyi, Leonor Correia Guedes, and Marcos António Gomes

Subjects

Male, 0301 basic medicine, Ceramide, medicine.medical_specialty, Parkinson's disease, Plasmalogen, medicine.disease_cause, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, Humans, Medicine, Aged, Mutation, business.industry, Parkinson Disease, Middle Aged, medicine.disease, Lipids, LRRK2, Sphingolipid, nervous system diseases, 3. Good health, 030104 developmental biology, Endocrinology, Neurology, chemistry, Glucosylceramidase, Female, Neurology (clinical), Geriatrics and Gerontology, business, Sphingomyelin, Glucocerebrosidase, Biomarkers, 030217 neurology & neurosurgery

Abstract

Introduction Mutations in the GBA gene, encoding for the lysosomal enzyme glucocerebrosidase, are associated with Gaucher disease. Alterations in plasma sphingolipids have been reported in Gaucher, and similarly in brain extracts in Lewy body disease. As GBA mutations are prevalent risk factors for Parkinson's disease and overlap of molecular pathways are presumable, here we assessed the lipid profiles in Parkinson's patients with and without GBA mutations. Methods We sequenced all GBA exons in 415 Parkinson's patients, previously genotyped for LRRK2. 64 patients (29 GBA positive vs. 35 non-GBA-carriers including 18 LRRK2 positive and 17 non-mutated) were analyzed for chitotriosidase activity and for the concentration of 40 lipid classes using HPLC-MS. Results 29/415 patients (6.9%) carried 8 different GBA mutations associated with Gaucher or Parkinson's, including one novel mutation. Chitotriosidase activity was similar across the genetic groups, while the levels of key lipids were altered in GBA mutation carriers: Monohexosylceramide, Ceramide and Sphingomyelin were elevated; while Phosphatidic acid (PA), Phosphatidylethanolamine (PE), Plasmalogen phosphatidylethanolamine (PEp) and Acyl Phosphatidylglycerol (AcylPG) were decreased. Conclusion The results suggest an important role for these lipids in GBA mediated Parkinson's disease and assist in the identification of common pathways between Gaucher and Parkinson's. Ultimately, our findings may lead to the identification of novel biomarkers for individuals at increased risk of developing Parkinson's disease.

Published

2017

28. International Survey of ALS Experts about Critical Questions for Assessing Patients with ALS

Author

Magdalena Kuźma-Kozakiewicz, Julian Grosskreutz, Peter M. Andersen, Susanne Petri, Marta Gromicho, Mamede de Carvalho, Maria Piotrkiewicz, Gabriel Miltenberger Miltenyi, and Adam Ryczkowski

Subjects

medicine.medical_specialty, Internationality, Neurology, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Registries, 030212 general & internal medicine, Amyotrophic lateral sclerosis, Medical History Taking, 10. No inequality, Expert Testimony, 2. Zero hunger, Hierarchy, business.industry, Amyotrophic Lateral Sclerosis, International survey, medicine.disease, 3. Good health, Europe, Health Care Surveys, Family medicine, Physical therapy, Neurology (clinical), Symptom Assessment, business, 030217 neurology & neurosurgery

Abstract

To define an applicable dataset for ALS patient registries we weighted specific clinical items as scored by worldwide ALS experts.Sixty participants were invited based on relevant clinical work, publications and personal acquaintance. They rated 160 clinical items consensually agreed by the members of our project, incorporating specialists from five European Centres. Scoring scheme was defined as: 1 - essential; 2 - important; 3 - not very important. A mixed effect model was applied to rank items and to find possible correlations with geographical region (Europe vs. outside Europe).We received 40 responses, 20 from Europe and 20 from outside; 42/160 data were scored as essential by50% of the respondents, including: date of birth, gender, date of disease onset, date of diagnosis, ethnicity, region of onset, predominant upper neuron (UMN) or lower motor neuron (LMN) impairment, proximal versus distal weakness, respiratory symptoms, dysarthria, weight loss, signs of LMN/UMN involvement, emotional incontinence, cognitive changes, respiratory signs, neck weakness, body mass index, ALSFRS-R at entry, ALSFRS-R subscores at entry, timing and pattern of spreading and staging, electromyography, spirometry, MRI, CK level, riluzole intake, genetic background, history of physical exercise and previous and current main occupation. Four components were scored as non-relevant, including place of birth, blood pressure and pain at onset. There was no significant difference between regions (European vs. non-European countries).Our study identified a consensual set of clinical data with 42 specific items that can be used as a minimal data set for patient registers and for clinical trials.

Published

2017

29. Parkinson’s Disease and Fabry Disease: Clinical, Biochemical and Neuroimaging Analysis of Three Pedigrees

Author

Estela Bicho, Ana Teresa Vide, Nuno Sousa, Paulo Gaspar, Nuno Jorge Lamas, Tiago Gil Oliveira, Joaquim J. Ferreira, Miguel Gago, Andreia Guimarães, Gabriel Miltenberger-Miltenyi, Olga Azevedo, and Universidade do Minho

Subjects

Research Report, Male, 0301 basic medicine, Parkinson's disease, α-galactosidase A, Comorbidity, Disease, Gb3, Gastroenterology, Cohort Studies, 0302 clinical medicine, Leukocytes, Prevalence, Dopaminergic, Brain, Parkinson Disease, Middle Aged, Magnetic Resonance Imaging, humanities, Pedigree, 3. Good health, Phenotype, medicine.anatomical_structure, Female, medicine.drug, Adult, medicine.medical_specialty, Levodopa, Urinary system, Neuroimaging, White matter, Parkinson’s Disease, 03 medical and health sciences, Cellular and Molecular Neuroscience, Internal medicine, a-Galactosidase A, medicine, Humans, Alpha-galactosidase A, Aged, Brain magnetic resonance imaging, Sphingolipids, Fabry disease, Science & Technology, business.industry, Brain Magnetic Resonance Imaging, medicine.disease, Doenças Genéticas, 030104 developmental biology, alpha-Galactosidase, Concomitant, Parkinson’s disease, GLA, Fabry Disease, Neurology (clinical), Glycolipids, business, 030217 neurology & neurosurgery

Abstract

Background: Sporadic Parkinson's disease (PD) patients have lower a-galactosidase A (alpha-GAL A) enzymatic activity and Fabry disease (FD) patients potentially carry an increased risk of PD.Objective: Determination of PD prevalence in FD and clinical, biochemical and vascular neuroimaging description of FD pedigrees with concomitant PD.Methods: Clinical screening for PD in 229 FD patients belonging to 31 families, harbouring GLA gene mutation p.F113L, and subsequent pedigree analysis. Gender-stratified comparison of FD+/PD+ patients with their family members with FD but without PD (FD+/PD-) regarding Mainz scores, plasma & leukocytes alpha-GAL A enzymatic activity, urinary Gb3 and plasma Lyso-Gb3, vascular brain neuroimaging.Results: Prevalence of PD in FD was 1.3% (3/229) (3% in patients aged >= 50 years). Three FD patients, one female (73 years old) (P1) and two males (60 and 65 years old) (P2 and P3), three different pedigrees, presented akinetic-rigid PD, with weak response to levodopa (16%-36%), and dopaminergic deficiency on 18F-DOPA PET. No pathogenic mutations were found in a PD gene panel. FD+/PD+ patients had worse clinical severity of FD (above upper 75% IQR in Mainz scores), and cortico-subcortical white matter/small vessel lesions. P3 patient was under enzyme therapy, started 1 year before PD diagnosis. P2-P3 patients had higher leucocyte alpha-GAL A activity (2,2-3 vs.1,0 (median)(nmol/h/mg)).Conclusion: We have shown a high prevalence of PD in a late-onset phenotype of FD, presenting high cerebrovascular burden and weak response to levodopa. Further studies will untangle how much of this PD phenotype is due to Gb3 deposition versus cerebrovascular lesions in the nigro-striatal network., The authors are grateful for the clinical support provided by all colleagues working in the Reference Centre on Lysosomal Storage Disorders, and in the Neurology and Cardiology Departments, Hospital da Senhora da Oliveira, EPE, Guimaraes.

Published

2020

30. Increased monohexosylceramide levels in the serum of established rheumatoid arthritis patients

Author

Maria Fuller, João Eurico Fonseca, Ana Rita Cruz-Machado, Vasco A. Conceição, Inês P Lopes, Gabriel Miltenberger-Miltenyi, Ângelo Calado, Jennifer Saville, and Repositório da Universidade de Lisboa

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Ceramide, Arthritis, Ceramides, Gastroenterology, Arthritis, Rheumatoid, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Sex Factors, Rheumatology, Cerebrosides, Sphingosine, Internal medicine, Medicine, Synovial fluid, Humans, Pharmacology (medical), Rheumatoid arthritis, Aged, business.industry, Age Factors, Biomarker, Middle Aged, medicine.disease, Sphingolipid, Pathophysiology, 030104 developmental biology, chemistry, Lipidomics, Serum sphingolipid levels, Biomarker (medicine), Female, business, 030217 neurology & neurosurgery, Biomarkers

Abstract

© The Author(s) 2019. Published by Oxford University Press on behalf of the British Society for Rheumatology. All rights reserved. For permissions, please email: journals.permissions@oup.com, Objectives: To identify serum sphingolipids that could act as candidate biomarkers in RA. Methods: We performed lipidomic analyses in the serum of 82 participants: 19 established RA patients, 18 untreated early RA patients, 13 untreated early arthritis patients not fulfilling the classification criteria for RA, 12 established SpA patients and 20 controls. We compared the lipid levels from the different patient groups with the control group through multiple-regression analyses controlling for age at diagnosis, gender and medication (cDMARDs and corticoids). Results: Established RA patients had significantly increased levels of sphingosine, monohexosylceramide and ceramide compared with controls, when controlling for age and gender. Monohexosylceramide levels remained significantly increased when additionally controlling for medication. On the contrary, SpA patients had significantly decreased levels of ceramide, in both analyses. Conclusion: We observed a detectable increase in the levels of certain sphingolipids in the serum of established RA patients when compared with controls, in line with previous observations in the synovial fluid. Such findings provide further evidence that sphingolipids may play a key role in the pathophysiology of RA., This study was supported by a grant from thePortuguese Society of Rheumatology and by UID/BIM/50005/2019, a project funded by Fundação para a Ciência e a Tecnologia (FCT)/Ministério da Ciência,Tecnologia e Ensino Superior (MCTES) through Fundosdo Orçamento de Estado.

