Your search keyword '"Neus Baena"' showing total 45 results

1. Novel 14q32.2 paternal deletion encompassing the whole DLK1 gene associated with Temple syndrome

Author

Neus Baena, David Monk, Cinthia Aguilera, Mario F. Fraga, Agustín F. Fernández, Elisabeth Gabau, Raquel Corripio, Nuria Capdevila, Juan Pablo Trujillo, Anna Ruiz, and Miriam Guitart

Subjects

Temple syndrome (TS14), Methylation, DLK1, Deletion, DMR, Medicine, Genetics, QH426-470

Abstract

Abstract Background Temple syndrome (TS14) is a rare imprinting disorder caused by maternal UPD14, imprinting defects or paternal microdeletions which lead to an increase in the maternal expressed genes and a silencing the paternally expressed genes in the 14q32 imprinted domain. Classical TS14 phenotypic features include pre- and postnatal short stature, small hands and feet, muscular hypotonia, motor delay, feeding difficulties, weight gain, premature puberty along and precocious puberty. Methods An exon array comparative genomic hybridization was performed on a patient affected by psychomotor and language delay, muscular hypotonia, relative macrocephaly, and small hand and feet at two years old. At 6 years of age, the proband presented with precocious thelarche. Genes dosage and methylation within the 14q32 region were analyzed by MS-MLPA. Bisulfite PCR and pyrosequencing were employed to quantification methylation at the four known imprinted differentially methylated regions (DMR) within the 14q32 domain: DLK1 DMR, IG-DMR, MEG3 DMR and MEG8 DMR. Results The patient had inherited a 69 Kb deletion, encompassing the entire DLK1 gene, on the paternal allele. Relative hypermethylation of the two maternally methylated intervals, DLK1 and MEG8 DMRs, was observed along with normal methylation level at IG-DMR and MEG3 DMR, resulting in a phenotype consistent with TS14. Additional family members with the deletion showed modest methylation changes at both the DLK1 and MEG8 DMRs consistent with parental transmission. Conclusion We describe a girl with clinical presentation suggestive of Temple syndrome resulting from a small paternal 14q32 deletion that led to DLK1 whole-gene deletion, as well as hypermethylation of the maternally methylated DLK1-DMR.

Published

2024

2. Case report: Identification of a novel variant p.Gly215Arg in the CHN1 gene causing Moebius syndrome

Author

Carmen Manso-Bazús, Nino Spataro, Elisabeth Gabau, Viviana P. Beltrán-Salazar, Juan Pablo Trujillo-Quintero, Nuria Capdevila, Anna Brunet-Vega, Neus Baena, A Arockia Jeyaprakash, Victor Martinez-Glez, and Anna Ruiz

Subjects

moebius syndrome, genetic diagnosis, CHN1, novel variant, congenital dysinnervation syndromes, Genetics, QH426-470

Abstract

Background: Moebius Syndrome (MBS) is a rare congenital neurological disorder characterized by paralysis of facial nerves, impairment of ocular abduction and other variable abnormalities. MBS has been attributed to both environmental and genetic factors as potential causes. Until now only two genes, PLXND1 and REV3L have been identified to cause MBS.Results: We present a 9-year-old male clinically diagnosed with MBS, presenting facial palsy, altered ocular mobility, microglossia, dental anomalies and congenital torticollis. Radiologically, he lacks both abducens nerves and shows altered symmetry of both facial and vestibulocochlear nerves. Whole-exome sequence identified a de novo missense variant c.643G>A; p.Gly215Arg in CHN1, encoding the α2-chimaerin protein. The p.Gly215Arg variant is located in the C1 domain of CHN1 where other pathogenic gain of function variants have been reported. Bioinformatic analysis and molecular structural modelling predict a deleterious effect of the missense variant on the protein function.Conclusion: Our findings support that pathogenic variants in the CHN1 gene may be responsible for different cranial congenital dysinnervation syndromes, including Moebius and Duane retraction syndromes. We propose to include CHN1 in the genetic diagnoses of MBS.

Published

2024

3. Genetic testing for familial hyperparathyroidism: clinical-genetic profile in a Mediterranean cohort

Author

Isabel Mazarico-Altisent, Ismael Capel, Neus Baena, Maria Rosa Bella-Cueto, Santi Barcons, Xavier Guirao, Rocío Pareja, Andreea Muntean, Valeria Arsentales, Assumpta Caixàs, and Mercedes Rigla

Subjects

parathyroid, primary hyperparathyroidism, multiple endocrine neoplasia type 1, multiple endocrine neoplasia type 4, cyclin-dependent kinase inhibitors, familial hyperparathyroidism, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

BackgroundApproximately 10% of primary hyperparathyroidism cases are hereditary, due to germline mutations in certain genes. Although clinically relevant, a systematized genetic diagnosis is missing due to a lack of firm evidence regarding individuals to test and which genes to evaluate.MethodsA customized gene panel (AIP, AP2S1, CASR, CDC73, CDKN1A, CDKN1B, CDKN2B, CDKN2C, GCM2, GNA11, MEN1, PTH, RET, and TRPV6) was performed in 40 patients from the Mediterranean area with suspected familial hyperparathyroidism (≤45 years of age, family history, high-risk histology, associated tumour, multiglandular disease, or recurrent hyperparathyroidism). We aimed to determine the prevalence of germline variants in these patients, to clinically characterize the probands and their relatives, and to compare disease severity in carriers versus those with a negative genetic test.ResultsGermline variants were observed in 9/40 patients (22.5%): 2 previously unknown pathogenic/likely pathogenic variants of CDKN1B (related to MEN4), 1 novel variant of uncertain significance of CDKN2C, 4 variants of CASR (3 pathogenic/likely pathogenic variants and 1 variant of uncertain significance), and 2 novel variants of uncertain significance of TRPV6. Familial segregation studies allowed diagnosis and early treatment of PHPT in first-degree relatives of probands.ConclusionThe observed prevalence of germline variants in the Mediterranean cohort under study was remarkable and slightly higher than that seen in other populations. Genetic screening for suspected familial hyperparathyroidism allows the early diagnosis and treatment of PHPT and other related comorbidities. We recommend genetic testing for patients with primary hyperparathyroidism who present with high-risk features.

Published

2023

4. New genes involved in Angelman syndrome-like: Expanding the genetic spectrum

Author

Cinthia Aguilera, Elisabeth Gabau, Ariadna Ramirez-Mallafré, Carme Brun-Gasca, Jana Dominguez-Carral, Veronica Delgadillo, Steve Laurie, Sophia Derdak, Natàlia Padilla, Xavier de la Cruz, Núria Capdevila, Nino Spataro, Neus Baena, Miriam Guitart, and Anna Ruiz

Subjects

Medicine, Science

Abstract

Angelman syndrome (AS) is a neurogenetic disorder characterized by severe developmental delay with absence of speech, happy disposition, frequent laughter, hyperactivity, stereotypies, ataxia and seizures with specific EEG abnormalities. There is a 10–15% of patients with an AS phenotype whose genetic cause remains unknown (Angelman-like syndrome, AS-like). Whole-exome sequencing (WES) was performed on a cohort of 14 patients with clinical features of AS and no molecular diagnosis. As a result, we identified 10 de novo and 1 X-linked pathogenic/likely pathogenic variants in 10 neurodevelopmental genes (SYNGAP1, VAMP2, TBL1XR1, ASXL3, SATB2, SMARCE1, SPTAN1, KCNQ3, SLC6A1 and LAS1L) and one deleterious de novo variant in a candidate gene (HSF2). Our results highlight the wide genetic heterogeneity in AS-like patients and expands the differential diagnosis.

Published

2021

5. Novel intragenic deletions within the UBE3A gene in two unrelated patients with Angelman syndrome: case report and review of the literature

Author

Cinthia Aguilera, Marina Viñas-Jornet, Neus Baena, Elisabeth Gabau, Concepción Fernández, Nuria Capdevila, Sanja Cirkovic, Adrijan Sarajlija, Marijana Miskovic, Danijela Radivojevic, Anna Ruiz, and Miriam Guitart

Subjects

Angelman syndrome (AS), UBE3A, Intragenic deletions, MLPA, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Patients with Angelman syndrome (AS) are affected by severe intellectual disability with absence of speech, distinctive dysmorphic craniofacial features, ataxia and a characteristic behavioral phenotype. AS is caused by the lack of expression in neurons of the UBE3A gene, which is located in the 15q11.2-q13 imprinted region. Functional loss of UBE3A is due to 15q11.2-q13 deletion, mutations in the UBE3A gene, paternal uniparental disomy and genomic imprinting defects. Case presentation We report here two patients with clinical features of AS referred to our hospital for clinical follow-up and genetic diagnosis. Methylation Specific-Multiplex Ligation-Dependent Probe Amplification (MS-MLPA) of the 15q11.2-q13 region was carried out in our laboratory as the first diagnostic tool detecting two novel UBE3A intragenic deletions. Subsequently, the MLPA P336-A2 kit was used to confirm and determine the size of the UBE3A deletion in the two patients. A review of the clinical features of previously reported patients with whole UBE3A gene or partial intragenic deletions is presented here together with these two new patients. Conclusion Although rare, UBE3A intragenic deletions may represent a small fraction of AS patients without a genetic diagnosis. Testing for UBE3A intragenic exonic deletions should be performed in those AS patients with a normal methylation pattern and no mutations in the UBE3A gene.

