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51. A randomized, double-blind trial of triheptanoin for drug-resistant epilepsy in glucose transporter 1 deficiency syndrome

Author

Striano, Pasquale, Auvin, Stéphane, Collins, Abigail, Horvath, Rita, Scheffer, Ingrid E, Tzadok, Michal, Miller, Ian, Kay Koenig, Mary, Lacy, Adrian, Davis, Ronald, Garcia-Cazorla, Angela, Saneto, Russell P, Brandabur, Melanie, Blair, Susan, Koutsoukos, Tony, De Vivo, Darryl, Striano, Pasquale [0000-0002-6065-1476], Auvin, Stéphane [0000-0003-3874-9749], Scheffer, Ingrid E [0000-0002-2311-2174], Miller, Ian [0000-0003-0416-1015], and Apollo - University of Cambridge Repository

Subjects
Adult, Drug Resistant Epilepsy, Glucose Transporter Type 1, drug resistance, Adolescent, Monosaccharide Transport Proteins, diet treatment, triheptanoin, glucose transporter 1 deficiency syndrome, Treatment Outcome, Double-Blind Method, Epilepsy, Absence, Seizures, epilepsy, Humans, Anticonvulsants, Drug Therapy, Combination, Child, Triglycerides, Carbohydrate Metabolism, Inborn Errors
Abstract

Funder: Ultragenyx Pharmaceutical Inc.; Id: http://dx.doi.org/10.13039/100013220, OBJECTIVE: This study was undertaken to evaluate efficacy and long-term safety of triheptanoin in patients >1 year old, not on a ketogenic diet, with drug-resistant seizures associated with glucose transporter 1 deficiency syndrome (Glut1DS). METHODS: UX007G-CL201 was a randomized, double-blind, placebo-controlled trial. Following a 6-week baseline period, eligible patients were randomized 3:1 to triheptanoin or placebo. Dosing was titrated to 35% of total daily calories over 2 weeks. After an 8-week placebo-controlled period, all patients received open-label triheptanoin through Week 52. RESULTS: The study included 36 patients (15 children, 13 adolescents, eight adults). A median 12.6% reduction in overall seizure frequency was observed in the triheptanoin arm relative to baseline, and a 13.5% difference was observed relative to placebo (p = .58). In patients with absence seizures only (n = 9), a median 62.2% reduction in seizure frequency was observed in the triheptanoin arm relative to baseline. Only one patient with absence seizures only was present in the control group, preventing comparison. No statistically significant differences in seizure frequency were observed. Common treatment-emergent adverse events included diarrhea, vomiting, abdominal pain, and nausea, mostly mild or moderate in severity. No serious adverse events were considered to be treatment related. One patient discontinued due to status epilepticus. SIGNIFICANCE: Triheptanoin did not significantly reduce seizure frequency in patients with Glut1DS not on the ketogenic diet. Treatment was associated with mild to moderate gastrointestinal treatment-related events; most resolved following dose reduction or interruption and/or medication for treatment. Triheptanoin was not associated with any long-term safety concerns when administered at dose levels up to 35% of total daily caloric intake for up to 1 year.

Published
2022

52. Age at disease onset and peak ammonium level rather than interventional variables predict the neurological outcome in urea cycle disorders

Author

Posset, Roland, Garcia-Cazorla, Angeles, Valayannopoulos, Vassili, Teles, Elisa Leão, Dionisi-Vici, Carlo, Brassier, Anaïs, Burlina, Alberto B., Burgard, Peter, Cortès-Saladelafont, Elisenda, Dobbelaere, Dries, Couce, Maria L., Sykut-Cegielska, Jolanta, Häberle, Johannes, Lund, Allan M., Chakrapani, Anupam, Schiff, Manuel, Walter, John H., Zeman, Jiri, Vara, Roshni, Kölker, Stefan, and Additional individual contributors of the E-IMD consortium

Published
2016
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55. Secondary Abnormalities of Neurotransmitters in Infants with Neurological Disorders

Author

Garcia-Cazorla, A., Serrano, M., and Perez-Duenas, B.

Abstract

Neurotransmitters are essential in young children for differentiation and neuronal growth of the developing nervous system. We aimed to identify possible factors related to secondary neurotransmitter abnormalities in pediatric patients with neurological disorders. We analyzed cerebrospinal fluid (CSF) and biogenic amine metabolites in 56 infants (33 males, 23 females; mean age 5.8mo [SD 4.1mo] range 1d-1y) with neurological disorders whose aetiology was initially unknown. Patients were classified into three clinical phenotypes: epileptic encephalopathy, severe motor impairment, and non-specific manifestations. All patients showed normal results for screening of inborn errors of metabolism. We report clinical, neuroimaging, and follow-up data. Among the patients studied, 10 had low homovanillic acid (HVA) levels and in four patients, 5-hydroxyindoleacetic acid (5-HIAA) was also reduced. Patients with neonatal onset had significantly lower levels of HVA than a comparison group. HVA deficiency was also associated with severe motor impairment and the final diagnosis related to neurodegenerative disorders. 5-HIAA values tended to be decreased in patients with brain cortical atrophy. The possibility of treating patients with L-Dopa and 5-hydroxytryptophan, in order to improve their neurological function and maturation, may be considered. (Contains 2 tables.)

Published
2007
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56. A randomized, double-blind trial of triheptanoin for drug-resistant epilepsy in glucose transporter 1 deficiency syndrome

Author

Striano, P, Auvin, S, Collins, A, Horvath, R, Scheffer, IE, Tzadok, M, Miller, I, Koenig, MK, Lacy, A, Davis, R, Garcia-Cazorla, A, Saneto, RP, Brandabur, M, Blair, S, Koutsoukos, T, De Vivo, D, Striano, P, Auvin, S, Collins, A, Horvath, R, Scheffer, IE, Tzadok, M, Miller, I, Koenig, MK, Lacy, A, Davis, R, Garcia-Cazorla, A, Saneto, RP, Brandabur, M, Blair, S, Koutsoukos, T, and De Vivo, D

Abstract

OBJECTIVE: This study was undertaken to evaluate efficacy and long-term safety of triheptanoin in patients >1 year old, not on a ketogenic diet, with drug-resistant seizures associated with glucose transporter 1 deficiency syndrome (Glut1DS). METHODS: UX007G-CL201 was a randomized, double-blind, placebo-controlled trial. Following a 6-week baseline period, eligible patients were randomized 3:1 to triheptanoin or placebo. Dosing was titrated to 35% of total daily calories over 2 weeks. After an 8-week placebo-controlled period, all patients received open-label triheptanoin through Week 52. RESULTS: The study included 36 patients (15 children, 13 adolescents, eight adults). A median 12.6% reduction in overall seizure frequency was observed in the triheptanoin arm relative to baseline, and a 13.5% difference was observed relative to placebo (p = .58). In patients with absence seizures only (n = 9), a median 62.2% reduction in seizure frequency was observed in the triheptanoin arm relative to baseline. Only one patient with absence seizures only was present in the control group, preventing comparison. No statistically significant differences in seizure frequency were observed. Common treatment-emergent adverse events included diarrhea, vomiting, abdominal pain, and nausea, mostly mild or moderate in severity. No serious adverse events were considered to be treatment related. One patient discontinued due to status epilepticus. SIGNIFICANCE: Triheptanoin did not significantly reduce seizure frequency in patients with Glut1DS not on the ketogenic diet. Treatment was associated with mild to moderate gastrointestinal treatment-related events; most resolved following dose reduction or interruption and/or medication for treatment. Triheptanoin was not associated with any long-term safety concerns when administered at dose levels up to 35% of total daily caloric intake for up to 1 year.