Published

2020

31. Predictors of Fabry disease in patients with hypertrophic cardiomyopathy: how to guide the diagnostic strategy?

Author

Rui Azevedo Guerreiro, Paulo Gaspar, Nuno Sousa, Carolina Lourenço, Gabriel Miltenberger-Miltenyi, N Craveiro, Olga Azevedo, Fernando Sá, Ricardo Faria, Rui Lima, Damião Cunha, Rui Faria, H Antunes, Renata Gomes, Liliana Reis, Inês Cruz, and Nuno Marques

Subjects

Adult, Male, medicine.medical_specialty, Cardiomyopathy, macromolecular substances, 030204 cardiovascular system & hematology, Bifascicular block, 03 medical and health sciences, Basal (phylogenetics), 0302 clinical medicine, Discriminant function analysis, Internal medicine, Medicine, Humans, In patient, cardiovascular diseases, 030212 general & internal medicine, Aged, Fabry disease, business.industry, Hypertrophic cardiomyopathy, Cardiomyopathy, Hypertrophic, Middle Aged, medicine.disease, Diagnostic strategy, 3. Good health, Pedigree, Hypertrophic, cardiovascular system, Cardiology, Etiology, Fabry Disease, Female, Cardiology and Cardiovascular Medicine, business

Abstract

Background Fabry disease (FD) is a treatable cause of hypertrophic cardiomyopathy (HCM). We aimed to determine the independent predictors of FD and to define a clinically useful strategy to discriminate FD among HCM. Methods Multicenter study including 780 patients with the ESC definition of HCM. FD screening was performed by enzymatic assay in males and genetic testing in females. Multivariate regression analysis identified independent predictors of FD in HCM. A discriminant function analysis defined a score based on the weighted combination of these predictors. Results FD was found in 37 of 780 patients with HCM (4.7%): 31 with p.F113L mutation due to a founder effect; and 6 with other variants (p.C94S; p.M96V; p.G183V; p.E203X; p.M290I; p.R356Q/p.G360R). FD prevalence in HCM adjusted for the founder effect was 0.9%. Symmetric HCM (OR 3.464, CI95% 1.151-10.430), basal inferolateral late gadolinium enhancement (LGE) (OR 10.677, CI95% 3.633-31.380), bifascicular block (OR 10.909, CI95% 2.377-50.059) and ST-segment depression (OR 4.401, CI95% 1.431-13.533) were independent predictors of FD in HCM. The score ID FABRY-HCM [−0.729 + (2.781xBifascicular block) + (0.590xST depression) + (0.831xSymmetric HCM) + (2.130xbasal inferolateral LGE)] had a negative predictive value of 95.8% for FD, with a cut-off of 1.0, meaning that, in the absence of both bifascicular block and basal inferolateral LGE, FD is a less probable cause of HCM, being more appropriate to perform HCM gene panel than targeted FD screening. Conclusion FD prevalence in HCM was 0.9%. Bifascicular block and basal inferolateral LGE were the most powerful predictors of FD in HCM. In their absence, HCM gene panel is the most appropriate step in etiological study of HCM.

Published

2020

32. p.G360R is a pathogenic GLA gene mutation responsible for a classic phenotype of Fabry disease

Author

J Guedes, R Fernandes, Daniela Marisa Carvalho Silva, Olga Azevedo, Hipólito Nzwalo, Ilídio de Jesus, D Bento, J Bispo, Pedro Azevedo, Ana Cabrita, Teresa Mota, Andre Aparecido Ramos, Nuno Marques, Gabriel Miltenberger-Miltenyi, and Universidade do Minho

Subjects

Male, Identification, Classic phenotype, Medicina Básica [Ciências Médicas], Mutation, Missense, Cardiovascular magnetic-resonance, 030204 cardiovascular system & hematology, Replacement therapy, Bioinformatics, medicine.disease_cause, Left ventricular hypertrophy, G360R, Fabry patient, 03 medical and health sciences, 0302 clinical medicine, Gla gene, medicine, Humans, Pharmacology (medical), Missense mutation, cardiovascular diseases, Stroke, GLA gene, Mutation, Fabry disease, Science & Technology, business.industry, Left-ventricular hypertrophy, Variants, Enzyme replacement therapy, Middle Aged, medicine.disease, Phenotype, p.G360R, 3. Good health, Alpha galactosidase, Echocardiography, alpha-Galactosidase, Ciências Médicas::Medicina Básica, Fabry Disease, Cardiology and Cardiovascular Medicine, business, 030217 neurology & neurosurgery

Abstract

The authors report the case of a classic phenotype of Fabry disease in a 60-year-old male patient presenting with left ventricular hypertrophy and stroke. Genetic analysis revealed 2 GLA-gene variants, i.e., p.R356Q and p.G360R. This clinical case highlights that the finding of 2 or more GLA gene variants in a Fabry patient should lead to a careful evaluation in order to determine their exact role in the condition. This case also provides the first clinical evidence that the p.G360R mutation is pathogenic and responsible for a classic phenotype of Fabry disease. The clinical improvement following the initiation of enzyme replacement therapy reinforces the importance of Fabry disease awareness and diagnosis in patients exhibiting red flags, such as left ventricular hypertrophy and stroke.

Published

2019

33. White matter hyperintensities in progranulin-associated frontotemporal dementia: A longitudinal GENFI study

Author

Rachelle Shafei, Albert Lladó, Benjamin Bender, Luisa Benussi, Elisabeth Wlasich, Martha S. Foiani, Isabel Santana, Christen Shoesmith, Ione O.C. Woollacott, Nick C. Fox, David L. Thomas, Jonathan D. Rohrer, Pietro Tiraboschi, Mario Masellis, Sergi Borrego-Écija, Giorgio G. Fumagalli, Ron Keren, Sandro Sorbi, Rick van Minkelen, Vesna Jelic, Ekaterina Rogaeva, Mollie Neason, Enrico Premi, Timothy Rittman, Lieke H.H. Meeter, Giacomina Rossi, Veronica Redaelli, Roberta Ghidoni, Begoña Indakoetxea, Johannes Levin, Håkan Thonberg, Rhian S Convery, Henrik Zetterberg, Gemma Lombardi, Giuseppe Di Fede, Chiara Fenoglio, Jose Bras, Daniela Galimberti, Simon Mead, Miren Zulaica, David M. Cash, Gabriel Miltenberger, Markus Otto, Simon Ducharme, Myriam Barandiaran, Katrina M. Moore, Alessandro Padovani, Thomas E. Cope, Elizabeth Finger, Maria Carmela Tartaglia, Martin N. Rossor, M. Jorge Cardoso, Sara Mitchell, Rik Vandenberghe, Pedro Rosa-Neto, John C. van Swieten, Sarah Anderl-Straub, Maria Rosário Almeida, Zigor Diaz, Robart Bartha, Maria de Arriba, Caroline V. Greaves, Philip Vandamme, Giorgio Giaccone, Adrian Danek, Miguel Tábuas-Pereira, Carolina Maruta, Roberto Gasparotti, Jennifer M. Nicholas, Martina Bocchetta, Elisa Semler, Valentina Bessi, C. Ferreira, Robert Laforce, Sandra V. Loosli, Ana Verdelho, Paola Caroppo, Jaume Olives, Giuliano Binetti, Carolin Heller, Jorge Villanua, Stefano Gazzina, Amanda Heslegrave, Alazne Gabilondo, Sandra E. Black, Y.A.L. Pijnenburg, Mikel Tainta, Carolyn Timberlake, Sónia Afonso, Matthis Synofzik, Janne M. Papma, Sebastien Ourselin, Núria Bargalló, Barbara Borroni, Ricardo Taipa, Hans-Otto Karnarth, Camilla Ferrari, David F. Tang-Wai, Diana Duro, Catharina Prix, Serge Gauthier, Sara Prioni, Carlo Wilke, Michele Veldsman, Alexandre de Mendonça, Andrea Arighi, Christopher C Butler, Raquel Sánchez-Valle, Toby Flanagan, Carole H. Sudre, Jason D. Warren, Rita Guerreiro, Linn Öijerstedt, Beatriz Santiago, Rosa Rademakers, Miguel Castelo-Branco, Fabrizio Tagliavini, Maria João Leitão, Anna Antonell, Mathieu Vandenbulcke, Rose Bruffaerts, Jessica L. Panman, Alexander Gerhard, Tobias Hoegen, Ana Gorostidi, Silvana Archetti, James B. Rowe, Michela Pievani, Elio Scarpini, Giovanni B. Frisoni, Benedetta Nacmias, Sonja Schönecker, Maura Cosseddu, Christin Andersson, Caroline Graff, Morris Freedman, Fermin Moreno, Mircea Balasa, Lize C. Jiskoot, Sudre, Carole H [0000-0001-5753-428X], Apollo - University of Cambridge Repository, Rowe, James [0000-0001-7216-8679], and Neurology