Published

2017

6. KIF6 gene as a pharmacogenetic marker for lipid-lowering effect in statin treatment.

Author

Cristina Ruiz-Iruela, Ariadna Padró-Miquel, Xavier Pintó-Sala, Neus Baena-Díez, Assumpta Caixàs-Pedragós, Roser Güell-Miró, Rosa Navarro-Badal, Xavier Jusmet-Miguel, Pilar Calmarza, José Luis Puzo-Foncilla, Pedro Alía-Ramos, and Beatriz Candás-Estébanez

Subjects

Medicine, Science

Abstract

INTRODUCTION:The therapeutic response to statins has a high interindividual variability with respect to reductions in plasma LDL-cholesterol (c-LDL) and increases in HDL cholesterol (c-HDL). Many studies suggest that there is a relationship between the rs20455 KIF6 gene variant (c.2155T> C, Trp719Arg) and a lower risk of cardiovascular disease in patients being treated with statins. AIM:The aim of this study was to investigate whether or not the c.2155T> C KIF6 gene variant modulates the hypercholesteremic effects of treatment with simvastatin, atorvastatin, or rosuvastatin. MATERIALS AND METHODS:This was a prospective, observational and multicenter study. Three hundred and forty-four patients who had not undergone prior lipid-lowering treatment were recruited. Simvastatin, atorvastatin or rosuvastatin were administered. Lipid profiles and multiple clinical and biochemical variables were assessed before and after treatment. RESULTS:The c.2155T> C variant of the KIF6 gene was shown to influence physiological responses to treatment with simvastatin and atorvastatin. Patients who were homozygous for the c.2155T> C variant (CC genotype, ArgArg) had a 7.0% smaller reduction of LDL cholesterol levels (p = 0.015) in response to hypolipidemic treatment compared to patients with the TT (TrpTrp) or CT (TrpArg) genotype. After pharmacological treatment with rosuvastatin, patients carrying the genetic variant had an increase in c-HDL that was 21.9% lower compared to patients who did not carry the variant (p = 0.008). CONCLUSION:Being a carrier of the c.2155T> C variant of the KIF6 gene negatively impacts patient responses to simvastatin, atorvastatin or rosuvastatin in terms of lipid lowering effect. Increasing the intensity of hypolipidemic therapy may be advisable for patients who are positive for the c.2155T> C variant.

Published

2018

7. Variabilidad fenotípica en 13 casos de deleción 16p11.2

Author

Diana Rodà, Elisabeth Gabau, Neus Baena, and Miriam Guitart

Subjects

Pediatrics, RJ1-570

Published

2018

8. Phenotype variability in thirteen 16p11.2 deletion patients

Author

Diana Rodà, Elisabeth Gabau, Neus Baena, and Miriam Guitart

Subjects

Pediatrics, RJ1-570

Published

2018

9. Lack of Postprandial Peak in Brain-Derived Neurotrophic Factor in Adults with Prader-Willi Syndrome.

Author

Marta Bueno, Susanna Esteba-Castillo, Ramon Novell, Olga Giménez-Palop, Ramon Coronas, Elisabeth Gabau, Raquel Corripio, Neus Baena, Marina Viñas-Jornet, Míriam Guitart, David Torrents-Rodas, Joan Deus, Jesús Pujol, Mercedes Rigla, and Assumpta Caixàs

Subjects

Medicine, Science

Abstract

Prader-Willi syndrome (PWS) is characterized by severe hyperphagia. Brain-derived neurotrophic factor (BDNF) and leptin are reciprocally involved in energy homeostasis.To analyze the role of BDNF and leptin in satiety in genetic subtypes of PWS.Experimental study.University hospital.90 adults: 30 PWS patients; 30 age-sex-BMI-matched obese controls; and 30 age-sex-matched lean controls.Subjects ingested a liquid meal after fasting ≥10 hours.Leptin and BDNF levels in plasma extracted before ingestion and 30', 60', and 120' after ingestion. Hunger, measured on a 100-point visual analogue scale before ingestion and 60' and 120' after ingestion.Fasting BDNF levels were lower in PWS than in controls (p = 0.05). Postprandially, PWS patients showed only a truncated early peak in BDNF, and their BDNF levels at 60' and 120' were lower compared with lean controls (p

Published

2016

10. High Performance of a Dominant/X-Linked Gene Panel in Patients with Neurodevelopmental Disorders

Author

Nino Spataro, Juan Pablo Trujillo-Quintero, Carmen Manso, Elisabeth Gabau, Nuria Capdevila, Victor Martinez-Glez, Antoni Berenguer-Llergo, Sara Reyes, Anna Brunet, Neus Baena, Miriam Guitart, and Anna Ruiz

Subjects

Genetics, neurodevelopmental disorders, intellectual disability, autism, gene panel, next generation sequencing, re-analysis, Genetics (clinical)

Abstract

Neurodevelopmental disorders (NDDs) affect 2–5% of the population and approximately 50% of cases are due to genetic factors. Since de novo pathogenic variants account for the majority of cases, a gene panel including 460 dominant and X-linked genes was designed and applied to 398 patients affected by intellectual disability (ID)/global developmental delay (GDD) and/or autism (ASD). Pathogenic variants were identified in 83 different genes showing the high genetic heterogeneity of NDDs. A molecular diagnosis was established in 28.6% of patients after high-depth sequencing and stringent variant filtering. Compared to other available gene panel solutions for NDD molecular diagnosis, our panel has a higher diagnostic yield for both ID/GDD and ASD. As reported previously, a significantly higher diagnostic yield was observed: (i) in patients affected by ID/GDD compared to those affected only by ASD, and (ii) in females despite the higher proportion of males among our patients. No differences in diagnostic rates were found between patients affected by different levels of ID severity. Interestingly, patients harboring pathogenic variants presented different phenotypic features, suggesting that deep phenotypic profiling may help in predicting the presence of a pathogenic variant. Despite the high performance of our panel, whole exome-sequencing (WES) approaches may represent a more robust solution. For this reason, we propose the list of genes included in our customized gene panel and the variant filtering procedure presented here as a first-tier approach for the molecular diagnosis of NDDs in WES studies.

Published

2023

11. Estudio genético en el hiperparatiroidismo primario: ¿a quién y qué genes estudiar?

Author

Ismael Capel, Isabel Mazarico-Altisent, and Neus Baena

Subjects

Nutrition and Dietetics, Endocrinology, Endocrinology, Diabetes and Metabolism

Published

2022

12. Systematic Collaborative Reanalysis of Genomic Data Improves Diagnostic Yield in Neurologic Rare Diseases

Author

Bullich, Gemma, primary, Matalonga, Leslie, additional, Pujadas, Montserrat, additional, Papakonstantinou, Anastasios, additional, Piscia, Davide, additional, Tonda, Raúl, additional, Artuch, Rafael, additional, Gallano, Pia, additional, Garrabou, Glòria, additional, González, Juan R., additional, Grinberg, Daniel, additional, Guitart, Míriam, additional, Laurie, Steven, additional, Lázaro, Conxi, additional, Luengo, Cristina, additional, Martí, Ramon, additional, Milà, Montserrat, additional, Ovelleiro, David, additional, Parra, Genís, additional, Pujol, Aurora, additional, Tizzano, Eduardo, additional, Macaya, Alfons, additional, Palau, Francesc, additional, Ribes, Antònia, additional, Pérez-Jurado, Luis A., additional, Beltran, Sergi, additional, Schlüter, Agatha, additional, Rodriguez-Palmero, Agustí, additional, Cáceres, Alejandro, additional, Nascimento, Andrés, additional, García-Cazorla, Àngels, additional, Cueto-González, Anna, additional, Marcé-Grau, Anna, additional, Nel.lo, Anna Ruiz, additional, Martínez-Monseny, Antonio, additional, Sànchez, Aurora, additional, García, Belén, additional, Pérez-Dueñas, Belén, additional, Gel, Bernat, additional, Fusté, Berta, additional, Hernández-Ferrer, Carles, additional, Casasnovas, Carlos, additional, Ortez, Carlos, additional, Arjona, César, additional, Hernando-Davalillo, Cristina, additional, de Benito, Daniel Natera, additional, Amador, Daniel Picó, additional, Gómez-Andrés, David, additional, Yubero, Dèlia, additional, Pelegrí-Sisó, Dolors, additional, Verdura, Edgard, additional, García-Arumí, Elena, additional, Castellanos, Elisabeth, additional, Gabau, Elisabeth, additional, Tobías, Ester, additional, López-Grondona, Fermina, additional, Cardellach, Francesc, additional, Garcia-Garcia, Francesc Josep, additional, Munell, Francina, additional, Tort, Frederic, additional, Aznar, Gemma, additional, Olivé-Cirera, Gemma, additional, Tell, Gemma, additional, Muñoz-Pujol, Gerard, additional, Paramonov, Ida, additional, Blanco, Ignacio, additional, Madrigal, Irene, additional, Valenzuela, Irene, additional, Gut, Ivo, additional, Cusco, Ivon, additional, Trotta, Jean-Rémi, additional, Cruz, Jordi, additional, Díaz-Manera, Jordi, additional, Milisenda, José César, additional, Ma Grau, Josep, additional, Garcia-Villoria, Judit, additional, Armstrong, Judith, additional, Cantó, Judith, additional, Sala-Coromina, Júlia, additional, Rodríguez-Revenga, Laia, additional, Alias, Laura, additional, Gort, Laura, additional, González-Quereda, Lídia, additional, Costa, Mar, additional, Fernández-Callejo, Marcos, additional, López-Sánchez, Marcos, additional, Álvarez-Mora, Maria Isabel, additional, Gut, Marta, additional, Serrano, Mercedes, additional, Raspall-Chaure, Miquel, additional, Toro, Mireia del, additional, Bayés, Mònica, additional, Díez, Neus Baena, additional, Spataro, Nino, additional, Capdevila, Núria, additional, Ugarteburu, Olatz, additional, Muñoz-Cabello, Patricia, additional, Duque, Penélope Romero, additional, Rabionet, Raquel, additional, Rojas-García, Ricard, additional, Calvo, Rosa, additional, Urreizti, Roser, additional, Bernal, Sara, additional, Boronat, Susana, additional, Balcells, Susanna, additional, and Vendrell, Teresa, additional