Published
2022

57. Human ultrarare genetic disorders of sulfur metabolism demonstrate redundancies in H2S homeostasis

Author

Kozich, Viktor, Schwahn, Bernd C., Sokolova, Jitka, Krizkova, Michaela, Ditroi, Tamas, Krijt, Jakub, Khalil, Youssef, Krizek, Tomas, Vaculikova-Fantlova, Tereza, Stiburkova, Blanka, Mills, Philippa, Clayton, Peter, Barvikova, Kristyna, Blessing, Holger, Sykut-Cegielska, Jolanta, Dionisi-Vici, Carlo, Gasperini, Serena, Garcia-Cazorla, Angeles, Haack, Tobias B., Honzik, Tomas, Jesina, Pavel, Kuster, Alice, Laugwitz, Lucia, Martinelli, Diego, Porta, Francesco, Santer, Rene, Schwarz, Guenter, Nagy, Peter, Kozich, Viktor, Schwahn, Bernd C., Sokolova, Jitka, Krizkova, Michaela, Ditroi, Tamas, Krijt, Jakub, Khalil, Youssef, Krizek, Tomas, Vaculikova-Fantlova, Tereza, Stiburkova, Blanka, Mills, Philippa, Clayton, Peter, Barvikova, Kristyna, Blessing, Holger, Sykut-Cegielska, Jolanta, Dionisi-Vici, Carlo, Gasperini, Serena, Garcia-Cazorla, Angeles, Haack, Tobias B., Honzik, Tomas, Jesina, Pavel, Kuster, Alice, Laugwitz, Lucia, Martinelli, Diego, Porta, Francesco, Santer, Rene, Schwarz, Guenter, and Nagy, Peter

Abstract

Regulation of H2S homeostasis in humans is poorly understood. Therefore, we assessed the importance of in-dividual enzymes in synthesis and catabolism of H2S by studying patients with respective genetic defects. We analyzed sulfur compounds (including bioavailable sulfide) in 37 untreated or insufficiently treated patients with seven ultrarare enzyme deficiencies and compared them to 63 controls. Surprisingly, we observed that patients with severe deficiency in cystathionine beta-synthase (CBS) or cystathionine gamma-lyase (CSE) -the enzymes primarily responsible for H2S synthesis -exhibited increased and normal levels of bioavailable sulfide, respectively. However, an approximately 21-fold increase of urinary homolanthionine in CBS deficiency strongly suggests that lacking CBS activity is compensated for by an increase in CSE-dependent H2S synthesis from accumulating ho-mocysteine, which suggests a control of H2S homeostasis in vivo. In deficiency of sulfide:quinone oxidoreductase -the first enzyme in mitochondrial H2S oxidation -we found normal H2S concentrations in a symptomatic patient and his asymptomatic sibling, and elevated levels in an asymptomatic sibling, challenging the requirement for this enzyme in catabolizing H2S under physiological conditions. Patients with ethylmalonic encephalopathy and sulfite oxidase/molybdenum cofactor deficiencies exhibited massive accumulation of thiosulfate and sulfite with formation of large amounts of S-sulfocysteine and S-sulfohomocysteine, increased renal losses of sulfur com-pounds and concomitant strong reduction in plasma total cysteine. Our results demonstrate the value of a comprehensive assessment of sulfur compounds in severe disorders of homocysteine/cysteine metabolism and provide evidence for redundancy and compensatory mechanisms in the maintenance of H2S homeostasis.

Published
2022

59. The phenotypic spectrum of organic acidurias and urea cycle disorders. Part 2: the evolving clinical phenotype

Author

Kölker, Stefan, Valayannopoulos, Vassili, Burlina, Alberto B., Sykut-Cegielska, Jolanta, Wijburg, Frits A., Teles, Elisa Leão, Zeman, Jiri, Dionisi-Vici, Carlo, Barić, Ivo, Karall, Daniela, Arnoux, Jean-Baptiste, Avram, Paula, Baumgartner, Matthias R., Blasco-Alonso, Javier, Boy, S. P. Nikolas, Rasmussen, Marlene Bøgehus, Burgard, Peter, Chabrol, Brigitte, Chakrapani, Anupam, Chapman, Kimberly, Cortès i Saladelafont, Elisenda, Couce, Maria L., de Meirleir, Linda, Dobbelaere, Dries, Furlan, Francesca, Gleich, Florian, González, Maria Julieta, Gradowska, Wanda, Grünewald, Stephanie, Honzik, Tomas, Hörster, Friederike, Ioannou, Hariklea, Jalan, Anil, Häberle, Johannes, Haege, Gisela, Langereis, Eveline, de Lonlay, Pascale, Martinelli, Diego, Matsumoto, Shirou, Mühlhausen, Chris, Murphy, Elaine, de Baulny, Hélène Ogier, Ortez, Carlos, Pedrón, Consuelo C., Pintos-Morell, Guillem, Pena-Quintana, Luis, Ramadža, Danijela Petković, Rodrigues, Esmeralda, Scholl-Bürgi, Sabine, Sokal, Etienne, Summar, Marshall L., Thompson, Nicholas, Vara, Roshni, Pinera, Inmaculada Vives, Walter, John H., Williams, Monique, Lund, Allan M., and Garcia Cazorla, Angeles

Published
2015
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61. A randomized, double‐blind trial of triheptanoin for drug‐resistant epilepsy in glucose transporter 1 deficiency syndrome

Author

Striano, Pasquale, primary, Auvin, Stéphane, additional, Collins, Abigail, additional, Horvath, Rita, additional, Scheffer, Ingrid E., additional, Tzadok, Michal, additional, Miller, Ian, additional, Kay Koenig, Mary, additional, Lacy, Adrian, additional, Davis, Ronald, additional, Garcia‐Cazorla, Angela, additional, Saneto, Russell P., additional, Brandabur, Melanie, additional, Blair, Susan, additional, Koutsoukos, Tony, additional, and De Vivo, Darryl, additional

Published
2022
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62. Novel CSF biomarkers of GLUT1 deficiency syndrome: implications beyond the brain's energy deficit

Author

Peters, Tessa M.A., primary, Merx, Jona, additional, Kooijman, Pieter C., additional, Noga, Marek, additional, De Boer, Siebolt, additional, Van Gemert, Loes A., additional, Salden, Guido, additional, Engelke, Udo F.H., additional, Lefeber, Dirk J., additional, Van Outersterp, Rianne E., additional, Berden, Giel, additional, Boltje, Thomas J., additional, Artuch, Rafael, additional, Pias, Leticia, additional, Garcia-Cazorla, Angeles, additional, Baric, Ivo, additional, Thony, Beat, additional, Oomens, Jos, additional, Martens, Jonathan, additional, Wevers, Ron A., additional, Verbeek, Marcel M., additional, Coene, Karlien L.M., additional, and Willemsen, Michel A.A.P., additional

Published
2022
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63. GDF-15 Is Elevated in Children with Mitochondrial Diseases and Is Induced by Mitochondrial Dysfunction.

Author

Raquel Montero, Delia Yubero, Joan Villarroya, Desiree Henares, Cristina Jou, Maria Angeles Rodríguez, Federico Ramos, Andrés Nascimento, Carlos Ignacio Ortez, Jaume Campistol, Belen Perez-Dueñas, Mar O'Callaghan, Mercedes Pineda, Angeles Garcia-Cazorla, Jaume Colomer Oferil, Julio Montoya, Eduardo Ruiz-Pesini, Sonia Emperador, Marija Meznaric, Laura Campderros, Susana G Kalko, Francesc Villarroya, Rafael Artuch, and Cecilia Jimenez-Mallebrera

Subjects
Medicine, Science
Abstract

BACKGROUND:We previously described increased levels of growth and differentiation factor 15 (GDF-15) in skeletal muscle and serum of patients with mitochondrial diseases. Here we evaluated GDF-15 as a biomarker for mitochondrial diseases affecting children and compared it to fibroblast-growth factor 21 (FGF-21). To investigate the mechanism of GDF-15 induction in these pathologies we measured its expression and secretion in response to mitochondrial dysfunction. METHODS:We analysed 59 serum samples from 48 children with mitochondrial disease, 19 samples from children with other neuromuscular diseases and 33 samples from aged-matched healthy children. GDF-15 and FGF-21 circulating levels were determined by ELISA. RESULTS:Our results showed that in children with mitochondrial diseases GDF-15 levels were on average increased by 11-fold (mean 4046pg/ml, 1492 SEM) relative to healthy (350, 21) and myopathic (350, 32) controls. The area under the curve for the receiver-operating-characteristic curve for GDF-15 was 0.82 indicating that it has a good discriminatory power. The overall sensitivity and specificity of GDF-15 for a cut-off value of 550pg/mL was 67.8% (54.4%-79.4%) and 92.3% (81.5%-97.9%), respectively. We found that elevated levels of GDF-15 and or FGF-21 correctly identified a larger proportion of patients than elevated levels of GDF-15 or FGF-21 alone. GDF-15, as well as FGF-21, mRNA expression and protein secretion, were significantly induced after treatment of myotubes with oligomycin and that levels of expression of both factors significantly correlated. CONCLUSIONS:Our data indicate that GDF-15 is a valuable serum quantitative biomarker for the diagnosis of mitochondrial diseases in children and that measurement of both GDF-15 and FGF-21 improves the disease detection ability of either factor separately. Finally, we demonstrate for the first time that GDF-15 is produced by skeletal muscle cells in response to mitochondrial dysfunction and that its levels correlate in vitro with FGF-21 levels.

Published
2016
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64. Targeted Next Generation Sequencing in Patients with Inborn Errors of Metabolism.