Subjects

Oncology, Male, SEGMENTATION, PROTEIN, physiopathology [Frontotemporal Dementia], DISEASE, 0302 clinical medicine, White matter hyperintensities, blood [Glial Fibrillary Acidic Protein], Longitudinal Studies, education.field_of_study, Regular Article, Neurology, Frontotemporal Dementia, Disease Progression, GRN, medicine.medical_specialty, lcsh:Computer applications to medicine. Medical informatics, MRI, Magnetic Resonance Imaging, White matter, 03 medical and health sciences, AGE, Humans, neurofilament protein L, education, Aged, CSF, Cerebrospinal fluid, Science & Technology, Trail Making Test, Frontotemporal dementia, Dementia, Progranulin, medicine.disease, POLYMORPHISM, Case-Control Studies, Asymptomatic Diseases, Mutation, Neurosciences & Neurology, Neurology (clinical), GENFI, 030217 neurology & neurosurgery, Executive dysfunction, blood [Frontotemporal Dementia], GFAP, Glial Fibrillary Acidic Protein, blood [Neurofilament Proteins], lcsh:RC346-429, genetics [Progranulins], Executive Function, Progranulins, pathology [Gray Matter], Neurofilament Proteins, BRAIN ATROPHY, GM, Grey Matter, Gray Matter, genetics [Frontotemporal Dementia], genetics [Nerve Tissue Proteins], 05 social sciences, Organ Size, Middle Aged, Magnetic Resonance Imaging, White Matter, genetics [Membrane Proteins], medicine.anatomical_structure, FTD, Frontotemporal dementia, GENFI, GENetic Frontotemporal dementia Initiative, lcsh:R858-859.7, Female, Life Sciences & Biomedicine, Adult, Heterozygote, Cognitive Neuroscience, Population, Prodromal Symptoms, Neuroimaging, PHENOTYPES, Nerve Tissue Proteins, MUTATION CARRIERS, WM, White Matter, Grey matter, diagnostic imaging [Frontotemporal Dementia], 050105 experimental psychology, diagnostic imaging [White Matter], Atrophy, TMEM106B protein, human, Internal medicine, mental disorders, Glial Fibrillary Acidic Protein, medicine, 0501 psychology and cognitive sciences, Radiology, Nuclear Medicine and imaging, ddc:610, lcsh:Neurology. Diseases of the nervous system, business.industry, GFAP protein, human, WMH, White Matter Hyperintensity, diagnostic imaging [Gray Matter], Membrane Proteins, Hyperintensity, GRN, Progranulin, TMEM106B, ddc:618.97, GRN protein, human, business

Abstract

Frontotemporal dementia (FTD) is a heterogeneous group of neurodegenerative disorders with both sporadic and genetic forms. Mutations in the progranulin gene (GRN) are a common cause of genetic FTD, causing either a behavioural presentation or, less commonly, language impairment. Presence on T2-weighted images of white matter hyperintensities (WMH) has been previously shown to be more commonly associated with GRN mutations rather than other forms of FTD. The aim of the current study was to investigate the longitudinal change in WMH and the associations of WMH burden with grey matter (GM) loss, markers of neurodegeneration and cognitive function in GRN mutation carriers. 336 participants in the Genetic FTD Initiative (GENFI) study were included in the analysis: 101 presymptomatic and 32 symptomatic GRN mutation carriers, as well as 203 mutation-negative controls. 39 presymptomatic and 12 symptomatic carriers, and 73 controls also had longitudinal data available. Participants underwent MR imaging acquisition including isotropic 1 mm T1-weighted and T2-weighted sequences. WMH were automatically segmented and locally subdivided to enable a more detailed representation of the pathology distribution. Log-transformed WMH volumes were investigated in terms of their global and regional associations with imaging measures (grey matter volumes), biomarker concentrations (plasma neurofilament light chain, NfL, and glial fibrillary acidic protein, GFAP), genetic status (TMEM106B risk genotype) and cognition (tests of executive function). Analyses revealed that WMH load was higher in both symptomatic and presymptomatic groups compared with controls and this load increased over time. In particular, lesions were seen periventricularly in frontal and occipital lobes, progressing to medial layers over time. However, there was variability in the WMH load across GRN mutation carriers - in the symptomatic group 25.0% had none/mild load, 37.5% had medium and 37.5% had a severe load - a difference not fully explained by disease duration. GM atrophy was strongly associated with WMH load both globally and in separate lobes, and increased WMH burden in the frontal, periventricular and medial regions was associated with worse executive function. Furthermore, plasma NfL and to a lesser extent GFAP concentrations were seen to be associated with increased lesion burden. Lastly, the presence of the homozygous TMEM106B rs1990622 TT risk genotypic status was associated with an increased accrual of WMH per year. In summary, WMH occur in GRN mutation carriers and accumulate over time, but are variable in their severity. They are associated with increased GM atrophy and executive dysfunction. Furthermore, their presence is associated with markers of WM damage (NfL) and astrocytosis (GFAP), whilst their accrual is modified by TMEM106B genetic status. WMH load may represent a target marker for trials of disease modifying therapies in individual patients but the variability across the GRN population would prevent use of such markers as a global outcome measure across all participants in a trial. ispartof: NEUROIMAGE-CLINICAL vol:24 ispartof: location:Netherlands status: published

Published

2019

34. Fabry Disease and the Heart: A Comprehensive Review

Author

Damião Cunha, Filipa Cordeiro, Gabriel Miltenberger-Miltenyi, Catarina Ferreira, Nuno Sousa, Olga Azevedo, Miguel Gago, and Universidade do Minho

Subjects

0301 basic medicine, Cardiomyopathy, Review, 030204 cardiovascular system & hematology, 0302 clinical medicine, Migalastat, Biology (General), Spectroscopy, Cardiac imaging, Heart, General Medicine, Enzyme replacement therapy, 3. Good health, Computer Science Applications, Chemistry, cardiovascular system, Cardiology, Electrical conduction system of the heart, enzyme replacement therapy, medicine.medical_specialty, QH301-705.5, migalastat, heart, Sudden death, Catalysis, Inorganic Chemistry, 03 medical and health sciences, Internal medicine, medicine, Animals, Humans, Physical and Theoretical Chemistry, QD1-999, Molecular Biology, Fabry disease, Science & Technology, business.industry, Organic Chemistry, Arrhythmias, Cardiac, medicine.disease, 030104 developmental biology, alpha-Galactosidase, Heart failure, business, cardiomyopathy

Abstract

Fabry disease (FD) is an X-linked lysosomal storage disorder caused by mutations of the GLA gene that result in a deficiency of the enzymatic activity of α-galactosidase A and consequent accumulation of glycosphingolipids in body fluids and lysosomes of the cells throughout the body. GB3 accumulation occurs in virtually all cardiac cells (cardiomyocytes, conduction system cells, fibroblasts, and endothelial and smooth muscle vascular cells), ultimately leading to ventricular hypertrophy and fibrosis, heart failure, valve disease, angina, dysrhythmias, cardiac conduction abnormalities, and sudden death. Despite available therapies and supportive treatment, cardiac involvement carries a major prognostic impact, representing the main cause of death in FD. In the last years, knowledge has substantially evolved on the pathophysiological mechanisms leading to cardiac damage, the natural history of cardiac manifestations, the late-onset phenotypes with predominant cardiac involvement, the early markers of cardiac damage, the role of multimodality cardiac imaging on the diagnosis, management and follow-up of Fabry patients, and the cardiac efficacy of available therapies. Herein, we provide a comprehensive and integrated review on the cardiac involvement of FD, at the pathophysiological, anatomopathological, laboratory, imaging, and clinical levels, as well as on the diagnosis and management of cardiac manifestations, their supportive treatment, and the cardiac efficacy of specific therapies, such as enzyme replacement therapy and migalastat.

Published

2021

35. Mild Left Ventricular Hypertrophy Unravels a Novel Nonsense Mutation of the GLA Gene Associated with the Classical Phenotype of Fabry Disease

Author

Damião Cunha, Paulo Gaspar, Olga Azevedo, Miguel Gago, Nuno Sousa, and Gabriel Miltenberger-Miltenyi

Subjects

0301 basic medicine, medicine.medical_specialty, media_common.quotation_subject, Nonsense, Nonsense mutation, 030204 cardiovascular system & hematology, 030105 genetics & heredity, Left ventricular hypertrophy, 03 medical and health sciences, 0302 clinical medicine, Gla gene, Internal medicine, medicine, Pharmacology (medical), cardiovascular diseases, media_common, Genetics, business.industry, medicine.disease, Fabry disease, Phenotype, 3. Good health, Endocrinology, Mutation (genetic algorithm), Cardiology and Cardiovascular Medicine, business

Abstract

We report on the clinical, biochemical, and genetic findings of a large family with the classical phenotype of Fabry disease due to the novel nonsense mutation c.607G>T (p.E203X) of the GLA gene, which occurs in the active site of the α-galactosidase A enzyme. This report highlights that (i) Fabry disease diagnosis should be considered in all cases of unexplained left ventricular hypertrophy (LVH), even in its milder forms; (ii) a complete evaluation of patients with unexplained LVH is important to find diagnostic red flags of treatable causes of LVH, such as Fabry disease; (iii) cascade family screening is paramount to the earlier diagnosis and treatment of other affected family members; and (iv) the Fabry disease phenotype is highly variable in heterozygote females, even within the same family.