Published

2022

13. Genetic study in primary hyperparathyroidism: Which patients and which genes to study?

Author

Ismael Capel, Isabel Mazarico-Altisent, and Neus Baena

Subjects

Parathyroid Neoplasms, Research, Humans, Hyperparathyroidism, Primary

Published

2022

14. New genes involved in Angelman syndrome-like: Expanding the genetic spectrum

Author

Núria Capdevila, Miriam Guitart, Ariadna Ramirez-Mallafré, Xavier de la Cruz, Veronica Delgadillo, Neus Baena, Anna Ruiz, Carme Brun-Gasca, Nino Spataro, Elisabeth Gabau, Natalia Padilla, Steve Laurie, Jana Dominguez-Carral, Cinthia Aguilera, Sophia Derdak, Institut Català de la Salut, [Aguilera C] Genetics Laboratory, UDIAT-Centre Diagnòstic, Parc Taulí Hospital Universitari, Institut d’Investigació i Innovació Parc Taulí I3PT, Universitat Autònoma de Barcelona, Sabadell, Spain. [Gabau E, Ramirez-Mallafré A, Dominguez-Carral J, Delgadillo V] Paediatric Unit, Parc Taulí Hospital Universitari, Institut d’Investigació i Innovació Parc Taulí I3PT, Universitat Autònoma de Barcelona, Sabadell, Spain. [Brun-Gasca C] Paediatric Unit, Parc Taulí Hospital Universitari, Institut d’Investigació i Innovació Parc Taulí I3PT, Universitat Autònoma de Barcelona, Sabadell, Spain. Departament de Psicologia Clínica i Psicologia de la Salut, Universitat Autònoma de Barcelona, Bellaterra, Spain. [Padilla N] Àrea de Neurociències, Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. [de la Cruz X] Àrea de Neurociències, Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. Institució Catalana de Recerca i Estudis Avançats (ICREA), Barcelona, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects

Male, Candidate gene, Investigative Techniques::Genetic Techniques::Sequence Analysis::Sequence Analysis, DNA::Whole Genome Sequencing::Whole Exome Sequencing [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT], Vesicle-Associated Membrane Protein 2, Receptors, Cytoplasmic and Nuclear, Gene Expression, Social Sciences, SYNGAP1, Pathology and Laboratory Medicine, Medical Conditions, Medicine and Health Sciences, Medicine, Angelman, Síndrome d', Gene Regulatory Networks, Child, Heat-Shock Proteins, Genetics, Multidisciplinary, Movement Disorders, Otros calificadores::Otros calificadores::/genética [Otros calificadores], Transcriptional Control, Neurodegenerative Diseases, Phenotype, Hypotonia, Semantics, Angelman, Síndrome d' - Aspectes genètics, enfermedades del sistema nervioso::enfermedades del sistema nervioso central::trastornos del movimiento::síndrome de Angelman [ENFERMEDADES], Nervous System Diseases::Central Nervous System Diseases::Movement Disorders::Angelman Syndrome [DISEASES], Neurology, Female, Malalties congènites, medicine.symptom, Pathogens, Research Article, técnicas de investigación::técnicas genéticas::análisis de secuencias::análisis de secuencias de ADN::secuenciación del genoma completo::secuenciación del exoma completo [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], Adult, Ataxia, Adolescent, Science, Biology, Young Adult, Signs and Symptoms, Angelman syndrome, Exome Sequencing, Other subheadings::Other subheadings::/genetics [Other subheadings], Humans, Genetic Predisposition to Disease, Gene Regulation, Gene, Genetic Association Studies, Alleles, business.industry, Genetic heterogeneity, Infant, Biology and Life Sciences, Human Genetics, Linguistics, Matrix Attachment Region Binding Proteins, SPTAN1, medicine.disease, Human genetics, Repressor Proteins, Genòmica, Genetic Loci, Angelman Syndrome, Clinical Medicine, business, Genètica, Transcription Factors

Abstract

Síndrome de Angelman; Fenotipo Síndrome d'Angelman; Fenotip Angelman syndrome; Phenotype Angelman syndrome (AS) is a neurogenetic disorder characterized by severe developmental delay with absence of speech, happy disposition, frequent laughter, hyperactivity, stereotypies, ataxia and seizures with specific EEG abnormalities. There is a 10–15% of patients with an AS phenotype whose genetic cause remains unknown (Angelman-like syndrome, AS-like). Whole-exome sequencing (WES) was performed on a cohort of 14 patients with clinical features of AS and no molecular diagnosis. As a result, we identified 10 de novo and 1 X-linked pathogenic/likely pathogenic variants in 10 neurodevelopmental genes (SYNGAP1, VAMP2, TBL1XR1, ASXL3, SATB2, SMARCE1, SPTAN1, KCNQ3, SLC6A1 and LAS1L) and one deleterious de novo variant in a candidate gene (HSF2). Our results highlight the wide genetic heterogeneity in AS-like patients and expands the differential diagnosis. This work is supported by Instituto de Salud Carlos III (MG, PI16/01411), Asociación Española de Síndrome de Angelman (EG), Institut d’investigació i innovació Parc Taulí I3PT (CA, CIR2016/025, CIR2018/021) and Ministerio de Economía y Competitividad (XD, SAF2016-14 80255-R). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

Published

2021

15. 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

16. Genetic and Clinical Heterogeneity in Thirteen New Cases with Aceruloplasminemia. Atypical Anemia as a Clue for an Early Diagnosis

Author

Algirdas Utkus, Domenico Girelli, Sally Pollard, Henry Houlden, Jordi Sánchez-Delgado, John B. Porter, Nicholas W. Wood, Dulcineia M. Albuquerque, Kamil Kowalczyk, Marc Vila Cuenca, Alessandro Marchetto, Birute Burnyte, Perla Eleftheriou, Alejandro Giorgetti, Bartosz Karaszewski, Eda Suku, Fabiana Busti, Giacomo Marchi, Neus Baena-Díez, Kleber Yotsumoto Fertrin, Clara Esteban-Jurado, Ester Jové-Buxeda, Chiara Piubelli, P Bignell, Mayka Sanchez, Viorica Chelban, Marina Dorigatti Borges, Anna Barqué, and Gintaras Kaubrys

Subjects

Male, Models, Molecular, Metabolismo del hierro, Enfermedad neurodegenerativa, Microcytic anemia, Ceruloplasmina, Anèmia, Bioinformatics, Neurodegenerative disease, lcsh:Chemistry, Liver disease, neurodegenerative disease, iron metabolism, Aceruloplasminemia, lcsh:QH301-705.5, Spectroscopy, Metabolisme del ferro, biology, Ceruloplasmin, Neurodegenerative Diseases, Anemia, General Medicine, Middle Aged, Iron metabolism, aceruloplasminemia, ceruloplasmin, anemia, Computer Science Applications, Aceruloplasminèmia, Liver, Malaltia neurodegenerativa, Female, Adult, 616.8, Catalysis, Article, Inorganic Chemistry, medicine, Humans, Physical and Theoretical Chemistry, Molecular Biology, Aged, Ferritin, business.industry, Genetic heterogeneity, Transferrin saturation, Ferritina, Organic Chemistry, ferritin, medicine.disease, Iron Metabolism Disorders, Early Diagnosis, lcsh:Biology (General), lcsh:QD1-999, Mutation, biology.protein, business