Author

Dèlia Yubero, Núria Brandi, Aida Ormazabal, Àngels Garcia-Cazorla, Belén Pérez-Dueñas, Jaime Campistol, Antonia Ribes, Francesc Palau, Rafael Artuch, Judith Armstrong, and Working Group

Subjects
Medicine, Science
Abstract

Next-generation sequencing (NGS) technology has allowed the promotion of genetic diagnosis and are becoming increasingly inexpensive and faster. To evaluate the utility of NGS in the clinical field, a targeted genetic panel approach was designed for the diagnosis of a set of inborn errors of metabolism (IEM). The final aim of the study was to compare the findings for the diagnostic yield of NGS in patients who presented with consistent clinical and biochemical suspicion of IEM with those obtained for patients who did not have specific biomarkers.The subjects studied (n = 146) were classified into two categories: Group 1 (n = 81), which consisted of patients with clinical and biochemical suspicion of IEM, and Group 2 (n = 65), which consisted of IEM cases with clinical suspicion and unspecific biomarkers. A total of 171 genes were analyzed using a custom targeted panel of genes followed by Sanger validation.Genetic diagnosis was achieved in 50% of patients (73/146). In addition, the diagnostic yield obtained for Group 1 was 78% (63/81), and this rate decreased to 15.4% (10/65) in Group 2 (X2 = 76.171; p < 0.0001).A rapid and effective genetic diagnosis was achieved in our cohort, particularly the group that had both clinical and biochemical indications for the diagnosis.

Published
2016
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65. Diagnosis of Genetic White Matter Disorders by Singleton Whole-Exome and Genome Sequencing Using Interactome-Driven Prioritization

Author

Schluter, A, Rodriguez-Palmero, A, Verdura, E, Velez-Santamaria, V, Ruiz, M, Fourcade, S, Planas-Serra, L, Martinez, JJ, Guilera, C, Giros, M, Artuch, R, Yoldi, ME, O'Callaghan, M, Garcia-Cazorla, A, Armstrong, J, Marti, I, Rezola, EM, Redin, C, Mandel, JL, Conejo, D, Sierra-Corcoles, C, Beltran, S, Gut, M, Vazquez, E, Del Toro, M, Troncoso, M, Perez-Jurado, LA, Gutierrez-Solana, LG, de Munain, AL, Casasnovas, C, Aguilera-Albesa, S, Macaya, A, and Pujol, A

Abstract

Background and Objectives Genetic white matter disorders (GWMD) are of heterogeneous origin, with >100 causal genes identified to date. Classic targeted approaches achieve a molecular diagnosis in only half of all patients. We aimed to determine the clinical utility of singleton whole-exome sequencing and whole-genome sequencing (sWES-WGS) interpreted with a phenotype- and interactome-driven prioritization algorithm to diagnose GWMD while identifying novel phenotypes and candidate genes. Methods A case series of patients of all ages with undiagnosed GWMD despite extensive standard-of-care paraclinical studies were recruited between April 2017 and December 2019 in a collaborative study at the Bellvitge Biomedical Research Institute (IDIBELL) and neurology units of tertiary Spanish hospitals. We ran sWES and WGS and applied our interactome-prioritization algorithm based on the network expansion of a seed group of GWMD-related genes derived from the Human Phenotype Ontology terms of each patient. Results We evaluated 126 patients (101 children and 25 adults) with ages ranging from 1 month to 74 years. We obtained a first molecular diagnosis by singleton WES in 59% of cases, which increased to 68% after annual reanalysis, and reached 72% after WGS was performed in 16 of the remaining negative cases. We identified variants in 57 different genes among 91 diagnosed cases, with the most frequent being RNASEH2B, EIF2B5, POLR3A, and PLP1, and a dual diagnosis underlying complex phenotypes in 6 families, underscoring the importance of genomic analysis to solve these cases. We discovered 9 candidate genes causing novel diseases and propose additional putative novel candidate genes for yet-to-be discovered GWMD. Discussion Our strategy enables a high diagnostic yield and is a good alternative to trio WES/WGS for GWMD. It shortens the time to diagnosis compared to the classical targeted approach, thus optimizing appropriate management. Furthermore, the interactome-driven prioritization pipeline enables the discovery of novel disease-causing genes and phenotypes, and predicts novel putative candidate genes, shedding light on etiopathogenic mechanisms that are pivotal for myelin generation and maintenance.

Published
2022

66. The clinical and biochemical hallmarks generally associated with GLUT1DS may be caused by defects in genes other than SLC2A1

Author

Sánchez-Lijarcio O, Yubero-Siles D, Leal F, Couce ML, González Gutiérrez-Solana L, López-Laso E, Garcia-Cazorla A, Pias-Peleteiro LD, de Azua Brea B, Ibáñez-Micó S, Mateo-Martínez G, Troncoso-Schifferli M, Witting-Enriquez S, Ugarte M, Artuch-Iriberri R, and Pérez-Dueñas B

Subjects
GLUT1DS, SLC2A1, hypoglycorrhachia, GLUT1
Abstract

Glucose transporter 1 deficiency syndrome (GLUT1DS) is a neurometabolic disorder caused by haploinsufficiency of the GLUT1 glucose transporter (encoded by SLC2A1) leading to defective glucose transport across the blood-brain barrier. This work describes the genetic analysis of 56 patients with clinical or biochemical GLUT1DS hallmarks. 55.4% of these patients had a pathogenic variant of SLC2A1, and 23.2% had a variant in one of 13 different genes. No pathogenic variant was identified for the remaining patients. Expression analysis of SLC2A1 indicated a reduction in SLC2A1 mRNA in patients with pathogenic variants of this gene, as well as in one patient with a pathogenic variant in SLC9A6, and in three for whom no candidate variant was identified. Thus, the clinical and biochemical hallmarks generally associated with GLUT1DS may be caused by defects in genes other than SLC2A1.

Published
2022

67. Genetic disorders of cellular trafficking

Author

Garcia-Cazorla A, De Oyarzabal-Sanz AL, Saudubray JM, Martinelly D, and Dionisi-Vici C

Subjects
autophagy, membrane contact sites, cellular trafficking, vesicular trafficking, inherited metabolic diseases
Abstract

Cellular trafficking is essential to maintain critical biological functions. Mutations in 346 genes, most of them described in the last 5 years, are associated with disorders of cellular trafficking. Whereas initially restricted to membrane trafficking, the recent detection of many diseases has contributed to the discovery of new biological pathways. Accordingly, we propose to redesign this rapidly growing group of diseases combining biological mechanisms and clinical presentation into the following categories: (i) membrane trafficking (including organelle-related); (ii) membrane contact sites; (iii) autophagy; (iv) cytoskeleton-related. We present the most recently described pathophysiological findings, disorders and phenotypes. Although all tissues and organs are affected, the nervous system is especially vulnerable.

Published
2022

68. Monoamine neurotransmitters in early epileptic encephalopathies: New insights into pathophysiology and therapy

Author

Julia-Palacios, N, Molina-Anguita, C, Bondarenko, MS, Cortes-Saladelafont, E, Aparicio, J, Cuadras, D, Horvath, G, Fons, C, Artuch, R, and Garcia-Cazorla, A

Abstract

Aim To study neurotransmitter status in children with early epileptic and developmental and epileptic encephalopathy (DEE) and to explore the clinical response to dopaminergic and serotoninergic therapies in a group of patients. Method Two hundred and five patients (111 males [54.1.%] and 94 females [45.9%], mean age 10 months at the onset of epilepsy [SD 1 year 1 month], range 0-3 year) with epileptic encephalopathy/DEE were recruited, including those with West syndrome, Ohtahara syndrome, early myoclonic encephalopathy, epilepsy of infancy with migrating focal seizures, myoclonic encephalopathy in non-progressive disorders, infantile spasms, Doose syndrome, Lennox-Gastaut syndrome, Landau-Kleffner syndrome, and those unclassified. Cerebrospinal fluid (CSF) neurotransmitter studies and patients' medical records were reviewed. Additionally, we present clinical data of 10 patients with low CSF neurotransmitter levels who received dopaminergic/serotoninergic treatments. Results Abnormal neurotransmitter values were identified in 68 (33%) patients. 5-Hydroxyindoleacetic acid (5-HIAA) deficit was the most prevalent alteration (91%). Low CSF 5-HIAA levels were significantly higher in 1- to 3-year-old children. A negative significant correlation was found between 5-HIAA levels and epilepsy duration before CSF study (Spearman's rho=-0.191, p=0.007). Abnormalities in deep grey matter were associated with low levels of CSF homovanillic acid and 5-HIAA. Ten patients with low CSF neurotransmitter levels received dopamine and/or serotonin therapies. Six of them showed initial decrease of seizure frequency and severity and maintained improvement in some neurodevelopmental skills. Interpretation A considerable number of patients showed neurotransmitter abnormalities. Age at seizure onset and duration of epilepsy before CSF study were the principal factors related to neurotransmitter depletion. Early monoamine supplementation would seem advisable as a neuroprotective strategy. What this paper adds 5-Hydroxyindoleacetic acid homeostasis is especially vulnerable in patients with epileptic encephalopathy/developmental and epileptic encephalopathy. Age of seizure onset and duration of epilepsy are determinants of neurotransmitter depletion.