Published

2017

36. Referee report. For: The C9orf72 expansion is associated with accelerated respiratory function decline in a large Amyotrophic Lateral Sclerosis cohort [version 1; peer review: 1 approved]

Author

Mamede De Carvalho and Miltényi, Gabriel Miltenberger

Published

2019

37. Serum neurofilament light chain in genetic frontotemporal dementia: a longitudinal, multicentre cohort study

Author

Emma L van der Ende, Lieke H Meeter, Jackie M Poos, Jessica L Panman, Lize C Jiskoot, Elise G P Dopper, Janne M Papma, Frank Jan de Jong, Inge M W Verberk, Charlotte Teunissen, Dimitris Rizopoulos, Carolin Heller, Rhian S Convery, Katrina M Moore, Martina Bocchetta, Mollie Neason, David M Cash, Barbara Borroni, Daniela Galimberti, Raquel Sanchez-Valle, Robert Laforce, Fermin Moreno, Matthis Synofzik, Caroline Graff, Mario Masellis, Maria Carmela Tartaglia, James B Rowe, Rik Vandenberghe, Elizabeth Finger, Fabrizio Tagliavini, Alexandre de Mendonça, Isabel Santana, Chris Butler, Simon Ducharme, Alex Gerhard, Adrian Danek, Johannes Levin, Markus Otto, Giovanni B Frisoni, Stefano Cappa, Yolande A L Pijnenburg, Jonathan D Rohrer, John C van Swieten, Martin N. Rossor, Jason D. Warren, Nick C. Fox, Ione O.C. Woollacott, Rachelle Shafei, Caroline Greaves, Rita Guerreiro, Jose Bras, David L. Thomas, Jennifer Nicholas, Simon Mead, Rick van Minkelen, Myriam Barandiaran, Begoña Indakoetxea, Alazne Gabilondo, Mikel Tainta, Maria de Arriba, Ana Gorostidi, Miren Zulaica, Jorge Villanua, Zigor Diaz, Sergi Borrego-Ecija, Jaume Olives, Albert Lladó, Mircea Balasa, Anna Antonell, Nuria Bargallo, Enrico Premi, Maura Cosseddu, Stefano Gazzina, Alessandro Padovani, Roberto Gasparotti, Silvana Archetti, Sandra Black, Sara Mitchell, Ekaterina Rogaeva, Morris Freedman, Ron Keren, David Tang-Wai, Linn Öijerstedt, Christin Andersson, Vesna Jelic, Hakan Thonberg, Andrea Arighi, Chiara Fenoglio, Elio Scarpini, Giorgio Fumagalli, Thomas Cope, Carolyn Timberlake, Timothy Rittman, Christen Shoesmith, Robart Bartha, Rosa Rademakers, Carlo Wilke, Hans-Otto Karnath, Benjamin Bender, Rose Bruffaerts, Philip Vandamme, Mathieu Vandenbulcke, Catarina B. Ferreira, Gabriel Miltenberger, Carolina Maruta, Ana Verdelho, Sónia Afonso, Ricardo Taipa, Paola Caroppo, Giuseppe Di Fede, Giorgio Giaccone, Sara Prioni, Veronica Redaelli, Giacomina Rossi, Pietro Tiraboschi, Diana Duro, Maria Rosario Almeida, Miguel Castelo-Branco, Maria João Leitão, Miguel Tabuas-Pereira, Beatriz Santiago, Serge Gauthier, Sonja Schonecker, Elisa Semler, Sarah Anderl-Straub, Luisa Benussi, Giuliano Binetti, Roberta Ghidoni, Michela Pievani, Gemma Lombardi, Benedetta Nacmias, Camilla Ferrari, Valentina Bessi, Rowe, James [0000-0001-7216-8679], Apollo - University of Cambridge Repository, Neurology, Amsterdam Reproduction & Development (AR&D), Pediatric surgery, Laboratory Medicine, Amsterdam Neuroscience - Neurodegeneration, Divisions, and Epidemiology

Subjects

0301 basic medicine, Adult, blood [Frontotemporal Dementia], Male, medicine.medical_specialty, Neurofilament light, C9orf72 Protein/genetics, blood [Neurofilament Proteins], diagnostic imaging [Frontotemporal Dementia], Cohort Studies, 03 medical and health sciences, Neurofilament Proteins/blood/genetics, 0302 clinical medicine, Atrophy, C9orf72, Neurofilament Proteins, Aged, Biomarkers, C9orf72 Protein, Female, Frontotemporal Dementia, Humans, Longitudinal Studies, Middle Aged, Internal medicine, medicine, Frontotemporal Dementia/blood/diagnostic imaging/genetics, ddc:610, genetics [C9orf72 Protein], genetics [Frontotemporal Dementia], blood [Biomarkers], business.industry, Neuropsychology, medicine.disease, genetics [Neurofilament Proteins], 030104 developmental biology, ddc:618.97, Biomarker (medicine), Neurology (clinical), business, 030217 neurology & neurosurgery, Biomarkers/blood, Cohort study, Frontotemporal dementia

Abstract

BACKGROUND: Neurofilament light chain (NfL) is a promising blood biomarker in genetic frontotemporal dementia, with elevated concentrations in symptomatic carriers of mutations in GRN, C9orf72, and MAPT. A better understanding of NfL dynamics is essential for upcoming therapeutic trials. We aimed to study longitudinal NfL trajectories in people with presymptomatic and symptomatic genetic frontotemporal dementia.METHODS: We recruited participants from 14 centres collaborating in the Genetic Frontotemporal Dementia Initiative (GENFI), which is a multicentre cohort study of families with genetic frontotemporal dementia done across Europe and Canada. Eligible participants (aged ≥18 years) either had frontotemporal dementia due to a pathogenic mutation in GRN, C9orf72, or MAPT (symptomatic mutation carriers) or were healthy at-risk first-degree relatives (either presymptomatic mutation carriers or non-carriers), and had at least two serum samples with a time interval of 6 months or more. Participants were excluded if they had neurological comorbidities that were likely to affect NfL, including cerebrovascular events. We measured NfL longitudinally in serum samples collected between June 8, 2012, and Dec 8, 2017, through follow-up visits annually or every 2 years, which also included MRI and neuropsychological assessments. Using mixed-effects models, we analysed NfL changes over time and correlated them with longitudinal imaging and clinical parameters, controlling for age, sex, and study site. The primary outcome was the course of NfL over time in the various stages of genetic frontotemporal dementia.FINDINGS: We included 59 symptomatic carriers and 149 presymptomatic carriers of a mutation in GRN, C9orf72, or MAPT, and 127 non-carriers. Nine presymptomatic carriers became symptomatic during follow-up (so-called converters). Baseline NfL was elevated in symptomatic carriers (median 52 pg/mL [IQR 24-69]) compared with presymptomatic carriers (9 pg/mL [6-13]; pINTERPRETATION: Our findings show the value of blood NfL as a disease progression biomarker in genetic frontotemporal dementia and suggest that longitudinal NfL measurements could identify mutation carriers approaching symptom onset and capture rates of brain atrophy. The characterisation of NfL over the course of disease provides valuable information for its use as a treatment effect marker.FUNDING: ZonMw and the Bluefield project.

Published

2019

38. Screening for Fabry disease in patients with left ventricular noncompaction

Author

Damião Cunha, H Antunes, Gabriel Miltenberger-Miltenyi, Olga Azevedo, Rui Azevedo Guerreiro, Rui Pontes dos Santos, N Craveiro, Liliana Reis, Nuno Marques, Nuno Sousa, and Ana Rita Pereira

Subjects

Adult, Male, lcsh:Diseases of the circulatory (Cardiovascular) system, medicine.medical_specialty, Cardiomyopathy, Hypertrabeculation, 030204 cardiovascular system & hematology, 03 medical and health sciences, Electrocardiography, Ventricular Dysfunction, Left, 0302 clinical medicine, Internal medicine, medicine, Humans, 030212 general & internal medicine, Overdiagnosis, Noncompaction, Genetic testing, General Environmental Science, Aged, Retrospective Studies, Heart Failure, Fabry disease, Isolated Noncompaction of the Ventricular Myocardium, medicine.diagnostic_test, business.industry, Retrospective cohort study, Middle Aged, medicine.disease, Magnetic Resonance Imaging, Chin, 3. Good health, medicine.anatomical_structure, 030228 respiratory system, lcsh:RC666-701, Heart failure, Cardiology, Screening, Left ventricular noncompaction, General Earth and Planetary Sciences, Fabry Disease, Female, Cardiology and Cardiovascular Medicine, business, 030217 neurology & neurosurgery