Abstract

Aceruloplasminemia is a rare autosomal recessive genetic disease characterized by mild microcytic anemia, diabetes, retinopathy, liver disease, and progressive neurological symptoms due to iron accumulation in pancreas, retina, liver, and brain. The disease is caused by mutations in the Ceruloplasmin (CP) gene that produce a strong reduction or absence of ceruloplasmin ferroxidase activity, leading to an impairment of iron metabolism. Most patients described so far are from Japan. Prompt diagnosis and therapy are crucial to prevent neurological complications since, once established, they are usually irreversible. Here, we describe the largest series of non-Japanese patients with aceruloplasminemia published so far, including 13 individuals from 11 families carrying 13 mutations in the CP gene (7 missense, 3 frameshifts, and 3 splicing mutations), 10 of which are novel. All missense mutations were studied by computational modeling. Clinical manifestations were heterogeneous, but anemia, often but not necessarily microcytic, was frequently the earliest one. This study confirms the clinical and genetic heterogeneity of aceruloplasminemia, a disease expected to be increasingly diagnosed in the Next-Generation Sequencing (NGS) era. Unexplained anemia with low transferrin saturation and high ferritin levels without inflammation should prompt the suspicion of aceruloplasminemia, which can be easily confirmed by low serum ceruloplasmin levels. Collaborative joint efforts are needed to better understand the pathophysiology of this potentially disabling disease. info:eu-repo/semantics/publishedVersion

Published

2020

17. Mutational spectrum by phenotype: panel-based NGS testing of patients with clinical suspicion of RASopathy and children with multiple café-au-lait macules

Author

Eric Legius, Neus Baena, Conxi Lázaro, Eduard Serra, Ignacio Blanco, Bernat Gel, Graciela Pi, Lluïsa Vilageliu, Mercè Pineda, Alex Negro, Daniel Grinberg, Hector Salvador, Elisabeth Castellanos, Inma Rosas, Hilde Brems, Guillem Pintos, and Andreu Alibés

Subjects

0301 basic medicine, Male, multiple CALMs, DNA Mutational Analysis, neurofibromatosis type 1, 030105 genetics & heredity, Malalties hereditàries, Medicine, Child, Children, Genetics (clinical), Neurofibromin 1, medicine.diagnostic_test, Cafe-au-Lait Spots, High-Throughput Nucleotide Sequencing, genetic testing, Phenotype, Cafe-au-lait macules, Neoplasm Proteins, Child, Preschool, Hereditary Cancer, Female, Infants, Genetic diseases, medicine.medical_specialty, Neurofibromatosis 1, Context (language use), RASopathy, NGS panel, 03 medical and health sciences, Genetics, Humans, Genetic Testing, Neurofibromatosis, RASopathies, Genetic testing, business.industry, Infant, Proteins, medicine.disease, Dermatology, 030104 developmental biology, Early Diagnosis, Clinical diagnosis, Mutation, business, Proteïnes

Abstract

Children with neurofibromatosis type 1 (NF1) may exhibit an incomplete clinical presentation, making difficult to reach a clinical diagnosis. A phenotypic overlap may exist in children with other RASopathies or with other genetic conditions if only multiple café-au-lait macules (CALMs) are present. The syndromes that can converge in these inconclusive phenotypes have different clinical courses. In this context, an early genetic testing has been proposed to be clinically useful to manage these patients. We present the validation and implementation into diagnostics of a custom NGS panel (I2HCP, ICO-IMPPC Hereditary Cancer Panel) for testing patients with a clinical suspicion of a RASopathy (n = 48) and children presenting multiple CALMs (n = 102). We describe the mutational spectrum and the detection rates identified in these two groups of individuals. We identified pathogenic variants in 21 out of 48 patients with clinical suspicion of RASopathy, with mutations in NF1 accounting for 10% of cases. Furthermore, we identified pathogenic mutations mainly in the NF1 gene, but also in SPRED1, in more than 50% of children with multiple CALMs, exhibiting an NF1 mutational spectrum different from a group of clinically diagnosed NF1 patients (n = 80). An NGS panel strategy for the genetic testing of these two phenotype-defined groups outperforms previous strategies.

Published

2020

18. High Incidence of Copy Number Variants in Adults with Intellectual Disability and Co-morbid Psychiatric Disorders

Author

Anna Ruiz, Lourdes Martorell, Elisabet Vilella, David Torrents-Rodas, Susanna Esteba-Castillo, Lluís Armengol, Marina Viñas-Jornet, Núria Ribas-Vidal, Neus Baena, Miriam Guitart, Elisabeth Gabau, and Ramon Novell

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, DNA Copy Number Variations, Genotype, Intellectual disability, Comorbidity, Behavioural disorders, Genetic analysis, Statistics, Nonparametric, Young Adult, 03 medical and health sciences, Genetics, Humans, Medicine, Prospective Studies, Copy-number variation, Psychiatry, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, Oligonucleotide Array Sequence Analysis, Original Research, Copy number variants, Adult patients, business.industry, Incidence, Mental Disorders, Middle Aged, medicine.disease, Co morbid, Phenotype, 030104 developmental biology, Spain, Cohort, Female, High incidence, Psychiatric disorders, business

Abstract

A genetic analysis of unexplained mild-moderate intellectual disability and co-morbid psychiatric or behavioural disorders is not systematically conducted in adults. A cohort of 100 adult patients affected by both phenotypes were analysed in order to identify the presence of copy number variants (CNVs) responsible for their condition identifying a yield of 12.8% of pathogenic CNVs (19% when including clinically recognizable microdeletion syndromes). Moreover, there is a detailed clinical description of an additional 11% of the patients harbouring possible pathogenic CNVs—including a 7q31 deletion (IMMP2L) in two unrelated patients and duplications in 3q29, 9p24.2p24.1 and 15q14q15.1—providing new evidence of its contribution to the phenotype. This study adds further proof of including chromosomal microarray analysis (CMA) as a mandatory test to improve the diagnosis in the adult patients in psychiatric services. Electronic supplementary material The online version of this article (10.1007/s10519-018-9902-6) contains supplementary material, which is available to authorized users.

Published

2018

19. W51. HIGH DIAGNOSTIC YIELD IN CHILDREN AND ADOLESCENTS WITH MILD TO BORDERLINE INTELLECTUAL FUNCTIONING AND COMORBID PSYCHIATRIC DISORDER

Author

Neus Baena, Anna Ruiz, Miriam Guitart, Patricia Karrera, Carmen Manso Bazús, Nino Spataro, Diego Palao, Montserrat Pàmias, and Lidia Torrent

Subjects

Pharmacology, Psychiatry and Mental health, medicine.medical_specialty, Borderline intellectual functioning, Neurology, business.industry, Yield (finance), medicine, Pharmacology (medical), Neurology (clinical), Psychiatry, business, Biological Psychiatry

Published

2021

20. The utility of Next Generation Sequencing for molecular diagnostics in Rett syndrome

Author

Francisco V Carratala-Marco, Sabine Scholl-Bürgi, Carmen Jovaní Casano, Samuel Ignacio Pascual Pascual, Xenia Alonso, Carlos Ignacio Ortez González, Mercedes Serrano, Laura Blasco Pérez, Pablo Lapunzina, Neus Baena, Alfons Macaya Ruíz, Miquel Raspall-Chaure, Victoria San Antonio-Arce, Encarna Guillén-Navarro, Guillermo Antiñolo Gil, Instituto de Salud Carlos III, European Commission, Fundación Española para la Ciencia y la Tecnología, Asociación Catalana del Síndrome de Rett, Fondo Biorett, and Mi Princesa Rett

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, CDKL5, lcsh:Medicine, Rett syndrome, Biology, Bioinformatics, DNA sequencing, Article, MECP2, 03 medical and health sciences, symbols.namesake, Neurodevelopmental disorder, medicine, lcsh:Science, Exome sequencing, Sanger sequencing, Multidisciplinary, Neurodevelopmental disorders, lcsh:R, Massively-parallel sequencing, medicine.disease, Molecular diagnostics, 030104 developmental biology, symbols, lcsh:Q

Abstract

Rett Working Group., Rett syndrome (RTT) is an early-onset neurodevelopmental disorder that almost exclusively affects girls and is totally disabling. Three genes have been identified that cause RTT: MECP2, CDKL5 and FOXG1. However, the etiology of some of RTT patients still remains unknown. Recently, next generation sequencing (NGS) has promoted genetic diagnoses because of the quickness and affordability of the method. To evaluate the usefulness of NGS in genetic diagnosis, we present the genetic study of RTT-like patients using different techniques based on this technology. We studied 1577 patients with RTT-like clinical diagnoses and reviewed patients who were previously studied and thought to have RTT genes by Sanger sequencing. Genetically, 477 of 1577 patients with a RTT-like suspicion have been diagnosed. Positive results were found in 30% by Sanger sequencing, 23% with a custom panel, 24% with a commercial panel and 32% with whole exome sequencing. A genetic study using NGS allows the study of a larger number of genes associated with RTT-like symptoms simultaneously, providing genetic study of a wider group of patients as well as significantly reducing the response time and cost of the study., The work was supported by grants from the Spanish Ministry of Health (Instituto de Salud Carlos III/FEDER, PI15/01013); Crowdfunding program PRECIPITA, from the Spanish Ministry of Health (Fundación Española para la Ciencia y la Tecnología); Catalan Association for Rett Syndrome; Fondobiorett and Mi Princesa Rett. The molecular analyses of eleven WES in 2014 were funded by the CNAG’s 2013 call "300 exomes to elucidate rare diseases”. AGC is supported by the ISCIII grant: FIS PI15/01082.