Published
2022

69. Volumetric study of brain MRI in a cohort of patients with neurotransmitter disorders

Author

Chiara Alfonsi, Christian Stephan-Otto, Elisenda Cortès-Saladelafont, Natalia Juliá Palacios, Inés Podzamczer-Valls, Nuria Gutiérrez Cruz, María Rosario Domingo Jiménez, Salvador Ibáñez Micó, Miguel Tomás Vila, Kathrin Jeltsch, Oya Kuseyri Hübschmann, Thomas Opladen, Ramón Velázquez Fragua, Teresa Gómez, Oscar Alcoverro Fortuny, Inmaculada García Jiménez, Eduardo López Laso, Ana Roche Martínez, Jordi Muchart López, and Àngels Garcia-Cazorla

Subjects
Monoamines, Inherited neurotransmitter disorders, Neurotransmitter Agents, amino acids, neuroimaging, Brain, Brain volumetric study, Neuroimaging, monoamines, brain volumetric study, volumetric deficit, Magnetic Resonance Imaging, Humans, Amino acids, Radiology, Nuclear Medicine and imaging, Neurology (clinical), Volumetric deficit, Succinate-Semialdehyde Dehydrogenase, Cardiology and Cardiovascular Medicine
Abstract

PURPOSE: Inborn errors of neurotransmitters are rare monogenic diseases. In general, conventional neuroimaging is not useful for diagnosis. Nevertheless, advanced neuroimaging techniques could provide novel diagnosis and prognosis biomarkers. We aim to describe cerebral volumetric findings in a group of Spanish patients with neurotransmitter disorders. METHODS: Fifteen 3D T1-weighted brain images from the International Working Group on Neurotransmitter related Disorders Spanish cohort were assessed (eight with monoamine and seven with amino acid disorders). Volumes of cortical and subcortical brain structures were obtained for each patient and then compared with those of two healthy individuals matched by sex and age. RESULTS: Regardless of the underlying disease, patients showed a smaller total cerebral tissue volume, which was apparently associated with clinical severity. A characteristic volumetric deficit pattern, including the right Heschl gyrus and the bilateral occipital gyrus, was identified. In severe cases, a distinctive pattern comprised the middle and posterior portions of the right cingulate, the left superior motor area and the cerebellum. In succinate semialdehyde dehydrogenase deficiency, volumetric affection seems to worsen over life. CONCLUSION: Despite the heterogeneity and limited size of our cohort, we found novel and relevant data. Total volume deficit appears to be a marker of severity, regardless of the specific neurotransmitter disease and irrespective of the information obtained from conventional neuroimaging. Volumetric assessment of individual brain structures could provide a deeper knowledge about pathophysiology, disease severity and specific clinical traits.

Published
2022

70. Correction to: Age at disease onset and peak ammonium level rather than interventional variables predict the neurological outcome in urea cycle disorders

Author

Posset, Roland, Garcia-Cazorla, Angeles, Valayannopoulos, Vassili, Leão Teles, Elisa, Dionisi-Vici, Carlo, Brassier, Anaïs, Burlina, Alberto B., Burgard, Peter, Cortès-Saladelafont, Elisenda, Dobbelaere, Dries, Couce, Maria L., Sykut-Cegielska, Jolanta, Häberle, Johannes, Lund, Allan M., Chakrapani, Anupam, Schiff, Manuel, Walter, John H., Zeman, Jiri, Vara, Roshni, Kölker, Stefan, and Additional individual contributors of the E-IMD consortium

Published
2018
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71. Prospective Multicenter Validation of a Simple Blood Test for the Diagnosis of Glut1 Deficiency Syndrome

Author

Mochel, Fanny, Gras, Domitille, Luton, Marie-Pierre, Nizou, Manon, Giovannini, Donatella, Delattre, Caroline, Aubart, Mélodie, Barth, Magalie, De Saint-Martin, Anne, Doummar, Diane, Essid, Nouha, Garros, Alexa, Le Camus, Caroline Hachon, Hoebeke, Celia, The Tich, Sylvie Nguyen, Perivier, Maximilien, Rivera, Serge, Rolland, Anne, Roubertie, Agathe, Sarret, Catherine, Sevin, Caroline, Ville, Dorothee, Sitbon, Marc, Costa, Jean-Marc, Pons, Roser, Garcia-Cazorla, Angels, Vuillaumier, Sandrine, Petit, Vincent, Boespflug-Tanguy, Odile, De Vivo, Darryl C., Mochel, Fanny, Gras, Domitille, Luton, Marie-Pierre, Nizou, Manon, Giovannini, Donatella, Delattre, Caroline, Aubart, Mélodie, Barth, Magalie, De Saint- Martin, Anne, Doummar, Diane, Essid, Nouha, Garros, Alexa, Hachon-Le Camus, Caroline, Hoebeke, Célia, The Tich, Sylvie Nguyen, Périvier, Maximilien, Rivera, Serge, Rolland, Anne, Roubertie, Agathe, Sarret, Catherine, Sevin, Caroline, Ville, Dorothée, Sitbon, Marc, Costa, Jean-Marc, Pons, Roser, Cazorla, Angeles Garcia-, Vuillaumier-Barrot, Sandrine, Petit, Vincent, Tanguy, Odile Boespflug-, and De Vivo, Darryl C

Published
2023
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72. Assessment of intellectual impairment, health-related quality of life, and behavioral phenotype in patients with neurotransmitter related disorders: Data from the iNTD registry

Author

Stacey Tay Kiat Hong, Georg F. Hoffmann, Angeles Garcia-Cazorla, Suet-Na Wong, Jan Kulhánek, Mareike Keller, Heiko Brennenstuhl, Oya Kuseyri Hübschmann, Yilmaz Yildiz, Mari Oppebøen, Kathrin Jeltsch, Francesca Manzoni, H. Serap Sivri, Alberto Burlina, Saadet Mercimek-Andrews, Elisenda Cortès-Saladelafont, Dimitrios I. Zafeiriou, Sven F. Garbade, Thomas Opladen, Pablo Mir, Jennifer Friedman, Vincenzo Leuzzi, Joaquín Alejandro Fernández Ramos, Mario Mastrangelo, Eduardo López-Laso, Jeanette Koht, Dora Steel, Toni S. Pearson, Natalia Alexandra Julia Palacios, Filippo Manti, Thomas Lücke, Tomas Honzik, Jesus Serrano-Lomelin, Galina Stevanović, Ivana Kavecan, Cheuk-Wing Fung, Manju A. Kurian, Roser Pons, Helly Goez, and University of Heidelberg

Subjects
Succinic semialdehyde dehydrogenase deficiency, Male, Internationality, Intelligence, 0302 clinical medicine, Quality of life, Neurotransmitter deficiencies, Neurotransmitter metabolism, Registries, Child, Genetics (clinical), behavioral phenotype, cognitive impairment, intelligence, quality of life, iNTD, Psychomotor learning, 0303 health sciences, Neurotransmitter Agents, Intelligence quotient, Middle Aged, 3. Good health, neurotransmitter deficiencies, Phenotype, Cognitive impairment, Child, Preschool, Anxiety, Female, medicine.symptom, Clinical psychology, Adult, Behavioral phenotype, Adolescent, Attention span, 03 medical and health sciences, Young Adult, Genetics, medicine, Humans, Cognitive Dysfunction, 030304 developmental biology, Behavior, business.industry, Neurotransmitterdeficiencies, Infant, medicine.disease, Sepiapterin reductase deficiency, business, 030217 neurology & neurosurgery
Abstract

Inherited disorders of neurotransmitter metabolism are a group of rare diseases, which are caused by impaired synthesis, transport, or degradation of neurotransmitters or cofactors and result in various degrees of delayed or impaired psychomotor development. To assess the effect of neurotransmitter deficiencies on intelligence, quality of life, and behavior, the data of 148 patients in the registry of the International Working Group on Neurotransmitter Related Disorders (iNTD) was evaluated using results from standardized age-adjusted tests and questionnaires. Patients with a primary disorder of monoamine metabolism had lower IQ scores (mean IQ 58, range 40-100) within the range of cognitive impairment (, Dietmar Hopp Stiftung (DE); Medical Faculty of the University of Heidelberg.