Abstract

Introduction and Aim: It is unclear whether left ventricular noncompaction (LVNC) is a distinct cardiomyopathy or a morphologic manifestation of different cardiomyopathies. We previously reported a case of LVNC in a Fabry disease (FD) patient, but it remains to be clarified whether LVNC is a cardiac manifestation of FD, a coincidental finding or an overdiagnosis, which has major therapeutic implications. This study aims to determine the prevalence of FD among patients with LVNC. Methods: We performed a retrospective study including all patients diagnosed with LVNC in eight hospital centers. Diagnosis of LVNC was based on at least one echocardiographic or cardiac magnetic resonance criterion. FD screening was performed by combined enzyme and genetic testing. Results: The study included 78 patients diagnosed with LVNC based on the Jenni (84.6%), Stöllberger (46.2%), Chin (21.8%), Petersen (83.8%) and Jacquier (16.2%) criteria. Left ventricular systolic dysfunction was present in 48.7%. Heart failure was found in 60.3%, ventricular dysrhythmias in 21.6% and embolic events in 11.5%. FD screening found no additional cases among patients with LVNC, besides the previously described case. Conclusion: No additional FD cases were found among patients with LVNC, which argues against the hypothesis that LVNC is a cardiac manifestation of FD. Resumo: Introdução e objetivo: Não está esclarecido se a não compactação do ventrículo esquerdo (NCVE) é uma miocardiopatia distinta ou uma manifestação morfológica de várias miocardiopatias. Nós reportamos previamente um caso de NCVE num doente com doença de Fabry (DF), mas permanece por esclarecer se a NCVE é uma manifestação cardíaca de DF, um achado coincidente ou um sobrediagnóstico, o que tem importantes implicações terapêuticas. Este estudo pretende determinar a prevalência de DF em doentes com NCVE. Métodos: Estudo retrospetivo incluindo todos os doentes diagnosticados com NCVE em oito centros hospitalares. O diagnóstico de NCVE foi baseado em pelo menos um dos critérios de ecocardiografia ou ressonância cardíaca. O rastreio de DF foi realizado por teste enzimático e genético. Resultados: O estudo incluiu 78 doentes diagnosticados com NCVE com base nos critérios de Jenni (84,6%), Stöllberger (46,2%), Chin (21,8%), Petersen (83,8%) e Jacquier (16,2%). A disfunção sistólica do VE estava presente em 48,7%. A insuficiência cardíaca foi encontrada em 60,3%, as disritmias ventriculares em 21,6% e os eventos embólicos em 11,5%. O rastreio de DF não encontrou casos adicionais nos doentes com NCVE, para além do caso previamente descrito. Conclusão: Não foram encontrados casos adicionais de DF nos doentes com NCVE, o que argumenta contra a hipótese de a NCVE ser uma manifestação cardíaca de DF. Keywords: Fabry disease, Noncompaction, Hypertrabeculation, Cardiomyopathy, Screening, Palavras-chave: Doença de Fabry, Não compactação, Hipertrabeculação, Cardiomiopatia, Rastreio

Published

2018

39. No supportive evidence for TIA1 gene mutations in a European cohort of ALS-FTD spectrum patients

Author

Ellen Gelpi, Mathieu Vandenbulcke, Yalda Baradaran-Heravi, Alex Michotte, Alexandre de Mendonça, Elisa Bonomi, Peter Paul De Deyn, Peter Heutink, Bruno Bergmans, Matthew J. Fraidakis, Matthis Synofzik, Dirk Peeters, Eva Parobkova, Christine Van Broeckhoven, Patrick Santens, Peter De Jonghe, Radoslav Matej, Maria Rosário Almeida, Rik Vandenberghe, Hung Phuoc Nguyen, Pau Pastor, Alessandro Padovani, Gabriel Miltenberger-Miltenyi, Jan De Bleecker, Philip Van Damme, Sara Van Mossevelde, Isabel Santana, Ricard Rojas-García, Olivier Deryck, Julie van der Zee, Eric Salmon, Ana Verdelho, Christiana Willems, Nina De Klippel, Miquel Aguilar, Lubina Dillen, Alberto Lleó, Sergi Borrego-Écija, Sebastiaan Engelborghs, Sandro Sorbi, Jonathan Baets, Camilla Ferrari, Monica Diez-Fairen, Silvia Bagnoli, Barbara Borroni, Raquel Sánchez-Valle, Johan Goeman, Anne Sieben, Ignacio Illán-Gala, Patrick Cras, Panagiotis Alexopoulos, Janina Turon-Sans, Benedetta Nacmias, Adrian Ivanoiu, Irene Piaceri, Janine Diehl-Schmid, Jan Versijpt, Silvana Archettim, C. Ferreira, Frederico Simões do Couto, Jordi Clarimón, Dirk Nuytten, Javier Simón-Sánchez, Carlo Wilke, UCL - SSS/IONS/NEUR - Clinical Neuroscience, UCL - (SLuc) Service de neurologie, BELNEU Consortium1, EU EOD Consortium, Clinical sciences, Neurology, and Pathologic Biochemistry and Physiology

Subjects

0301 basic medicine, Oncology, Male, Aging, Geriatrics & Gerontology, Gene mutation, Frontotemporal dementia (FTD), AMYOTROPHIC-LATERAL-SCLEROSIS, Pathogenesis, Cohort Studies, 0302 clinical medicine, Gene Frequency, Medicine and Health Sciences, Missense mutation, Amyotrophic lateral sclerosis (ALS), Amyotrophic lateral sclerosis, genetics [Frontotemporal Dementia], Medicine(all), General Neuroscience, ddc, genetics [Amyotrophic Lateral Sclerosis], genetics [European Continental Ancestry Group], Frontotemporal Dementia, Cohort, T cellerestricted intracellular antigen-1 gene (TIA1), Female, Life Sciences & Biomedicine, Cohort study, Frontotemporal dementia, medicine.medical_specialty, European Continental Ancestry Group, genetics [White People], Mutation, Missense, White People, 03 medical and health sciences, Internal medicine, mental disorders, medicine, Humans, ddc:610, genetics [T-Cell Intracellular Antigen-1], Biology, Allele frequency, T cell–restricted intracellular antigen-1 gene (TIA1), Science & Technology, business.industry, TIA1 protein, human, Amyotrophic Lateral Sclerosis, Neurosciences, TAR DNA-Binding protein 43 (TDP-43), FRONTOTEMPORAL DEMENTIA, medicine.disease, T-Cell Intracellular Antigen-1, 030104 developmental biology, Human medicine, Neurology (clinical), Neurosciences & Neurology, Geriatrics and Gerontology, business, 030217 neurology & neurosurgery, Developmental Biology

Abstract

We evaluated the genetic contribution of the T cell-restricted intracellular antigen-1 gene (TIA1) in a European cohort of frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS) patients. Exonic resequencing of TIA1 in 1120 patients (693 FTD, 341 ALS, 86 FTD-ALS) and 1039 controls identified in total 5 rare heterozygous missense variants, affecting the TIA1 low-complexity domain (LCD). Only 1 missense variant, p.Met290Thr, identified in a familial FTD patient with disease onset at 64 years, was absent from controls yet received a combined annotation-dependent depletion score of 11.42. By contrast, 3 of the 4 variants also detected in unaffected controls, p.Val294Glu, p.Gln318Arg, and p.Ala381Thr, had combined annotation-dependent depletion scores greater than 20. Our findings in a large European patient-control series indicate that variants in TIA1 are not a common cause of ALS and FTD. The observation of recurring TIA1 missense variants in unaffected individuals lead us to conclude that the exact genetic contribution of TIA1 to ALS and FTD pathogenesis remains to be further elucidated. ispartof: NEUROBIOLOGY OF AGING vol:69 ispartof: location:United States status: published

Published

2018

40. The Project MinE databrowser: bringing large-scale whole-genome sequencing in ALS to researchers and the public

Author

Gijs H.P. Tazelaar, Yolanda Campos, Pamela J. Shaw, Rick A.A. van der Spek, Ammar Al-Chalabi, Ian R. A. Mackenzie, John Landers, Mónica Povedano Panades, Ceren Tunca, Johnathan Cooper-Knock, Karen E. Morrison, Orla Hardiman, Janez Zidar, Vivian E. Drory, Atay Vural, Vera Fominyh, Kristel R. van Eijk, Raymond D. Schellevis, Ahmad Al Khleifat, Phillipe Corcia, Ersen Kavak, Stephan Newhouse, Mamede de Carvalho, Kevin P. Kenna, Sara L. Pulit, William J. Brands, Nazli Basak, Marc Gotkine, Gabriel Miltenberger-Miltenyi, Matthieu Moisse, Jesus S. Mora, Annelot M. Dekker, Joke J.F.A. van Vugt, Boris Rogelj, Philip Van Damme, Wim Robberecht, Ervina Bilić, Maarten Kooyman, William Sproviero, Nicolas Dupré, Blaz Koritnik, Tuncay Seker, Leonard H. van den Berg, Jan H. Veldink, Ross P. Byrne, Brendan J. Kenna, Naomi R. Wray, P. Couratier, Perry T.C. van Doormaal, Jonathan D. Glass, Johnathan Mill, Russell L. McLaughlin, Bas Middelkoop, Lev Brylev, Alberto Garcia Redondo, Nicola Ticozzi, Markus Weber, Wouter van Rheenen, Mayana Zatz, Christopher Shaw, Cemile Kocoglu, Ivana Munitic, Ekaterina Rogaeva, Miguel Mitne-Neto, Peter M. Andersen, Vincenzo Silani, Michael A. van Es, Fulya Akçimen, Aleksey Shatunov, Matthew C. Kiernan, Ian P. Blair, Guy A. Rouleau, Adriano Chiò, Alfredo Iacoangeli, and Victoria Lopez Alonso

Subjects

Whole genome sequencing, Resource (project management), Computer science, Project MinE, Scale (social sciences), Genetic variation, Genomics, Biostatistics, Set (psychology), Data science

Abstract

Amyotrophic lateral sclerosis (ALS) is a rapidly progressive fatal neurodegenerative disease affecting 1 in 350 people. The aim of Project MinE is to elucidate the pathophysiology of ALS through whole-genome sequencing at least 15,000 ALS patients and 7,500 controls at 30X coverage. Here, we present the Project MinE data browser (databrowser.projectmine.com). a unique and intuitive one-stop, open-access server that provides detailed information on genetic variation analyzed in a new and still growing set of 4,366 ALS cases and 1,832 matched controls. Through its visual components and interactive design, the browser specifically aims to be a resource to those without a biostatistics background and allow clinicians and preclinical researchers to integrate Project MinE data into their own research. The browser allows users to query a transcript and immediately access a unique combination of detailed (meta)data, annotations and association statistics that would otherwise require analytic expertise and visits to scattered resources.