Published

2017

21. RNA editing independently occurs at three mir-376a-1 sites and may compromise the stability of the microRNA hairpin

Author

Hugo Fernandez-Bellon, Diego A. Hartasánchez, Marina Brasó-Vives, Maria Lopez-Valenzuela, Ronald E. Bontrop, Eva Garcia-Ramallo, Yolanda Espinosa-Parrilla, Neus Baena, Yukio Kawahara, Miriam Guitart, Ivanela Kondova, and Alicia Gallego

Subjects

0301 basic medicine, Small RNA, Pan troglodytes, Placenta, RNA Stability, In silico, Computational biology, Biology, 03 medical and health sciences, symbols.namesake, Pregnancy, microRNA, Genetics, Animals, Post-transcriptional regulation, Cerebral Cortex, Sanger sequencing, Gorilla gorilla, Epistasis, Genetic, General Medicine, Phenotype, MicroRNAs, 030104 developmental biology, RNA editing, symbols, Macaca, Nucleic Acid Conformation, Female, RNA Editing, Function (biology)

Abstract

RNA editing is being recognized as an important post-transcriptional mechanism that may have crucial roles in introducing genetic variation and phenotypic diversity. Despite microRNA editing recurrence, defining its biological relevance is still under extended debate. To better understand microRNA editing function and regulation we performed an exhaustive characterization of the A-to-I site-specific patterns in mir-376a-1, a mammalian microRNA which RNA editing is involved in the regulation of development and in disease. Thorough an integrative approach based on high-throughput small RNA sequencing, Sanger sequencing and computer simulations we explored mir-376a-1 editing in samples from various individuals and primate species including human placenta and macaque, gorilla, chimpanzee and human brain cortex. We observed that mir-376a-1 editing is a common phenomenon in the mature and primary microRNA molecules and it is more frequently detected in brain than in placenta. Primary mir-376a-1 is edited at three positions, -1, +4 and +44. Editing frequency estimations and in silico simulations indicated that editing was not equally recurrent along the three mir-376a-1 sites, nevertheless no epistatic interactions among them were observed. Particularly, the +4 site, located in the seed region of the mature miR-376a-5p, reached the highest editing frequency in all samples. Secondary structure predictions revealed that the +4 position was the one that conferred the highest stability to the mir-376a-1 hairpin. We suggest that molecular stability might partially explain the editing recurrence observed in certain microRNAs and that editing events conferring new functional regulatory roles in particular tissues and species could have been conserved along evolution, as it might be the case of mir-376a-1 in primate brain cortex.

Published

2017

22. Author response for 'Mutational spectrum by phenotype: panel‐based NGS testing of patients with clinical suspicion of RASopathy and children with multiple café‐au‐lait macules'

Author

Hector Salvador, Eric Legius, Neus Baena, Eduard Serra, Guillem Pintos, Elisabeth Castellanos, Daniel Grinberg, Andreu Alibés, Inma Rosas, Alejandro Negro, Ignacio Blanco, Hilde Brems, Lluïsa Vilageliu, Bernat Gel, Conxi Lázaro, Graciela Pi, and Mercè Pineda

Subjects

medicine.medical_specialty, business.industry, medicine, RASopathy, medicine.disease, business, Dermatology, Cafe-au-lait macules

Published

2019

23. Genetic contribution to lipid target achievement with statin therapy: a prospective study

Author

Neus Baena-Díez, Jose Luis Puzo-Foncilla, Pedro Alía-Ramos, Rosa Navarro-Badal, Pilar Calmarza, Beatriz Candás-Estébanez, Ariadna Padró-Miquel, Assumpta Caixàs-Pedragós, Roser Güell-Miró, Cristina Ruiz-Iruela, and Xavier Pintó-Sala

Subjects

0301 basic medicine, Oncology, Male, medicine.medical_specialty, CYP2D6, Statin, medicine.drug_class, Atorvastatin, Hyperlipidemias, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Genetics, Medicine, Humans, Rosuvastatin, Prospective Studies, Prospective cohort study, CYP2C9, Pharmacology, business.industry, Cholesterol, HDL, nutritional and metabolic diseases, Genetic Variation, Lipid metabolism, Cholesterol, LDL, Middle Aged, Lipids, Cholesterol Ester Transfer Proteins, 030104 developmental biology, Cytochrome P-450 CYP2D6, Simvastatin, Molecular Medicine, lipids (amino acids, peptides, and proteins), Female, Hydroxymethylglutaryl-CoA Reductase Inhibitors, business, medicine.drug, ATP Binding Cassette Transporter 1, Follow-Up Studies

Abstract

Statin therapy response is highly variable. Variants of lipid metabolism genes and statin pharmacokinetic modulators could play a role, however, the impact of most of these variants remains unconfirmed. A prospective and multicenter study included 252 patients was carried out in order to assess, according to achievement of LDL-C or non-HDL-C therapeutic targets and quantitative changes in lipid profiles, the impact of CETP, ABCA1, CYP2D6, and CYP2C9 gene candidate variants on the simvastatin, atorvastatin, and rosuvastatin response. Patients carrier ABCA1 rs2230806 and CYP2D6*3 variants are less likely to achieve therapeutic lipid targets (p = 0.020, OR = 0.59 [0.37, 0.93]; p = 0.040, OR = 0.23 [0.05, 0.93], respectively). Among CETP variants, rs708272 was linked to a 10.56% smaller reduction in LDL-C with rosuvastatin (95% CI = [1.27, 19.86] %; p = 0.028). In contrast, carriers of rs5882 had a 13.33% greater reduction in LDL-C (95% CI = [25.38, 1.28]; p = 0.032). If these findings are confirmed, ABCA1, CYP2D6, and CETP genotyping could be used to help predict which statin and dosage is appropriate in order to improve personalized medicine.

Published

2019

24. Correction: Arterial tortuosity syndrome: 40 new families and literature review

Author

Damien Bonnet, Paul Coucke, David R. Deyle, Mohammed Z. Haider, Fahrettin Uysal, Eudice E. Fontenot, Inge De Wandele, Margot A. Cousin, Waheed Al-Manea, Sehime Gulsun Temel, Massimiliano Rossi, Fabienne Giuliano, Sofie De Schepper, Joshua S. Hardin, Mazen Al-Essa, Ergun Cil, N Canham, Majed Dasouki, Harry C. Dietz, Juliette Albuisson, Pamela Moceri, Sophie Dupuis-Girod, Koenraad Devriendt, David Warner, Bart Loeys, Özlem M. Bostan, Andrea Taylor, Neus Baena, Elise Schaefer, Sheela Nampoothiri, Eric W. Klee, Karin Pichler, Elaine C. Davis, Andy Willaert, Odile Boute, Tiffany Busa, Björn Fischer-Zirnsak, Alper Gezdirici, Jamal Ghoumid, Manuel F. Landecho, Shehla Mohammed, Yuri A. Zarate, Maria Ramos-Arroyo, Tom R. Collins, Aude Beyens, Stanislas Lyonnet, Laura Muiño-Mosquera, Uwe Kornak, Marine Vanhomwegen, Helen Michael, Anna Rajeb, Mohammed Zain Seidahmed, Anne De Paepe, Deepthi De Silva, Bert Callewaert, Elisabeth Steichen-Gersdorf, Lut Van Laer, Annekatrien Boel, Anne Legrand, Xavier Jeunemaitre, Lionel Van Maldergem, Katrina Prescott, Mustafa A. Salih, and Julie De Backer

Subjects

medicine.medical_specialty, Arterial tortuosity syndrome, business.industry, Published Erratum, MEDLINE, medicine.disease, Human genetics, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, medicine, Intensive care medicine, business, 030217 neurology & neurosurgery, Genetics (clinical)

Abstract

In the published version of this paper the author Neus Baena's name was incorrectly given as Neus Baena Diez. This has now been corrected in both the HTML and PDF versions of the paper.