Published
2021

74. Free-thiamine is a potential biomarker of thiamine transporter-2 deficiency: a treatable cause of Leigh syndrome

Author

Ortigoza-Escobar, Juan Darío, Molero-Luis, Marta, Arias, Angela, Oyarzabal, Alfonso, Darín, Niklas, Serrano, Mercedes, Garcia-Cazorla, Angels, Tondo, Mireia, Hernández, María, Garcia-Villoria, Judit, Casado, Mercedes, Gort, Laura, Mayr, Johannes A., Rodríguez-Pombo, Pilar, Ribes, Antonia, Artuch, Rafael, and Pérez-Dueñas, Belén

Published
2016
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76. The most recurrent monogenic disorders that overlap with the phenotype of Rett syndrome

Author

S. Vidal, N. Brandi, P. Pacheco, J. Maynou, G. Fernandez, C. Xiol, A. Pascual-Alonso, M. Pineda, J. Armstrong, O'Callaghan Maria del Mar, Àngels Garcia-Cazorla, Maria del Carmen Serrano Munuera, Silvia Cuso García, Monica Troncoso, Guillermo Fariña, Juan José García Peñas, Belen Gil Fournier, Soraya Ramiro León, Miriam Guitart, Neus Baena, Guiomar Perez de Nanclares, Intzane Ocio Oci, Eva Gutiérrez-Delicado, Belén Abarrategui, Eva Barroso, Fernando Santos-Simarro, Pablo Lapunzina, Francisco J. García, Juan M. Acedo, Asunción García, Miguel A. Martinez, and Antonio Martínez-Bermejo

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Methyl-CpG-Binding Protein 2, CDKL5, Rett syndrome, Genotype-phenotype correlations, SYNGAP1, Bioinformatics, RTT, Rett-like, MECP2, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Neurodevelopmental disorder, 030225 pediatrics, Rett Syndrome, medicine, Humans, STXBP1, Genetic Association Studies, Monogenic disorders, business.industry, High-Throughput Nucleotide Sequencing, General Medicine, medicine.disease, Phenotype, FOXG1, Neurodevelopmental Disorders, Mutation, Pediatrics, Perinatology and Child Health, Female, Neurology (clinical), business, 030217 neurology & neurosurgery
Abstract

Rett syndrome (RTT) is an early-onset neurodevelopmental disorder that is caused by mutations in the MECP2 gene; however, defects in other genes (CDKL5 and FOXG1) can lead to presentations that resemble classic RTT, although they are not completely identical. Here, we attempted to identify other monogenic disorders that share features of RTT. A total of 437 patients with a clinical diagnosis of RTT-like were studied; in 242 patients, a custom panel with 17 genes related to an RTT-like phenotype was run via a HaloPlex-Target-Enrichment-System. In the remaining 195 patients, a commercial TruSight-One-Sequencing-Panel was analysed. A total of 40 patients with clinical features of RTT had variants which affect gene function in six genes associated with other monogenic disorders. Twelve patients had variants in STXBP1, nine in TCF4, six in SCN2A, five in KCNQ2, four in MEF2C and four in SYNGAP1. Genetic studies using next generation sequencing (NGS) allowed us to study a larger number of genes associated with RTT-like simultaneously, providing a genetic diagnosis for a wider group of patients. These new findings provide the clinician with more information and clues that could help in the prevention of future symptoms or in pharmacologic therapy.

Published
2019

77. Betaine anhydrous in homocystinuria: results from the RoCH registry

Author

Yann Nadjar, Luis Aldámiz-Echevarría, Vassili Valayannopoulos, Vincent Rigalleau, María L. Couce, Pascal Cathebras, Dries Dobbelaere, Aline Cano, Nathalie Guffon, Lena Damaj, Manuel Schiff, Angeles Garcia-Cazorla, Virginie Levrat, Didier Eyer, Mercedes Martinez-Pardo Casanova, François Maillot, Guy Touati, Dominique Brunet, Luis Peña-Quintana, Jaime Dalmau, Sylvie Hieronimus, CHU Necker - Enfants Malades [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Hôpital Robert Debré, Bordeaux population health (BPH), Université de Bordeaux (UB)-Institut de Santé Publique, d'Épidémiologie et de Développement (ISPED)-Institut National de la Santé et de la Recherche Médicale (INSERM), Maladies RAres du DEveloppement embryonnaire et du MEtabolisme : du Phénotype au Génotype et à la Fonction - ULR 7364 (RADEME), Université de Lille-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille), and Université Francois Rabelais [Tours]

Subjects
0301 basic medicine, Male, lcsh:Medicine, 030105 genetics & heredity, chemistry.chemical_compound, 0302 clinical medicine, Betaine, Pharmacology (medical), Registries, RoCH registry, Child, Homocysteine, Genetics (clinical), biology, Interstitial lung disease, General Medicine, [SDV.MHEP.EM]Life Sciences [q-bio]/Human health and pathology/Endocrinology and metabolism, 3. Good health, Treatment Outcome, Child, Preschool, Population study, Female, Homocystinuria, France, Safety, Adult, medicine.medical_specialty, Adolescent, Efficacy, Cobalamin, 03 medical and health sciences, Young Adult, Betaine anhydrous, Efficacy, Homocystinuria, RoCH registry, Safety, Internal medicine, medicine, Humans, Adverse effect, Retrospective Studies, business.industry, Research, lcsh:R, Infant, Betaine anhydrous, medicine.disease, Cystathionine beta synthase, chemistry, Spain, Methylenetetrahydrofolate reductase, biology.protein, [SDV.SP.PHARMA]Life Sciences [q-bio]/Pharmaceutical sciences/Pharmacology, [SDV.SPEE]Life Sciences [q-bio]/Santé publique et épidémiologie, business, 030217 neurology & neurosurgery
Abstract

Background The Registry of Adult and Paediatric Patients Treated with Cystadane® – Homocystinuria (RoCH) is a non-interventional, observational, multi-centre, post-authorization safety study that aimed to identify safety of betaine anhydrous (Cystadane®) in the treatment of patients with inborn errors of homocysteine metabolism (homocystinuria) in order to minimise the treatment associated risks and establish better knowledge on its clinical use. The registry included patients of all ages with homocystinuria who were treated with betaine anhydrous in conjunction with other therapies. Clinical data were collected retrospectively from 2007 to 2013, then prospectively up to February 2014. All adverse events (AEs) reported during the study were recorded. The clinical and biological status of patients was monitored at least once a year. Results A total of 125 patients with homocystinuria (adults [> 18 years]: 50; paediatric [≤18 years]: 75) were enrolled at 29 centres in France and Spain. Patients were treated with betaine anhydrous for a mean duration of 7.4 ± 4.3 years. The median total daily dose of betaine anhydrous at the first and last study visits was 6 g/day for cystathionine β-synthase (CBS)-deficient vitamin B6 responders and 9 g/day for methylenetetrahydrofolate reductase-deficient patients, while the median daily dose increased in CBS-deficient B6 non-responders (from 6 to 9 g/day) and cobalamin metabolism-defective patients (from 3 to 6 g/day) between the first and last visits. Treatment caused a mean overall reduction of 29% in plasma homocysteine levels in the study population. A total of 277 AEs were reported during the study, of which two non-serious AEs (bad taste and headache) and one serious AE (interstitial lung disease) were considered to be drug related. Overall, betaine anhydrous was well tolerated with no major safety concerns. Conclusions Data from the RoCH registry provided real-world evidence on the clinical safety and efficacy of betaine anhydrous in the management of homocystinuria in paediatric and adult patients. Electronic supplementary material The online version of this article (10.1186/s13023-019-1036-2) contains supplementary material, which is available to authorized users.