Published

2018

41. Rare nonsynonymous variants in SORT1 are associated with increased risk for frontotemporal dementia

Author

Albert Lladó, Jordi Clarimón, Barbara Borroni, Roberta Ghidoni, Rik Vandenberghe, Giovanni B. Frisoni, Isabel Santana, Alberto Lleó, Sara Van Mossevelde, Christiana Willems, Benedetta Nacmias, Mathieu Vandenbulcke, Mercè Boada, Adrian Ivanoiu, Giuliano Binetti, Maria Rosário Almeida, Peter Paul De Deyn, Marc Cruts, Monica Diez-Fairen, Miquel Aguilar, Anne Sieben, Marleen Van den Broeck, Gabriel Miltenberger-Miltenyi, Eline Wauters, Christine Van Broeckhoven, Patrick Cras, Raquel Sánchez-Valle, Estrella Gómez-Tortosa, Sandro Sorbi, Isabel Hernández, Ellen Gelpi, Agustín Ruiz, Julie van der Zee, Lubina Dillen, Alexandre de Mendonça, Luisa Benussi, Karin Peeters, Sebastiaan Engelborghs, Alessandro Padovani, Pau Pastor, Stéphanie Philtjens, Frisoni, Giovanni, Repositório da Universidade de Lisboa, BELNEU Consortium, EU EOD Consortium, Physiotherapy, Human Physiology and Anatomy, Clinical sciences, Neurology, and Pathologic Biochemistry and Physiology

Subjects

0301 basic medicine, Nonsynonymous substitution, Male, Aging, Geriatrics & Gerontology, Granulin, AMYOTROPHIC-LATERAL-SCLEROSIS, Cohort Studies, 0302 clinical medicine, Progranulins, Belgium, Medicine(all), Genetics, PLASMA, General Neuroscience, Adaptor Proteins, Vesicular Transport/chemistry, Middle Aged, Europe, Genetic Variation/genetics, Intercellular Signaling Peptides and Proteins, Female, Frontotemporal dementia, Genetic association, Rare variants, Sortilin, Life Sciences & Biomedicine, Cohort study, Protein Binding, Risk, Neuroscience(all), DIAGNOSTIC-CRITERIA, Clinical Neurology, PROGRANULIN LEVELS, C9ORF72, Biology, 03 medical and health sciences, Protein Domains, Genetic variation, mental disorders, medicine, Dementia, Humans, BELGIAN COHORT, Adaptor Proteins, Vesicular Transport/chemistry/genetics, LOBAR DEGENERATION, Gene, Genetic Association Studies, Aged, Science & Technology, HEXANUCLEOTIDE REPEAT, Binding Sites, MUTATIONS, Neurosciences, Genetic Variation, medicine.disease, Ageing, Adaptor Proteins, Vesicular Transport, 030104 developmental biology, ddc:618.97, Human medicine, Neurology (clinical), Neurosciences & Neurology, Geriatrics and Gerontology, 030217 neurology & neurosurgery, Developmental Biology

Abstract

© 2018 The Authors. Published by Elsevier Inc. This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/), We investigated the genetic role of sortilin (SORT1) in frontotemporal dementia (FTD). SORT1 is the neuronal receptor for granulin, encoded by the progranulin gene (GRN), a major causal gene for inherited FTD. In Belgian cohorts of 636 FTD patients and 1066 unaffected control individuals, we identified 5 patient-only nonsynonymous rare variants in SORT1. Rare variant burden analysis showed a significant increase in rare coding variants in patients compared to control individuals (p = 0.04), particularly in the β-propeller domain (p = 0.04), with 2 rare variants located in the predicted binding site for GRN (p = 0.001). We extended these observations by analyzing 3 independent patient/control cohorts sampled in Spain, Italy, and Portugal by partners of the European Early-Onset Dementia Consortium, together with 1155 FTD patients and 1161 control persons. An additional 7 patient-only nonsynonymous variants were observed in SORT1 in European patients. Meta-analysis of the rare nonsynonymous variants in the Belgian and European patient/control cohorts revealed a significant enrichment in FTD patients (p = 0.006), establishing SORT1 as a genetic risk factor for FTD., The research was funded in part by the Belgian Science Policy Office Interuniversity Attraction Poles program; the Flemish government initiated Methusalem excellence program and Impulse Program on Networks for Dementia Research; the Research Foundation Flanders (FWO), the Agency for Innovation by Science and Technology Flanders (IWT) and the University of Antwerp Research Fund; Belgium. SP received a PhD fellowship of the FWO and EW of the IWT. RG, LB, and GB (IRCCS Fatebenefratelli, Brescia, Italy) were supported by Ricerca Corrente, Italian Ministry of Health.

Published

2018

42. Soft Tissue Metastasis of Parathyroid Carcinoma: Description of a Difficult Case

Author

Ana Filipa Martins, Joao Martin Martins, Sonia do Vale, Cristopher Juhlin, Lucas Batista, Marco Franco, Dolores Lopez-Presa, and Gabriel Miltenberger-Miltenyi

Subjects

Endocrinology, Diabetes and Metabolism

Published

2015

43. Post mortem genetic test, the clinical diagnosis is not fade with the death of the patient

Author

Sílvia, Ribeiro, Luís, Coelho, Katerina, Puentes, Gabriel, Miltenberger-Miltenyi, Bebiana, Faria, Lucy, Calvo, João, Primo, Víctor, Sanfins, and António, Lourenço

Subjects

Adult, Male, Death, Sudden, Cardiac, Fatal Outcome, Adolescent, Humans, Female, Autopsy, Genetic Testing, Middle Aged, Brugada Syndrome

Abstract

In up to one-third of cases of sudden death, the medico-legal autopsy finding is inconclusive, and the option to perform a molecular autopsy is covered in international guidelines. The importance of postmortem genetic testing lies in its ability to identify hereditary diseases, often those with an autosomal dominant transmission pattern, and, through consultations and screening of relatives, to identify family members with a pathogenic mutation, who are often asymptomatic, providing an opportunity to change the course of their lives. The authors present three clinical cases that highlight the importance of postmortem genetic studies and family studies, as well as the integration of the data obtained in a cardiology consultation, which may be for arrhythmology, coronary disease or cardiomyopathy, depending on the specific condition. This could modify the course of the disease in many relatives.

Published

2017

44. Genetic polymorphisms of proangiogenic factors seem to favor hepatocellular carcinoma development in alcoholic cirrhosis

Author

Helena Cortez-Pinto, Gabriel Miltenberger-Miltenyi, Mariana V. Machado, and André Janeiro

Subjects

Adult, Male, Vascular Endothelial Growth Factor A, endocrine system, medicine.medical_specialty, Alcoholic liver disease, Carcinoma, Hepatocellular, Time Factors, Cirrhosis, Alcohol Drinking, endocrine system diseases, Angiogenesis, Polymorphism, Single Nucleotide, Risk Assessment, Gastroenterology, Liver disease, Gene Frequency, Liver Cirrhosis, Alcoholic, Risk Factors, Internal medicine, Odds Ratio, medicine, Humans, Genetic Predisposition to Disease, Prospective Studies, Angiogenic Proteins, Aged, Chi-Square Distribution, Hepatology, business.industry, General surgery, Liver Neoplasms, Case-control study, Kinase insert domain receptor, Middle Aged, Hypoxia-Inducible Factor 1, alpha Subunit, medicine.disease, Vascular Endothelial Growth Factor Receptor-2, Vascular endothelial growth factor A, Phenotype, Case-Control Studies, Hepatocellular carcinoma, Female, business

Abstract

Angiogenesis has been associated with hepatic cirrhosis and hepatocellular carcinoma (HCC). Alcohol promotes liver hypoxia, a trigger of angiogenesis. We aimed to evaluate whether the frequency of three polymorphisms in hypoxia-induced factor-1α (HIF-1α), vascular endothelial growth factor A (VEGFA), and KDR (encoding vascular endothelial growth factor receptor 2) genes was higher in alcoholics presenting liver disease (ALD) and ALD patients who developed HCC.Functional HIF-1α 1744C/T, VEGFA 2578C/A, and KDR 1416A/T single-nucleotide polymorphisms were studied in 125 ALD patients and 88 heavy drinkers without liver disease (NLD). ALD patients were followed up to 9 years or until they died; 26 patients developed HCC.ALD patients were older than NLD (56±11 vs. 50±13, P0.001), but drank less (215±164 vs. 331±293 g/day, P0.001). No differences were found between HIF-1α, VEGFA, or KDR allelic frequencies or genotypes, isolated or simultaneously, between ALD and NLD. In ALD patients, those who developed HCC had a higher KDR 1416T allele frequency (36 vs. 15%, P=0.004; odds ratio 2.72; 95% confidence interval 1.35-5.46). There was also a progressive increase in genotypes with one or two T alleles in patients who developed HCC: AA 50 vs. 73%, AT 35 vs. 23%, and TT 15 vs. 4% (P=0.009). The simultaneous presence of KDR 1416T and VEGFA 2578A was associated with an increased risk of HCC (odds ratio 3.088; 95% confidence interval 1.20-7.96).Genetic polymorphisms in proangiogenic factors did not associate with the risk of ALD in heavy drinkers. However, KDR and VEFGA polymorphisms may confer an increased risk of HCC in patients with ALD.