Published

2019

25. Arterial tortuosity syndrome: 40 new families and literature review

Author

Uwe Kornak, Fabienne Giuliano, Aude Beyens, Mustafa A. Salih, Massimiliano Rossi, Marine Vanhomwegen, Lut Van Laer, Fahrettin Uysal, Koenraad Devriendt, David R. Deyle, Mohammed Z. Haider, Elise Schaefer, Tom R. Collins, Annekatrien Boel, Mazen Al-Essa, Elaine C. Davis, Elisabeth Steichen-Gersdorf, Ergun Cil, Eudice E. Fontenot, Andy Willaert, Bart Loeys, Eric W. Klee, Björn Fischer-Zirnsak, Joshua S. Hardin, Sophie Dupuis-Girod, N Canham, Majed Dasouki, Harry C. Dietz, Laura Muiño-Mosquera, Yuri A. Zarate, Karin Pichler, Xavier Jeunemaitre, Neus Baena Diez, Maria Ramos-Arroyo, Damien Bonnet, Paul Coucke, Waheed Al-Manea, Anne De Paepe, Tiffany Busa, Anna Rajeb, Shehla Mohammed, Odile Boute, Sofie De Schepper, Mohammed Zain Seidahmed, Juliette Albuisson, Andrea Taylor, Deepthi De Silva, Inge De Wandele, Helen Michael, Margot A. Cousin, Sehime Gulsun Temel, Pamela Moceri, Julie De Backer, Lionel Van Maldergem, Stanislas Lyonnet, Özlem M. Bostan, Katrina Prescott, Bert Callewaert, Anne Legrand, David Warner, Sheela Nampoothiri, Alper Gezdirici, Jamal Ghoumid, and Manuel F. Landecho

Subjects

0301 basic medicine, Marfan syndrome, Adult, Joint Instability, Male, Connective Tissue Disorder, Pathology, medicine.medical_specialty, Arterial tortuosity syndrome, Adolescent, Vascular Malformations, Biopsy, Perforation (oil well), Glucose Transport Proteins, Facilitative, Smad2 Protein, 030204 cardiovascular system & hematology, 03 medical and health sciences, 0302 clinical medicine, Aneurysm, Transforming Growth Factor beta, medicine, Humans, Diaphragmatic hernia, Child, Genetics (clinical), Vascular tissue, Aorta, Skin, Hernia, Diaphragmatic, Respiratory Distress Syndrome, Newborn, biology, business.industry, Connective Tissue Growth Factor, Infant, Skin Diseases, Genetic, Arteries, medicine.disease, 3. Good health, Pedigree, 030104 developmental biology, Child, Preschool, Mutation, biology.protein, Female, Human medicine, business, Elastin

Abstract

PurposeWe delineate the clinical spectrum and describe the histology in arterial tortuosity syndrome (ATS), a rare connective tissue disorder characterized by tortuosity of the large and medium-sized arteries, caused by mutations in SLC2A10.MethodsWe retrospectively characterized 40 novel ATS families (50 patients) and reviewed the 52 previously reported patients. We performed histology and electron microscopy (EM) on skin and vascular biopsies and evaluated TGF-β signaling with immunohistochemistry for pSMAD2 and CTGF.ResultsStenoses, tortuosity, and aneurysm formation are widespread occurrences. Severe but rare vascular complications include early and aggressive aortic root aneurysms, neonatal intracranial bleeding, ischemic stroke, and gastric perforation. Thus far, no reports unequivocally document vascular dissections or ruptures. Of note, diaphragmatic hernia and infant respiratory distress syndrome (IRDS) are frequently observed. Skin and vascular biopsies show fragmented elastic fibers (EF) and increased collagen deposition. EM of skin EF shows a fragmented elastin core and a peripheral mantle of microfibrils of random directionality. Skin and end-stage diseased vascular tissue do not indicate increased TGF-β signaling.ConclusionOur findings warrant attention for IRDS and diaphragmatic hernia, close monitoring of the aortic root early in life, and extensive vascular imaging afterwards. EM on skin biopsies shows disease-specific abnormalities.GENETICS in MEDICINE advance online publication, 11 January 2018; doi:10.1038/gim.2017.253. ispartof: Genetics in Medicine vol:20 issue:10 pages:1236-1245 ispartof: location:United States status: published

Published

2018

26. Delineation ofEFTUD2Haploinsufficiency-Related Phenotypes Through a Series of 36 Patients

Author

Marie Gonzales, Alice Goldenberg, Jean-Luc Alessandri, Charles Decaestecker, Alain Verloes, Daphné Lehalle, Marie-Line Jacquemont, Marlène Rio, Muriel Holder-Espinasse, Christopher T. Gordon, Alexandre Vasiljevic, Michel Vekemans, Loïc de Pontual, Sandrine Marlin, Laurent Pasquier, Didier Lacombe, Robert Smigiel, Lucile Boutaud, Sylvie Manouvrier-Hanu, Valérie Malan, Arnold Munnich, Jeanne Amiel, Stanislas Lyonnet, Christel Thauvin-Robinet, Roseline Caumes, Geneviève Baujat, Odile Boute-Benejean, Florence Petit, Myriam Oufadem, Gilles Morin, Neus Baena, Clarisse Baumann, Dominique Gaillard, Tania Attié-Bitach, Géraldine Goudefroye, and Michèle Mathieu-Dramard

Subjects

Male, Pediatrics, medicine.medical_specialty, Microcephaly, Hearing loss, Haploinsufficiency, Disease, Choanal atresia, Biology, Anus, Imperforate, Diagnosis, Differential, Hearing Loss, Bilateral, Pregnancy, Intellectual Disability, Prenatal Diagnosis, Intellectual disability, Genetics, medicine, Humans, Abnormalities, Multiple, Ear, External, Child, Ribonucleoprotein, U5 Small Nuclear, Genetics (clinical), Ophthalmoplegia, Infant, Peptide Elongation Factors, medicine.disease, External ear malformation, Thrombocytopenia, Phenotype, Child, Preschool, Atresia, Mutation, Female, medicine.symptom, Hand Deformities, Congenital, Mandibulofacial Dysostosis

Abstract

Mandibulofacial dysostosis, Guion-Almeida type (MFDGA) is a recently delineated multiple congenital anomalies/mental retardation syndrome characterized by the association of mandibulofacial dysostosis (MFD) with external ear malformations, hearing loss, cleft palate, choanal atresia, microcephaly, intellectual disability, oesophageal atresia (OA), congenital heart defects (CHDs), and radial ray defects. MFDGA emerges as a clinically recognizable entity, long underdiagnosed due to highly variable presentations. The main differential diagnoses are CHARGE and Feingold syndromes, oculoauriculovertebral spectrum, and other MFDs. EFTUD2, located on 17q21.31, encodes a component of the major spliceosome and is disease causing in MFDGA, due to heterozygous loss-of-function (LoF) mutations. Here, we describe a series of 36 cases of MFDGA, including 24 previously unreported cases, and we review the literature in order to delineate the clinical spectrum ascribed to EFTUD2 LoF. MFD, external ear anomalies, and intellectual deficiency occur at a higher frequency than microcephaly. We characterize the evolution of the facial gestalt at different ages and describe novel renal and cerebral malformations. The most frequent extracranial malformation in this series is OA, followed by CHDs and skeletal abnormalities. MFDGA is probably more frequent than other syndromic MFDs such as Nager or Miller syndromes. Although the wide spectrum of malformations complicates diagnosis, characteristic facial features provide a useful handle.

Published

2014

27. Phenotype variability in thirteen 16p11.2 deletion patients

Author

Neus Baena, Miriam Guitart, Diana Rodà, and Elisabeth Gabau

Subjects

Genetics, Text mining, business.industry, Management of Technology and Innovation, Biology, business, Phenotype, Pediatrics, RJ1-570

Published

2018

28. Arterial tortuosity syndrome: 40 new families and literature review

Author

Beyens, Aude, primary, Albuisson, Juliette, additional, Boel, Annekatrien, additional, Al-Essa, Mazen, additional, Al-Manea, Waheed, additional, Bonnet, Damien, additional, Bostan, Ozlem, additional, Boute, Odile, additional, Busa, Tiffany, additional, Canham, Nathalie, additional, Cil, Ergun, additional, Coucke, Paul J., additional, Cousin, Margot A., additional, Dasouki, Majed, additional, De Backer, Julie, additional, De Paepe, Anne, additional, De Schepper, Sofie, additional, De Silva, Deepthi, additional, Devriendt, Koenraad, additional, De Wandele, Inge, additional, Deyle, David R., additional, Dietz, Harry, additional, Dupuis-Girod, Sophie, additional, Fontenot, Eudice, additional, Fischer-Zirnsak, Björn, additional, Gezdirici, Alper, additional, Ghoumid, Jamal, additional, Giuliano, Fabienne, additional, Diéz, Neus Baena, additional, Haider, Mohammed Z., additional, Hardin, Joshua S., additional, Jeunemaitre, Xavier, additional, Klee, Eric W., additional, Kornak, Uwe, additional, Landecho, Manuel F., additional, Legrand, Anne, additional, Loeys, Bart, additional, Lyonnet, Stanislas, additional, Michael, Helen, additional, Moceri, Pamela, additional, Mohammed, Shehla, additional, Muiño-Mosquera, Laura, additional, Nampoothiri, Sheela, additional, Pichler, Karin, additional, Prescott, Katrina, additional, Rajeb, Anna, additional, Ramos-Arroyo, Maria, additional, Rossi, Massimiliano, additional, Salih, Mustafa, additional, Seidahmed, Mohammed Z., additional, Schaefer, Elise, additional, Steichen-Gersdorf, Elisabeth, additional, Temel, Sehime, additional, Uysal, Fahrettin, additional, Vanhomwegen, Marine, additional, Van Laer, Lut, additional, Van Maldergem, Lionel, additional, Warner, David, additional, Willaert, Andy, additional, Collins, Tom R., additional, Taylor, Andrea, additional, Davis, Elaine C., additional, Zarate, Yuri, additional, and Callewaert, Bert, additional

Published

2018

29. Lack of Postprandial Peak in Brain-Derived Neurotrophic Factor in Adults with Prader-Willi Syndrome

Author

Neus Baena, Assumpta Caixàs, Susanna Esteba-Castillo, Mercedes Rigla, Marina Viñas-Jornet, Miriam Guitart, Ramón Coronas, David Torrents-Rodas, Raquel Corripio, Olga Giménez-Palop, Marta Bueno, Joan Deus, Jesús Pujol, Elisabeth Gabau, Ramon Novell, and Caixàs i Pedragós, Assumpta