Published
2019

78. Joubert syndrome: a model for untangling recessive disorders with extreme genetic heterogeneity

Author

Bachmann-Gagescu, R, Dempsey, J C, Phelps, I G, OʼRoak, B J, Knutzen, D M, Rue, T C, Ishak, G E, Isabella, C R, Gorden, N, Adkins, J, Boyle, E A, de Lacy, N, OʼDay, D, Alswaid, A, Ramadevi A, Radha, Lingappa, L, Lourenço, C, Martorell, L, Garcia-Cazorla, À, Ozyürek, H, Haliloğlu, G, Tuysuz, B, Topçu, M, Chance, P, Parisi, M A, Glass, I A, Shendure, J, and Doherty, D

Published
2015
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80. Implementation of second-tier tests in newborn screening for the detection of vitamin B12 related acquired and genetic disorders: results on 258,637 newborns

Author

Sonia Pajares, Aleix Navarro-Sastre, Laura Gort, Silvia Meavilla, José Antonio Arranz, Mireia del Toro, Clara Carnicer, M. Santos, Frederic Tort, Antonia Ribes, Judit García-Villoria, Rafael Artuch, José Luis Marín, Camila García-Volpe, Ana Argudo, José Manuel González de Aledo-Castillo, Rosa Fernández, R.M. López, Aida Ormazabal, Angeles Garcia-Cazorla, Institut Català de la Salut, [Pajares S] Sección de Errores Congénitos del Metabolismo IBC, Servicio de Bioquímica y Genética Molecular, Hospital Clínic de Barcelona, 08028 Barcelona, Spain. Center for Biomedical Research Network on Rare Diseases (CIBERER), Madrid, Spain. [Arranz JA, Del Toro M, Carnicer C] Unitat de Malalties Metabòliques Hereditàries, Vall d’Hebron Hospital Universitari, Barcelona, Spain. [Ormazabal A, García-Cazorla Á] Center for Biomedical Research Network on Rare Diseases (CIBERER), Madrid, Spain. Inborn Errors of Metabolism Unit, Hospital Sant Joan de Déu, Barcelona, Spain. [Navarro-Sastre A] Sección de Errores Congénitos del Metabolismo IBC, Servicio de Bioquímica y Genética Molecular, Hospital Clínic de Barcelona, 08028 Barcelona, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects
Newborn screening, Pediatrics, medicine.medical_specialty, Anemia, Methylmalonic acidemia, Methylmalonic acid, Congenital, Hereditary, and Neonatal Diseases and Abnormalities [DISEASES], Homocystinuria, Cobalamin, enfermedades y anomalías neonatales congénitas y hereditarias::enfermedades genéticas congénitas::alteraciones congénitas del metabolismo::alteraciones congénitas del metabolismo de los aminoácidos::acidemia propiónica [ENFERMEDADES], 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, 030225 pediatrics, medicine, Congenital, Hereditary, and Neonatal Diseases and Abnormalities::Genetic Diseases, Inborn::Metabolism, Inborn Errors::Amino Acid Metabolism, Inborn Errors::Propionic Acidemia [DISEASES], Infants nadons, Pharmacology (medical), Vitamin B12, Propionic acidemia, Homocysteine, Genetics (clinical), business.industry, Aminoàcids - Metabolisme - Trastorns, personas::Grupos de Edad::lactante::recién nacido [DENOMINACIONES DE GRUPOS], nutritional and metabolic diseases, General Medicine, enfermedades y anomalías neonatales congénitas y hereditarias [ENFERMEDADES], medicine.disease, Persons::Age Groups::Infant::Infant, Newborn [NAMED GROUPS], Second-tier test, Vitamin B12 deficiency, chemistry, Methylcitric acid, Medicine, Metabolisme, Errors congènits del, business, 030217 neurology & neurosurgery
Abstract

Background Alteration of vitamin B12 metabolism can be genetic or acquired, and can result in anemia, failure to thrive, developmental regression and even irreversible neurologic damage. Therefore, early diagnosis and intervention is critical. Most of the neonatal cases with acquired vitamin B12 deficiency have been detected by clinical symptoms and only few of them trough NBS programs. We aim to assess the usefulness of the second-tier test: methylmalonic acid (MMA), methylcitric acid (MCA) and homocysteine (Hcys) in our newborn screening program and explore the implications on the detection of cobalamin (vitamin B12) related disorders, both genetic and acquired conditions. Methods A screening strategy using the usual primary markers followed by the analysis of MMA, MCA and Hcys as second tier-test in the first dried blood spot (DBS) was developed and evaluated. Results During the period 2015–2018 a total of 258,637 newborns were screened resulting in 130 newborns with acquired vitamin B12 deficiency (incidence 1:1989), 19 with genetic disorders (incidence 1:13,613) and 13 were false positive. No false negatives were notified. Concerning the second-tier test, the percentage of cases with MMA above the cut-off levels, both for genetic and acquired conditions was very similar (58% and 60%, respectively). Interestingly, the percentage of cases with increased levels of Hcys was higher in acquired conditions than in genetic disorders (87% and 47%, respectively). In contrast, MCA was high only in 5% of the acquired conditions versus in 53% of the genetic disorders, and it was always very high in all patients with propionic acidemia. Conclusions When screening for methylmalonic acidemia and homocystinuria, differential diagnosis with acquired vitamin B12 deficiency should be done. The results of our strategy support the inclusion of this acquired condition in the NBS programs, as it is easily detectable and allows the adoption of corrective measures to avoid the consequences of its deficiency.

Published
2021

83. Circulating Cell-Free Mitochondrial DNA in Cerebrospinal Fluid as a Biomarker for Mitochondrial Diseases

Author

Trifunov, Selena, primary, Paredes-Fuentes, Abraham J, additional, Badosa, Carmen, additional, Codina, Anna, additional, Montoya, Julio, additional, Ruiz-Pesini, Eduardo, additional, Jou, Cristina, additional, Garrabou, Glòria, additional, Grau-Junyent, Josep M, additional, Yubero, Dèlia, additional, Montero, Raquel, additional, Muchart, Jordi, additional, Ortigoza-Escobar, Juan D, additional, O’Callaghan, Maria M, additional, Nascimento, Andrés, additional, Català, Albert, additional, Garcia-Cazorla, Àngels, additional, Jimenez-Mallebrera, Cecilia, additional, and Artuch, Rafael, additional

Published
2021
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84. Copper Toxicity Associated With an ATP7A-Related Complex Phenotype

Author

Natera-de Benito, Daniel, primary, Sola, Abel, additional, Sousa, Paulo Rego, additional, Boronat, Susana, additional, Expósito-Escudero, Jessica, additional, Carrera-García, Laura, additional, Ortez, Carlos, additional, Jou, Cristina, additional, Muchart, Jordi, additional, Rebollo, Monica, additional, Armstrong, Judith, additional, Colomer, Jaume, additional, Garcia-Cazorla, Àngels, additional, Hoenicka, Janet, additional, Palau, Francesc, additional, and Nascimento, Andres, additional

Published
2021
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85. Brain MR patterns in inherited disorders of monoamine neurotransmitters: An analysis of 70 patients

Author

Hübschmann OK, Mohr A, Friedman J, Manti F, Horvath G, Cortés-Saladelafont E, Mercimek-Andrews S, Yildiz Y, Pons R, Kulhánek J, Oppebøen M, Koht JA, Podzamczer-Valls I, Domingo-Jimenez R, Ibáñez S, Alcoverro-Fortuny O, Gómez-Alemany T, de Castro P, Alfonsi C, Zafeiriou DI, López-Laso E, Guder P, Santer R, Honzík T, Hoffmann GF, Garbade SF, Sivri HS, Leuzzi V, Jeltsch K, Garcia-Cazorla A, Opladen T, Harting I, International Working Group on Neurotransmitter Related Disorders, [Kuseyri Hübschmann O] Department of Child Neurology and Metabolic Disorders, University Children's Hospital, Heidelberg, Germany. [Mohr A] Department of Neuroradiology, University Hospital Heidelberg, Heidelberg, Germany. [Friedman J] UCSD Departments of Neuroscience and Pediatrics, Rady Children's Hospital Division of Neurology, Rady Children's Institute for Genomic Medicine, San Diego, California. [Manti F] Unit of Child Neurology and Psychiatry, Department of Human Neuroscience, Sapienza, University of Rome, Rome, Italy. [Horvath G] University of British Columbia, Department of Pediatrics, Division of Biochemical Genetics, BC Children's Hospital, Vancouver, British Columbia, Canada. [Cortès-Saladelafont E] Inborn Errors of Metabolism Unit, Department of Neurology, Institut de Recerca Sant Joan de Déu and CIBERER-ISCIII, Barcelona, Spain. Unit of Pediatric Neurology and Metabolic Disorders, Department of Pediatrics, Hospital Germans Trias i Pujol and Faculty of Medicine,Universitat Autònoma de Barcelona, Barcelona, Spain. [Alcoverro-Fortuny O, Gómez-Alemany T] Hospital General de Granollers, Granollers, Spain, and Hospital General de Granollers