Published

2014

45. KRAS mutation analysis on low percentage of colon cancer cells: the importance of quality assurance

Author

Jean Marc Guinebretière, J.H.J.M. van Krieken, N. A 't Hart, Gerlinde Winter, Sabine Tejpar, Gabriel Miltenberger-Miltenyi, Gerald Hoefler, J. E Boers, J Diebold, Jeroen R. Dijkstra, Sónia Pereira, Etienne Rouleau, Daniëlle A.M. Heideman, Susan D. Richman, A Hirschmann, Bart Biesmans, Philip Quirke, Gerrit A. Meijer, Pathology, and CCA - Oncogenesis

Subjects

Oncology, medicine.medical_specialty, Quality Assurance, Health Care, Colorectal cancer, DNA Mutational Analysis, Cell Count, Biology, Adenocarcinoma, Bioinformatics, medicine.disease_cause, Polymerase Chain Reaction, High Resolution Melt, Pathology and Forensic Medicine, Proto-Oncogene Proteins p21(ras), symbols.namesake, Limit of Detection, Translational research [ONCOL 3], Internal medicine, Cell Line, Tumor, Proto-Oncogene Proteins, medicine, Humans, Molecular Biology, Sanger sequencing, Reproducibility of Results, Cell Biology, General Medicine, DNA, Neoplasm, medicine.disease, Translational research Tissue engineering and pathology [ONCOL 3], KRAS Mutation Analysis, Genes, ras, Molecular Diagnostic Techniques, Mutation (genetic algorithm), Mutation, Mutation testing, symbols, ras Proteins, KRAS, Colorectal Neoplasms

Abstract

Contains fulltext : 118710.pdf (Publisher’s version ) (Closed access) KRAS mutation testing is mandatory for patients with metastatic colorectal cancer who are eligible for treatment with an epidermal growth factor receptor targeting agent, since tumors with a mutation are not sensitive to the drug. Several methods for mutation testing are in use and the need for external quality assurance has been demonstrated. An often little addressed but important issue in external quality assurance schemes is a low percentage of tumor cells in the test samples, where the analytical sensitivity of most tests becomes critical. Using artificial samples based on a mixture of cell lines with known mutation status of the KRAS gene, we assessed the reliability of a series of commonly used methods (Sanger sequencing, high resolution melting, pyrosequencing, and amplification refractory mutation system-polymerase chain reaction) on samples with 0, 2.5, 5, 10, and 15 % mutated cells. Nine laboratories throughout Europe participated and submitted a total of ten data sets. The limit of detection of each method differed, ranging from >15-5 % tumor cells. All methods showed a decreasing correct mutation call rate proportionally with decreasing percentage of tumor cells. Our findings indicate that laboratories and clinicians need to be aware of the decrease in correct mutation call rate proportionally with decreasing percentage of tumor cells and that external quality assurance schemes need to address the issue of low tumor cell percentage in the test samples.

Published

2013

46. TBK1 mutation spectrum in an extended European patient cohort with frontotemporal dementia and amyotrophic lateral sclerosis

Author

Isabel Santana, Estrella Gómez-Tortosa, Federica Perrone, Patrick Cras, Alexandre de Mendonça, Jonathan Baets, Panagiotis Alexopoulos, Peter De Jonghe, Alessandro Padovani, Giovanni B. Frisoni, Frederico Simões do Couto, Håkan Thonberg, Philip Van Damme, Silvia Testi, Peter Paul De Deyn, Roberta Ghidoni, Matthew J. Fraidakis, Marc Bruyland, Maria Rosário Almeida, Alex Michotte, Jordi Clarimón, Agustín Ruiz, Jean Delbeck, Ilse Gijselinck, Jennifer Just, Olivier Deryck, Raquel Sánchez-Valle, Wim Robberecht, Matthis Synofzik, Giuliano Binetti, Adrian Ivanoiu, Sara Ortega-Cubero, Rik Vandenberghe, Isabel Hernández, Walter Maetzler, Ludger Schöls, Robert Perneczky, Kristel Sleegers, Ellen Gelpi, Alberto Lleó, Christine Van Broeckhoven, Julie van der Zee, Mercè Boada, Lubina Dillen, Eric Salmon, Marc Cruts, Patrick Santens, Sebastiaan Engelborghs, Janine Diehl-Schmid, Albert Lladó, Gian Maria Fabrizi, Radoslav Matej, Silvia Bagnoli, Pau Pastor, Frank Jessen, Barbara Borroni, Dirk Nuytten, Adrian Danek, Jan Versijpt, Bavo Heeman, Stayko Sarafov, Caroline Graff, Benedetta Nacmias, Luisa Benussi, Bart Dermaut, Johan Goeman, Michael T. Heneka, Katrien Smets, Gabor G. Kovacs, Christiana Willems, Sara Van Mossevelde, Albena Jordanova, Jan De Bleecker, Ricardo Rojas-García, Alfredo Ramirez, Bruno Bergmans, Ivailo Tournev, Veerle Bäumer, Gabriel Miltenberger-Miltenyi, Sandro Sorbi, Frisoni, Giovanni, Repositório da Universidade de Lisboa, Belgian Neurology Consortium, and European Early-Onset Dementia Consortium

Subjects

0301 basic medicine, Male, ARGYROPHILIC GRAINS, amyotrophic lateral sclerosis, TBK1, TDP-43, diagnosis [Amyotrophic Lateral Sclerosis], FAMILIAL ALS, medicine.disease_cause, frontotemporal dementia, DISEASE, Cohort Studies, ddc:616.89, diagnosis [Frontotemporal Dementia], 0302 clinical medicine, NFkB luciferase reporter assay, metabolism [Protein Serine-Threonine Kinases], C9orf72, Medicine and Health Sciences, Missense mutation, Amyotrophic lateral sclerosis, Mutation frequency, genetics [Frontotemporal Dementia], Genetics (clinical), Research Articles, Sequence Deletion, Genetics, Genetics & Heredity, Mutation, metabolism [Protein-Serine-Threonine Kinases], NF-kappa B, FTD, TBK1 protein, human, Middle Aged, Protein-Serine-Threonine Kinases, genetics [Amyotrophic Lateral Sclerosis], genetics [European Continental Ancestry Group], Phenotype, ALS, NFκB luciferase reporter assay, TANK-Binding Kinase 1, mutations, metabolism [NF-kappa B], Female, Life Sciences & Biomedicine, Frontotemporal dementia, Mutations, Research Article, TANK‐Binding Kinase 1, Heterozygote, DIAGNOSTIC-CRITERIA, epidemiology [Frontotemporal Dementia], genetics [White People], C9ORF72, genetics [Protein Serine-Threonine Kinases], epidemiology [Amyotrophic Lateral Sclerosis], Biology, Protein Serine-Threonine Kinases, genetics [Protein-Serine-Threonine Kinases], White People, 03 medical and health sciences, mental disorders, medicine, Humans, BELGIAN COHORT, ddc:610, LOBAR DEGENERATION, Gene, Alleles, Genetic Association Studies, Aged, 0604 Genetics, Science & Technology, HEXANUCLEOTIDE REPEAT, 1103 Clinical Sciences, medicine.disease, REPEAT EXPANSION, Enzyme Activation, 030104 developmental biology, Amino Acid Substitution, Case-Control Studies, Human medicine, Trinucleotide repeat expansion, 030217 neurology & neurosurgery

Abstract

© 2016 The Authors. **Human Mutation published by Wiley Periodicals, Inc. This is an open access article under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non-commercial and no modifications or adaptations are made., We investigated the mutation spectrum of the TANK-Binding Kinase 1 (TBK1) gene and its associated phenotypic spectrum by exonic resequencing of TBK1 in a cohort of 2,538 patients with frontotemporal dementia (FTD), amyotrophic lateral sclerosis (ALS), or FTD plus ALS, ascertained within the European Early-Onset Dementia Consortium. We assessed pathogenicity of predicted protein-truncating mutations by measuring loss of RNA expression. Functional effect of in-frame amino acid deletions and missense mutations was further explored in vivo on protein level and in vitro by an NFκB-induced luciferase reporter assay and measuring phosphorylated TBK1. The protein-truncating mutations led to the loss of transcript through nonsense-mediated mRNA decay. For the in-frame amino acid deletions, we demonstrated loss of TBK1 or phosphorylated TBK1 protein. An important fraction of the missense mutations compromised NFκB activation indicating that at least some functions of TBK1 are lost. Although missense mutations were also present in controls, over three times more mutations affecting TBK1 functioning were found in the mutation fraction observed in patients only, suggesting high-risk alleles (P = 0.03). Total mutation frequency for confirmed TBK1 LoF mutations in the European cohort was 0.7%, with frequencies in the clinical subgroups of 0.4% in FTD, 1.3% in ALS, and 3.6% in FTD-ALS.

Published

2016

47. Mild Left Ventricular Hypertrophy Unravels a Novel Nonsense Mutation of the GLA Gene Associated with the Classical Phenotype of Fabry Disease

Author

Olga, Azevedo, Miguel, Gago, Gabriel, Miltenberger-Miltenyi, Paulo, Gaspar, Nuno, Sousa, and Damião, Cunha

Subjects

Adult, Male, Heterozygote, Middle Aged, Pedigree, Young Adult, Phenotype, Sex Factors, Codon, Nonsense, Echocardiography, alpha-Galactosidase, Fabry Disease, Humans, Female, Hypertrophy, Left Ventricular

Abstract

We report on the clinical, biochemical, and genetic findings of a large family with the classical phenotype of Fabry disease due to the novel nonsense mutation c.607GT (p.E203X) of the GLA gene, which occurs in the active site of the α-galactosidase A enzyme. This report highlights that (i) Fabry disease diagnosis should be considered in all cases of unexplained left ventricular hypertrophy (LVH), even in its milder forms; (ii) a complete evaluation of patients with unexplained LVH is important to find diagnostic red flags of treatable causes of LVH, such as Fabry disease; (iii) cascade family screening is paramount to the earlier diagnosis and treatment of other affected family members; and (iv) the Fabry disease phenotype is highly variable in heterozygote females, even within the same family.