Subjects

0301 basic medicine, Leptin, Physiology, Peptide Hormones, lcsh:Medicine, Biochemistry, Energy homeostasis, Body Mass Index, Endocrinology, 0302 clinical medicine, Neurotrophic factors, Ingestion, Insulin, Homeostasis, Childhood obesity, lcsh:Science, Body mass index, Prader-Willi, Síndrome de, Multidisciplinary, digestive, oral, and skin physiology, Uniparental disomy, Postprandial, Physiological Parameters, Prader-Willi syndrome, Prader-Willi Syndrome, Research Article, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Childhood Obesity, 030209 endocrinology & metabolism, Context (language use), 03 medical and health sciences, Internal medicine, medicine, Clinical genetics, Obesity, Growth hormone, Medicine and health sciences, Diabetic Endocrinology, Brain-derived neurotrophic factor, business.industry, lcsh:R, Body Weight, Biology and Life Sciences, nutritional and metabolic diseases, medicine.disease, Hormones, 030104 developmental biology, Disorders of imprinting, Growth Hormone, lcsh:Q, Physiological Processes, business

Abstract

Context: Prader-Willi syndrome (PWS) is characterized by severe hyperphagia. Brain-derived neurotrophic factor (BDNF) and leptin are reciprocally involved in energy homeostasis. Objectives: To analyze the role of BDNF and leptin in satiety in genetic subtypes of PWS. Design: Experimental study. Setting: University hospital. Subjects: 90 adults: 30 PWS patients; 30 age-sex-BMI-matched obese controls; and 30 age-sex-matched lean controls. Interventions: Subjects ingested a liquid meal after fasting ≥10 hours. Main Outcome Measures: Leptin and BDNF levels in plasma extracted before ingestion and 30’, 60’, and 120’ after ingestion. Hunger, measured on a 100-point visual analogue scale before ingestion and 60’ and 120’ after ingestion. Results: Fasting BDNF levels were lower in PWS than in controls (p = 0.05). Postprandially, PWS patients showed only a truncated early peak in BDNF, and their BDNF levels at 60' and 120' were lower compared with lean controls (p

Published

2016

30. Novel Mutations Causing C5 Deficiency in Three North-African Families

Author

Pere Soler-Palacín, Andrea Martín-Nalda, Elisabeth Gabau, Clara Franco-Jarava, Manuel Hernández-González, Natalia Padilla, Xavier de la Cruz, David Comas, Roger Colobran, Ricardo Pujol-Borrell, Neus Baena, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), and European Commission

Subjects

0301 basic medicine, Male, Hereditary Complement Deficiency Diseases, Complement system, Immunology, Population, Biology, Frameshift mutation, 03 medical and health sciences, Exon, African continental ancestry group, medicine, Immunology and Allergy, Humans, Complement 5 deficiency, Allele, education, Child, Genetics, education.field_of_study, Meningococcal disease, Immunologic Deficiency Syndromes, Complement C5, Infant, C5 Deficiency, Complement deficiency, medicine.disease, Pedigree, 030104 developmental biology, Child, Preschool, Africa, Mutation, Female, Complement membrane attack complex

Abstract

Colobran, Roger et al., The complement system plays a central role in defense to encapsulated bacteria through opsonization and membrane attack complex (MAC) dependent lysis. The three activation pathways (classical, lectin, and alternative) converge in the cleavage of C5, which initiates MAC formation and target lysis. C5 deficiency is associated to recurrent infections by Neisseria spp. In the present study, complement deficiency was suspected in three families of North-African origin after one episode of invasive meningitis due to a non-groupable and two uncommon Meningococcal serotypes (E29, Y). Activity of alternative and classical pathways of complement were markedly reduced and the measurement of terminal complement components revealed total C5 absence. C5 gene analysis revealed two novel mutations as causative of the deficiency: Family A propositus carried a homozygous deletion of two adenines in the exon 21 of C5 gene, resulting in a frameshift and a truncated protein (c.2607_2608del/p.Ser870ProfsX3 mutation). Families B and C probands carried the same homozygous deletion of three consecutive nucleotides (CAA) in exon 9 of the C5 gene, leading to the deletion of asparagine 320 (c.960_962del/p.Asn320del mutation). Family studies confirmed an autosomal recessive inheritance pattern. Although sharing the same geographical origin, families B and C were unrelated. This prompted us to investigate this mutation prevalence in a cohort of 768 North-African healthy individuals. We identified one heterozygous carrier of the p.Asn320del mutation (allelic frequency = 0.065 %), indicating that this mutation is present at low frequency in North-African population., This study was funded by Instituto de Salud Carlos III, grant PI14/00405, cofinanced by the European Regional Development Fund (ERDF), and by MINECO grant CGL2013-44351-P.

Published

2015

31. Characterization of six marker chromosomes by comparative genomic hybridization

Author

Neus Baena, Sergi Villatoro, J.M. Belloso, Miriam Guitart, Elisabeth Gabau, María Rosa Caballín, and R. Vidal

Subjects

Adult, Male, Adolescent, Euchromatin, Aneuploidy, Biology, Facial dysmorphism, Genetics, medicine, Humans, In Situ Hybridization, Fluorescence, Genetics (clinical), Chromosome Aberrations, medicine.diagnostic_test, Genome, Human, Infant, Newborn, Nucleic Acid Hybridization, medicine.disease, Phenotype, Chromosome Banding, Child, Preschool, Karyotyping, Speech delay, %22">Fish , Female, medicine.symptom, Comparative genomic hybridization, Fluorescence in situ hybridization

Abstract

We applied comparative genomic hybridization (CGH) in six patients with de novo prenatal or postnatal extra marker chromosomes (MC). In four cases, MCs were mosaic and in one of them, the MC was detected in less than 50% of the cells. In three cases, CGH identified the origin of the extra MCs. In the other three, two prenatal cases and one child with an abnormal phenotype, CGH showed normal profiles. Among these cases, a normal profile and entirely C-band positive was identified suggesting that MC did not contain euchromatin. Genetic imbalances detected by CGH were as follow: a gain of 8p10-p12 in a boy with facial dysmorphism, hyperactivity and speech delay, a gain of 8q10-q12 in a healthy man with a history of spontaneous abortions, and a gain of 15q11-q13 in a girl with speech delay, and motor skill and object manipulation difficulties. Clinical data of these patients were compared with those reported in the literature. We conclude that CGH is a very useful and powerful tool for characterizing prenatal or postnatal MCs, even when the mosaicism is present and the MCs are present in less than 50% of the cells.

Published

2005

32. Prenatal detection of congenital renal malformations by fetal ultrasonographic examination

Author

Ettore Cariati, Cariati Ettore, Neus Baena, Francesco Benedicenti, Vytautas Kasiulevicius, Algirdas Utkus, Fabrizio Bianchi, and Reproductive Origins of Adult Health and Disease (ROAHD)

Subjects

Male, medicine.medical_specialty, Prenatal diagnosis, Gestational Age, SONOGRAPHY, Kidney, DIAGNOSIS, Ultrasonography, Prenatal, DISEASE, Congenital Abnormalities, Dysgenesis, Pregnancy, Genetics, medicine, Humans, Registries, URINARY-TRACT ANOMALIES, Genetics (clinical), ULTRASOUND, Fetus, prenatal diagnosis, business.industry, Obstetrics, STRUCTURAL ABNORMALITIES, screening, Ultrasound, Infant, Newborn, Gestational age, ROUTINE ULTRASONOGRAPHY, General Medicine, medicine.disease, Bilateral Renal Agenesis, Europe, medicine.anatomical_structure, renal malformations, multicenter study, fetal ultrasound, congenital birth defects, birth registry, REGISTRY, Female, business

Abstract

The study was performed to evaluate the prevalence of prenatal ultrasound diagnoses for renal anomalies in 20 registries of 12 European countries, and to compare the different prenatal scanning policies. Standardized data were acquired from 709,030 livebirths, stillbirths, and induced abortions during the study period of 2.5 years and transmitted for central analysis. At least one renal malforruation was diagnosed in 1130 infants and fetuses. Prenatal diagnosis (PD) was given in 81.8% of all cases, 29% of these pregnancies were terminated. The highest detection rate was reported for unilateral multicystic dysplastic kidneys with 97% (102/105). An early diagnosis was documented for exstrophy of bladder at a mean gestational age of 18.5 weeks. Dilatations of the upper urinary tract were seen late in pregnancy at 28.3 weeks. Terminations of pregnancies (TOP) were performed in 67% (58/86) of the detected bilateral renal agenesis/dysgenesis, but only 4% of the unilateral multicystic dysplastic renal malformations (4/102). In about 1/3 of the cases, renal malformations are within the category of associated malformations, which include multiple non-syndromal malformations, chromosomal aberrations, and non-chromosomal syndromes. Renal malformations were detected in 2/3 of the associated category by the first prenatal ultrasound scan. Detection rates vary in the different countries of the European community due to diverse policies, ethical, and religious background. Countries with no routine ultrasound show the lowest rates in detection, and termination of pregnancy. Prenatally detected renal malformations should result in a careful examination for further anomalies. Prenatal ultrasound fulfills the needs of screening examinations and is a good tool in detecting lethal and severe renal malformations. (c) 2005 Elsevier SAS. All rights reserved.