Subjects
Male, Pathology, Movement disorders, Neurotransmissors, diagnóstico::técnicas y procedimientos diagnósticos::diagnóstico::técnicas y procedimientos diagnósticos::técnicas diagnósticas neurológicas::neuroimágenes [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], monoamines, Child, Genetics (clinical), 0303 health sciences, Brain Mapping, 030305 genetics & heredity, Inherited neurotransmitter disorders, monoamines, MRI, tetrahydrobiopterin deficiency, inherited neurotransmitter disorders, Brain, watershed injury, Middle Aged, Magnetic Resonance Imaging, medicine.anatomical_structure, Child, Preschool, Female, medicine.symptom, Adult, medicine.medical_specialty, Adolescent, Encephalopathy, Diagnosis::Diagnostic Techniques and Procedures::Diagnosis::Diagnostic Techniques and Procedures::Diagnostic Techniques, Neurological::Neuroimaging [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT], Grey matter, 03 medical and health sciences, Young Adult, Atrophy, enfermedades y anomalías neonatales congénitas y hereditarias::enfermedades genéticas congénitas::alteraciones congénitas del metabolismo::alteraciones congénitas del metabolismo de los aminoácidos::enfermedades y anomalías neonatales congénitas y hereditarias::enfermedades genéticas congénitas::alteraciones congénitas del metabolismo::fenilcetonurias [ENFERMEDADES], Neuroimaging, Genetics, medicine, Humans, Tetrahydrobiopterin deficiency, Amino Acid Metabolism, Inborn Errors, Nervous System Diseases::Central Nervous System Diseases::Brain Diseases::Brain Diseases, Metabolic [DISEASES], 030304 developmental biology, Retrospective Studies, enfermedades del sistema nervioso::enfermedades del sistema nervioso central::enfermedades cerebrales::enfermedades cerebrales metabólicas [ENFERMEDADES], Inherited neurotransmitter disorders, Sistema nerviós - Malalties, Tyrosine hydroxylase, business.industry, Ressonància magnètica, Infant, medicine.disease, Monoamine neurotransmitter, Congenital, Hereditary, and Neonatal Diseases and Abnormalities::Genetic Diseases, Inborn::Metabolism, Inborn Errors::Amino Acid Metabolism, Inborn Errors::Congenital, Hereditary, and Neonatal Diseases and Abnormalities::Genetic Diseases, Inborn::Metabolism, Inborn Errors::Phenylketonurias [DISEASES], business
Abstract

RM; Trastornos hereditarios de neurotransmisores; Monoaminas; Deficiencia de tetrahidrobiopterina RM; Trastorns dels neurotransmissors heretats; Monoamines; Deficiència de tetrahidrobiopterina MRI; Inherited neurotransmitter disorders; Monoamines; Tetrahydrobiopterin deficiency; Inherited monoamine neurotransmitter disorders (iMNDs) are rare disorders with clinical manifestations ranging from mild infantile hypotonia, movement disorders to early infantile severe encephalopathy. Neuroimaging has been reported as non-specific. We systematically analyzed brain MRIs in order to characterize and better understand neuroimaging changes and to re-evaluate the diagnostic role of brain MRI in iMNDs. 81 MRIs of 70 patients (0.1-52.9 years, 39 patients with tetrahydrobiopterin deficiencies, 31 with primary disorders of monoamine metabolism) were retrospectively analyzed and clinical records reviewed. 33/70 patients had MRI changes, most commonly atrophy (n = 24). Eight patients, six with dihydropteridine reductase deficiency (DHPR), had a common pattern of bilateral parieto-occipital and to a lesser extent frontal and/or cerebellar changes in arterial watershed zones. Two patients imaged after acute severe encephalopathy had signs of profound hypoxic-ischemic injury and a combination of deep gray matter and watershed injury (aromatic l-amino acid decarboxylase (AADCD), tyrosine hydroxylase deficiency (THD)). Four patients had myelination delay (AADCD; THD); two had changes characteristic of post-infantile onset neuronal disease (AADCD, monoamine oxidase A deficiency), and nine T2-hyperintensity of central tegmental tracts. iMNDs are associated with MRI patterns consistent with chronic effects of a neuronal disorder and signs of repetitive injury to cerebral and cerebellar watershed areas, in particular in DHPRD. These will be helpful in the (neuroradiological) differential diagnosis of children with unknown disorders and monitoring of iMNDs. We hypothesize that deficiency of catecholamines and/or tetrahydrobiopterin increase the incidence of and the CNS susceptibility to vascular dysfunction.

Published
2021

86. GRIN database: A unified and manually curated repertoire of GRIN variants

Author

García-Recio A, Santos-Gómez A, Soto D, Julià-Palacios NA, Garcia-Cazorla A, Altafaj X, and Olivella M

Subjects
disease-associated mutations, intellectual disability, epilepsy, NMDA receptors
Abstract

Glutamatergic neurotransmission is crucial for brain development, wiring neuronal function, and synaptic plasticity mechanisms. Recent genetic studies showed the existence of autosomal dominant de novo GRIN gene variants associated with GRIN-related disorders (GRDs), a rare pediatric neurological disorder caused by N-methyl- d-aspartate receptor (NMDAR) dysfunction. Notwithstanding, GRIN variants identification is exponentially growing and their clinical, genetic, and functional annotations remain highly fragmented, representing a bottleneck in GRD patient's stratification. To shorten the gap between GRIN variant identification and patient stratification, we present the GRIN database (GRINdb), a publicly available, nonredundant, updated, and curated database gathering all available genetic, functional, and clinical data from more than 4000 GRIN variants. The manually curated GRINdb outputs on a web server, allowing query and retrieval of reported GRIN variants, and thus representing a fast and reliable bioinformatics resource for molecular clinical advice. Furthermore, the comprehensive mapping of GRIN variants' genetic and clinical information along NMDAR structure revealed important differences in GRIN variants' pathogenicity and clinical phenotypes, shedding light on GRIN-specific fingerprints. Overall, the GRINdb and web server is a resource for molecular stratification of GRIN variants, delivering clinical and investigational insights into GRDs. GRINdb is accessible at http://lmc.uab.es/grindb.

Published
2021

89. Disease-associated GRIN protein truncating variants trigger NMDA receptor loss-of-function

Author

Santos-Gómez A, Miguez-Cabello F, García-Recio A, Locubiche S, García-Díaz R, Soto V, Guerrero-López R, Julià-Palacios NA, Ciruela F, Garcia-Cazorla A, Soto D, Olivella M, and Altafaj X

Abstract

De novo GRIN variants, encoding for the ionotropic glutamate NMDA receptor subunits, have been recently associated with GRIN-related disorders, a group of rare paediatric encephalopathies. Current investigational and clinical efforts are focused to functionally stratify GRIN variants, towards precision therapies of this primary disturbance of glutamatergic transmission that affects neuronal function and brain. In the present study, we aimed to comprehensively delineate the functional outcomes and clinical phenotypes of GRIN protein truncating variants (PTVs)-accounting for ~20% of disease-associated GRIN variants-hypothetically provoking NMDAR hypofunctionality. To tackle this question, we created a comprehensive GRIN PTVs variants database compiling a cohort of nine individuals harbouring GRIN PTVs, together with previously identified variants, to build-up an extensive GRIN PTVs repertoire composed of 293 unique variants. Genotype-phenotype correlation studies were conducted, followed by cell-based assays of selected paradigmatic GRIN PTVs and their functional annotation. Genetic and clinical phenotypes meta-analysis revealed that heterozygous GRIN1, GRIN2C, GRIN2D, GRIN3A and GRIN3B PTVs are non-pathogenic. In contrast, heterozygous GRIN2A and GRIN2B PTVs are associated with specific neurological clinical phenotypes in a subunit- and domain-dependent manner. Mechanistically, cell-based assays showed that paradigmatic pathogenic GRIN2A and GRIN2B PTVs result on a decrease of NMDAR surface expression and NMDAR-mediated currents, ultimately leading to NMDAR functional haploinsufficiency. Overall, these findings contribute to delineate GRIN PTVs genotype-phenotype association and GRIN variants stratification. Functional studies showed that GRIN2A and GRIN2B pathogenic PTVs trigger NMDAR hypofunctionality, and thus accelerate therapeutic decisions for this neurodevelopmental condition.