Published

2016

48. Molecular characterization of parathyroid tumors from two patients with hereditary colorectal cancer syndromes

Author

Erik Björck, Catharina Larsson, Lucas Batista, Luqman Sulaiman, Gabriel Miltenberger-Miltenyi, Sónia do Vale, Joao Martin Martins, Florbela Ferreira, Felix Haglund, Adam Andreasson, Inga-Lena Nilsson, Anders Höög, and C. Christofer Juhlin

Subjects

Adenoma, Male, Cancer Research, Pathology, medicine.medical_specialty, Proliferation index, Tumor suppressor gene, Adenomatous polyposis coli, Colorectal cancer, Adenomatous Polyposis Coli Protein, Parafibromin, Gene Dosage, Copy number analysis, Gene dosage, Familial adenomatous polyposis, Genetics, medicine, Humans, Promoter Regions, Genetic, Genetics (clinical), Adaptor Proteins, Signal Transducing, Aged, Aged, 80 and over, biology, Tumor Suppressor Proteins, Nuclear Proteins, DNA Methylation, medicine.disease, Gene Expression Regulation, Neoplastic, Parathyroid Neoplasms, Oncology, Mutation, biology.protein, Cancer research, Female, MutL Protein Homolog 1

Abstract

The tumor suppressor adenomatous polyposis coli (APC) has recently been implicated in parathyroid development. We here report clinical, histopathological and molecular investigations in parathyroid tumors arising in two patients; one familial adenomatous polyposis (FAP) syndrome patient carrying a constitutional APC mutation, and one Lynch syndrome patient demonstrating a germline MLH1 mutation as well as a non-classified, missense alteration of the APC gene. We sequenced the entire APC gene in tumor and constitutional DNA from both cases, assessed the levels of APC promoter 1A and 1B methylation by bisulfite Pyrosequencing analysis and performed immunohistochemistry for APC and parafibromin. In addition, copy number analysis regarding the APC gene on chromosome 5q21-22 was performed using qRT-PCR. Histopathological workup confirmed both tumors as parathyroid adenomas without signs of malignancy or atypia. No somatic mutations or copy number changes for the APC gene were discovered in the tumors; however, in both cases, the APC promoter 1A was hypermethylated while the APC promoter 1B was unmethylated. APC promoter 1B-specific mRNA and total APC mRNA levels were higher than in normal parathyroid samples. Immunohistochemical analyses revealed strong APC protein immunoreactivity and positive parafibromin expression in both parathyroid tumors. Absence of additional somatic APC mutations and copy number changes in addition to the positive APC immunoreactivity obtained suggest that the tumors arose without biallelic inactivation of the APC tumor suppressor gene. The finding of an unmethylated APC promoter 1B and high APC 1B mRNA levels could explain the maintained APC protein expression. Moreover, the findings of positive parafibromin and APC immunoreactivity as well as a low MIB-1 proliferation index and absence of histopathological features of malignancy/atypical adenoma indicate that the parathyroid adenomas arising in these patients did not harbor malignant potential.

Published

2012

49. Nova mutação na síndroma de QT Longo em doente com diagnóstico prévio de epilepsia

Author

Gabriel Miltenberger-Miltenyi, João de Sousa, Maria José Correia, João Silva Marques, Cláudia Jorge, António Nunes Diogo, Arminda Veiga, Jorge Oliver-De La Cruz, João Nóbrega, and Rita Peralta

Subjects

lcsh:Diseases of the circulatory (Cardiovascular) system, lcsh:RC666-701, Cardiology and Cardiovascular Medicine

Abstract

Resumo: A síndroma de QT longo congénita (SQTL) pode manifestar-se por síncopes ou convulsões recorrentes, no contexto de taquicardia ventricular polimórfica, podendo simular epilepsia.Nos doentes tratados com cardioversor-desfibrilhador implantável (CDI) a recorrência de arritmias com consequente terapêutica com choques frequentes pode conduzir a reacções adversas, nomeadamente psicogénicas.Apresentamos o caso de uma doente de 22 anos com síncopes e crises convulsivas, cujo diagnóstico era desde a infância de epilepsia, e em quem a SQTL foi diagnosticada apenas em idade adulta. Por falência da terapêutica beta-bloqueante implantou CDI, e por persistência de arritmias foi submetida a simpaticectomia cardíaca esquerda. O follow-up pós-cirurgia aos 3 meses mostrou redução significativa do número de arritmias.O estudo genético identificou uma mutação patogénica no gene KCNH2 (SQTL tipo 2), em heterozigotia, a mutação c.1817 C >T p.S606F, ainda não descrita na literatura. Relatamos também a rara ocorrência de tempestade arrítmica no contexto de infecção a H1N1.O caso clínico ilustra as dificuldades quer do diagnóstico quer do tratamento da SQTL. É discutida a possibilidade duma base genética partilhada entre a doença disrítmica e neurológica. Abstract: Congenital long QT syndrome (LQTS) can present as syncope or seizures, secondary to polymorphic ventricular tachycardia, mimicking a primary seizure disorder.In patients treated with an implantable cardioverter-defibrillator (ICD), the recurrence of arrhythmias with subsequent frequent therapeutic shocks may cause adverse reactions, which can be psychogenic.We report the case of a 22-year-old woman with syncope and seizures who was diagnosed in childhood as epileptic and in whom LQTS was diagnosed only in adulthood. Beta-blocker therapy failed and an ICD was implanted. However, as arrhythmias persisted, left cardiac sympathetic denervation was performed. After surgery, three-month follow-up showed a significant reduction in arrhythmias.The genetic study identified a heterozygous mutation, c.1817 C>T p.S606F, on the KCNH2 gene that has not previously been reported in the literature. We also report the rare occurrence of an electrical storm in the course of H1N1 infection.This case illustrates the difficulties in the diagnosis and treatment of LQTS. The possibility of a common genetic basis for arrhythmic diseases and epilepsy is discussed. Palavras-chave: Síndroma de QT longo, Epilepsia, Canalopatia, Keywords: Long QT syndrome, Epilepsy, Channelopathy

Published

2011

50. Novel mutation in long QT syndrome in a patient with prior diagnosis of epilepsy

Author

Jorge Cruz, Maria José Correia, João Nóbrega, Rita Peralta, Cláudia Jorge, António Nunes Diogo, João Silva Marques, Arminda Veiga, and Gabriel Miltenberger-Miltenyi

Subjects

medicine.medical_specialty, lcsh:Diseases of the circulatory (Cardiovascular) system, biology, business.industry, Long QT syndrome, Prior diagnosis, Syncope (genus), biology.organism_classification, medicine.disease, Ventricular tachycardia, Epilepsy, Channelopathy, lcsh:RC666-701, Internal medicine, medicine, Cardiology, General Earth and Planetary Sciences, Psychogenic disease, cardiovascular diseases, business, Novel mutation, General Environmental Science

Abstract

Congenital long QT syndrome (LQTS) can present as syncope or seizures, secondary to polymorphic ventricular tachycardia, mimicking a primary seizure disorder.In patients treated with an implantable cardioverter-defibrillator (ICD), the recurrence of arrhythmias with subsequent frequent therapeutic shocks may cause adverse reactions, which can be psychogenic.We report the case of a 22-year-old woman with syncope and seizures who was diagnosed in childhood as epileptic and in whom LQTS was diagnosed only in adulthood.Beta-blocker therapy failed and an ICD was implanted. However, as arrhythmias persisted, left cardiac sympathetic denervation was performed. After surgery, three-month follow-up showed a significant reduction in arrhythmias.The genetic study identified a heterozygous mutation, c.1817 C>T p.S606F, on the KCNH2 gene that has not previously been reported in the literature.We also report the rare occurrence of an electrical storm in the course of H1N1 infection.This case illustrates the difficulties in the diagnosis and treatment of LQTS. The possibility of a common genetic basis for arrhythmic diseases and epilepsy is discussed. Resumo: A síndroma de QT longo congénita (SQTL) pode manifestar-se por síncopes ou convulsões recorrentes, no contexto de taquicardia ventricular polimórfica, podendo simular epilepsia.Nos doentes tratados com cardioversor-desfibrilhador implantável (CDI) a recorrência de arritmias com consequente terapêutica com choques frequentes pode conduzir a reacções adversas, nomeadamente psicogénicas.Apresentamos o caso de uma doente de 22 anos com síncopes e crises convulsivas, cujo diagnóstico era desde a infância de epilepsia, e em quem a SQTL foi diagnosticada apenas em idade adulta. Por falência da terapêutica beta-bloqueante implantou CDI, e por persistência de arritmias foi submetida a simpaticectomia cardíaca esquerda. O follow-up pós-cirurgia aos 3 meses mostrou redução significativa do número de arritmias.O estudo genético identificou uma mutação patogénica no gene KCNH2 (SQTL tipo 2), em heterozigotia, a mutação c.1817 C >T p.S606F, ainda não descrita na literatura. Relatamos também a rara ocorrência de tempestade arrítmica no contexto de infecção a H1N1.O caso clínico ilustra as dificuldades quer do diagnóstico quer do tratamento da SQTL. É discutida a possibilidade duma base genética partilhada entre a doença disrítmica e neurológica. Keywords: Long QT syndrome, Epilepsy, Channelopathy, Palavras-chave: Síndroma de QT longo, Epilepsia, Canalopatia

Published

2011