Published
2021

90. An Integrative Approach to Predict Phenotypic Severity in Nonketotic Hyperglycinemia

Author

René Santer, Oya Kuseyri Hübschmann, Tomas Honzik, Georg F. Hoffmann, Sven F. Garbade, Thomas Opladen, Jan Kulhánek, Toni S. Pearson, Elisenda Cortès-Saladelafont, Salvador Ibáñez, Dimitrios I. Zafeiriou, Kathrin Jeltsch, Mireia Olivella, Gabriella Horvath, M. Concepción García-Jiménez, Alice Kuster, Angeles Garcia-Cazorla, Philipp Guder, and Natalia Alexandra Julia Palacios

Subjects
History, medicine.medical_specialty, Polymers and Plastics, Hyperglycinemia, business.industry, Clinical course, International working group, medicine.disease, Phenotype, Industrial and Manufacturing Engineering, Potential conflict, Clinical trial, Internal medicine, medicine, Christian ministry, Business and International Management, Age of onset, business
Abstract

Background: Nonketotic hyperglycinemia (NKH) is a inherited neurometabolic disorder with variable clinical course and severity, in a spectrum ranging from infantile epileptic encephalopathy to psychiatric disorders. A precise phenotypic characterization and an evaluation of predictive approaches are needed. We report the results of the patient registry of the International Working Group on Neurotransmitter related Disorders (iNTD). Methods: The iNTD patient registry is a multicenter, uncontrolled, non-randomized, open, unblinded observational study (registered on DRKS, DRKS00007878). Longitudinal clinical and biochemical data of 25 individuals with NKH were studied with in silico analyses, pathogenicity scores and molecular modeling of GLDC and AMT variants. Findings: Age of onset (p=0 · 004) and diagnosis are earlier in life in severe NKH( p=0 · 005). Presenting symptoms affect the age at diagnosis. Psychiatric problems occur predominantly in attenuated NKH. Onset-age ≥3 months (66% specificity, 100% sensitivity, AUC = 0·87) and cerebrospinal fluid (CSF)/plasma glycine ratio ≤0 · 09 (57% specificity, 100% sensitivity, AUC = 0·88) are sensitive indicators for attenuated NKH while CSF glycine concentration ≥116 · 5 µmol/L (100% specificity, 93% sensitivity, AUC = 0·97) and CSF/plasma glycine ratio ≥0 · 15 15 (100% specificity, 64% sensitivity, AUC = 0·88) are specific for severe forms. A ratio threshold of 0 · 128 discriminates the overlapping range. In our study, we present ten new GLDC variants, two mild variants resulting in attenuated phenotype. Two severe variants and a combination of one mild and one severe variant lead to severe phenotype. Interpretation: This study widens the phenotypic spectrum of attenuated NKH and expands the number of pathogenic variants. The multiparametric approach provides a promising tool to predict disease severity, helping to improve clinical management and decision-making strategies. Trial Registration: This study was registered German Clinical Trials Register, https://www.drks.de, DRKS00007878). Funding: Ministry of Health of the Czech Republic (RVO-VFN 64165 GJIH-0599-00-7-846, ProgresQ26/LF1), FIS P118/00111 and PI19/00348 “Instituto de Salud Carlos III”, “Fondo Europeo de desarrollo regional (FEDER)”, and Dietmar Hopp Foundation. Declaration of Interest: A.G.C. has received teaching honorarium from PTC Therapeutics GT, Inc. G.F.H. receives teaching as well as consultancy honorarium from PTC Therapeutics GT, Inc. O.K.H. has received teaching honorarium from PTC Therapeutics GT, Inc. T.O. receives teaching honorarium and research support from PTC. GFH has received honoraria as a speaker from Takeda and consultancy honoraria from PTC Therapeutics International GT. T.S.P receives consulting honoraria from Teva Pharmaceuticals. The other authors declare no potential conflict of interest. Ethical Approval: iNTD registry study was approved by the Institutional Research Ethics Board (IRB) Heidelberg University Hospital (S-471/2014)

Published
2021

91. Choosing Strategies to Deal with Artifactual EEG Data in Children with Cognitive Impairment

Author

Tost A, Migliorelli C, Bachiller A, Medina-Rivera IF, Romero S, Garcia-Cazorla A, and Mañanas MA

Subjects
accelerometer, energy function, Rett Syndrome (RTT), electroencephalography (EEG), artifact detection, data distribution
Abstract

Rett syndrome is a disease that involves acute cognitive impairment and, consequently, a complex and varied symptomatology. This study evaluates the EEG signals of twenty-nine patients and classify them according to the level of movement artifact. The main goal is to achieve an artifact rejection strategy that performs well in all signals, regardless of the artifact level. Two different methods have been studied: one based on the data distribution and the other based on the energy function, with entropy as its main component. The method based on the data distribution shows poor performance with signals containing high amplitude outliers. On the contrary, the method based on the energy function is more robust to outliers. As it does not depend on the data distribution, it is not affected by artifactual events. A double rejection strategy has been chosen, first on a motion signal (accelerometer or EEG low-pass filtered between 1 and 10 Hz) and then on the EEG signal. The results showed a higher performance when working combining both artifact rejection methods. The energy-based method, to isolate motion artifacts, and the data-distribution-based method, to eliminate the remaining lower amplitude artifacts were used. In conclusion, a new method that proves to be robust for all types of signals is designed.

Published
2021

93. Paradigmatic De Novo GRIN1 Variants Recapitulate Pathophysiological Mechanisms Underlying GRIN1-Related Disorder Clinical Spectrum

Author

Santos-Gómez A, Miguez-Cabello F, Julià-Palacios NA, García-Navas D, Soto-Insuga V, García-Peñas JJ, Fuentes P, Ibáñez-Micó S, Cuesta L, Cancho R, Andreo-Lillo P, Gutiérrez-Aguilar G, Alonso-Luengo O, Málaga I, Hedrera-Fernández A, Garcia-Cazorla A, Soto D, Olivella M, and Altafaj X

Subjects
glutamatergic neurotransmission, neurodevelopmental disorders, GRIN-related disorders, NMDA receptors
Abstract

BACKGROUND: GRIN-related disorders (GRD), the so-called grinpathies, is a group of rare encephalopathies caused by mutations affecting GRIN genes (mostly GRIN1, GRIN2A and GRIN2B genes), which encode for the GluN subunit of the N-methyl D-aspartate (NMDA) type ionotropic glutamate receptors. A growing number of functional studies indicate that GRIN-encoded GluN1 subunit disturbances can be dichotomically classified into gain- and loss-of-function, although intermediate complex scenarios are often present. METHODS: In this study, we aimed to delineate the structural and functional alterations of GRIN1 disease-associated variants, and their correlations with clinical symptoms in a Spanish cohort of 15 paediatric encephalopathy patients harbouring these variants. RESULTS: Patients harbouring GRIN1 disease-associated variants have been clinically deeply-phenotyped. Further, using computational and in vitro approaches, we identified different critical checkpoints affecting GluN1 biogenesis (protein stability, subunit assembly and surface trafficking) and/or NMDAR biophysical properties, and their association with GRD clinical symptoms. CONCLUSIONS: Our findings show a strong correlation between GRIN1 variants-associated structural and functional outcomes. This structural-functional stratification provides relevant insights of genotype-phenotype association, contributing to future precision medicine of GRIN1-related encephalopathies.

Published
2021

94. Assessment of intellectual impairment, health-related quality of life, and behavioral phenotype in patients with neurotransmitter related disorders: Data from the iNTD registry

Author

Keller, Mareike Brennenstuhl, Heiko Huebschmann, Oya Kuseyri and Manti, Filippo Julia Palacios, Natalia Alexandra Friedman, Jennifer Yildiz, Yilmaz Koht, Jeanette Aimee Wong, Suet-Na and Zafeiriou, Dimitrios I. Lopez-Laso, Eduardo Pons, Roser and Kulhanek, Jan Jeltsch, Kathrin Serrano-Lomelin, Jesus and Garbade, Sven F. Opladen, Thomas Goez, Helly Burlina, Alberto Cortes-Saladelafont, Elisenda Fernandez Ramos, Joaquin Alejandro Garcia-Cazorla, Angeles Hoffmann, Georg F. Kiat Hong, Stacey Tay Honzik, Tomas Kavecan, Ivana Kurian, Manju A. Leuzzi, Vincenzo Luecke, Thomas Manzoni, Francesca and Mastrangelo, Mario Mercimek-Andrews, Saadet Mir, Pablo and Oppeboen, Mari Pearson, Toni S. Sivri, H. Serap Steel, Dora and Stevanovic, Galina Fung, Cheuk-Wing Neurotransmitter Related Disorders

Abstract

Inherited disorders of neurotransmitter metabolism are a group of rare diseases, which are caused by impaired synthesis, transport, or degradation of neurotransmitters or cofactors and result in various degrees of delayed or impaired psychomotor development. To assess the effect of neurotransmitter deficiencies on intelligence, quality of life, and behavior, the data of 148 patients in the registry of the International Working Group on Neurotransmitter Related Disorders (iNTD) was evaluated using results from standardized age-adjusted tests and questionnaires. Patients with a primary disorder of monoamine metabolism had lower IQ scores (mean IQ 58, range 40-100) within the range of cognitive impairment (

Published
2021

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