Published

2005

33. Prenatal diagnostic procedures used in pregnancies with congenital malformations in 14 regions of Europe

Author

Helen Dolk, Maria Loane, Hermien E. K. de Walle, Miriam Gatt, David H. Stone, Neus Baena, Blanca Gener, Ester Garne, Yves Gillerot, Gioacchino Scarano, Annette Queisser-Luft, Carmen Mosquera-Tenreiro, Maria Feijoo, Claude Stoll, Catherine De Vigan, Marie-Claude Addor, University of Groningen, and Reproductive Origins of Adult Health and Disease (ROAHD)

Subjects

Adult, medicine.medical_specialty, prenatal ultrasound, chorion villus sampling, Population, Chorionic villus sampling, Prenatal diagnosis, uptake rate, Medical Records, Ultrasonography, Prenatal, Predictive Value of Tests, Pregnancy, Prenatal Diagnosis, Outcome Assessment, Health Care, medicine, Humans, Abnormalities, Multiple, prenatal diagnostic procedures, Registries, education, Genetics (clinical), Gynecology, Chromosome Aberrations, education.field_of_study, medicine.diagnostic_test, Obstetrics, business.industry, MEDICINE, Obstetrics and Gynecology, WOMEN, Congenital malformations, medicine.disease, Europe, medicine.anatomical_structure, Amniocentesis, amniocentesis, Gestation, Chorionic villi, Female, business, Maternal Age

Abstract

Objective To investigate outcomes of ultrasound investigations (US) and invasive diagnostic procedures in cases of congenital malformations (CM), and to compare the use of invasive prenatal test techniques (amniocentesis (AC) versus chorionic villus sampling (CVS)) among European populations.Design Analysis of data from population-based registries of CM.Subjects 25 400 cases of CM recorded by 14 EUROCAT registries covering a total population of 1013 352 births 1995-99.Results US were performed in 91% of cases, and positively detected CM in 35% of cases. AC was performed in 24% of the cases and CVS in 3% of cases. Thirty-eight percent of invasive tests gave positive results. Fifty-two percent of cases with maternal age greater than or equal to35 years had an invasive test performed compared to 20% of cases with younger mothers.Considerable variation was found between registries in the uptake rate of invasive tests in cases with older maternal age and on the use of invasive tests with only four regions employing CVS techniques in at least a third of the cases having invasive tests. For chromosomal anomalies US gave positive results in 46% of cases with maternal ageConclusion Prenatal US was performed in 91% of all pregnancies with CM but the test was only positive in a third of the cases. There was large regional variation in the uptake rate of invasive tests with maternal age of 35 years or more. For every CVS carried out there were nine AC tests. US is an important tool in the prenatal diagnosis of chromosomal anomalies in Europe. Copyright (C) 2004 John Wiley Sons, Ltd.

Published

2004

34. Contribution of ultrasonographic examination to the prenatal detection of trisomy 21: experience from 19 European registers

Author

Pa Boyd, Neus Baena, Diana Wellesley, Claude Stoll, C. De Vigan, Maurizio Clementi, and E. Cariati

Subjects

Down syndrome, medicine.medical_specialty, Aneuploidy, Gestational Age, Prenatal diagnosis, Biology, Ultrasonography, Prenatal, Pregnancy, Genetics, medicine, Humans, Mass Screening, Registries, medicine.diagnostic_test, business.industry, Obstetrics, Ultrasound, Pregnancy Outcome, medicine.disease, Europe, Amniocentesis, Gestation, Female, Down Syndrome, business, Trisomy, Maternal Age

Abstract

The objective of this study was to evaluate the contribution of ultrasound scanning to the prenatal detection of trisomy 21 in a large unselected European population. Data from 19 congenital malformation registers in 11 European countries were included. The prenatal ultrasound screening programs in the countries ranged from no routine screening to three ultrasound investigations per patient. Routine serum screening was offered in four of the 11 countries and routine screening on the basis of maternal age amniocentesis in all. The results show that overall 53% of cases of trisomy 21 were detected prenatally with a range from 3% in Lithuania to 88% in Paris. Ninety-eight percent of women whose babies were diagnosed before 24 weeks gestation chose to terminate the pregnancy. Centres/countries that offer serum screening do not have a significantly higher detection rate of trisomy 21 when compared to those that offer maternal age amniocentesis and anomaly scanning only. Fifty percent of trisomy 21 cases were born to women aged 35 years or more. In conclusions, second trimester ultrasound plays an important role in the prenatal diagnosis of trisomy 21. Of those cases prenatally diagnosed, 64% of cases in women

Published

2004

35. Turner syndrome: Evaluation of prenatal diagnosis in 19 European registries

Author

C. De Vigan, E. Cariati, Claude Stoll, Maurizio Clementi, María Rosa Caballín, Miriam Guitart, and Neus Baena

Subjects

medicine.medical_specialty, Pregnancy, Obstetrics, business.industry, Ultrasound, Gestational age, Cystic hygroma, Karyotype, Prenatal diagnosis, medicine.disease, Endocrinology, Internal medicine, Hydrops fetalis, Turner syndrome, Genetics, medicine, business, Genetics (clinical)

Abstract

This study evaluated the prenatal diagnosis of Turner syndrome by ultrasound examination in an unselected population from all over Europe. Data from 19 congenital malformation registries from 11 European countries were analyzed. Turner syndrome was diagnosed in 125 cases (7.2%) in a total of 1,738 chromosome abnormalities. Sixty-seven percent of cases were detected prenatally by ultrasound examination due to the presence of congenital defects. The most frequent anomalies were cystic hygroma (59.5%) and hydrops fetalis (19%). The most frequent karyotype was 45,X (81.6%) followed by different types of mosaicism (16.8%). Significant differences in congenital defects (P = 0.0003) were observed between 45,X karyotypes and 45,X mosaicism cases. Prenatal counseling for 45,X mosaicism should take into account the expectation of a milder phenotype. In 78.6% of cases diagnosed by ultrasound examination due to congenital anomalies, the pregnancy was terminated. Prenatal detection of Turner syndrome by ultrasound examination was high in this unselected population.

Published

2004

36. Genetic Testing in Hereditary Breast and Ovarian Cancer Using Massive Parallel Sequencing

Author

Miriam Guitart, Marina Viñas, Eugeni Saigí, Neus Baena, Gemma Llort, Carmen Yagüe, Miquel Àngel Seguí, Montse Torra, Anna Ruiz, and Anna Brunet

Subjects

endocrine system diseases, Article Subject, DNA Mutational Analysis, lcsh:Medicine, Breast Neoplasms, Biology, Sensitivity and Specificity, General Biochemistry, Genetics and Molecular Biology, DNA sequencing, law.invention, symbols.namesake, law, medicine, False positive paradox, Humans, skin and connective tissue diseases, Polymerase chain reaction, Genetic testing, BRCA2 Protein, Ovarian Neoplasms, Sanger sequencing, Genetics, Massive parallel sequencing, General Immunology and Microbiology, medicine.diagnostic_test, BRCA1 Protein, lcsh:R, High-Throughput Nucleotide Sequencing, General Medicine, Mutation, symbols, Pyrosequencing, Female, Research Article

Abstract

High throughput methods such as next generation sequencing are increasingly used in molecular diagnosis. The aim of this study was to develop a workflow for the detection ofBRCA1andBRCA2mutations using massive parallel sequencing in a 454 GS Junior bench top sequencer. Our approach was first validated in a panel of 23 patients containing 62 unique variants that had been previously Sanger sequenced. Subsequently, 101 patients with familial breast and ovarian cancer were studied.BRCA1andBRCA2exon enrichment has been performed by PCR amplification using the BRCA MASTR kit (Multiplicom). Bioinformatic analysis of reads is performed with the AVA software v2.7 (Roche). In total, all 62 variants were detected resulting in a sensitivity of 100%. 71 false positives were called resulting in a specificity of 97.35%. All of them correspond to deletions located in homopolymeric stretches. The analysis of the homopolymers stretches of 6 bp or longer using the BRCA HP kit (Multiplicom) increased the specificity of the detection ofBRCA1andBRCA2mutations to 99.99%. We show here that massive parallel pyrosequencing can be used as a diagnostic strategy to test forBRCA1andBRCA2mutations meeting very stringent sensitivity and specificity parameters replacing traditional Sanger sequencing with a lower cost.

Published

2014

37. A common cognitive, psychiatric, and dysmorphic phenotype in carriers of NRXN1 deletion

Author

Marina Viñas-Jornet, Núria Ribas-Vidal, Maria Dolors Coll, Anna Ruiz, Miriam Guitart, Susanna Esteba-Castillo, Ramon Novell, Elisabeth Gabau, Joan San, and Neus Baena

Subjects

medicine.medical_specialty, Intellectual disability, Mentally ill, dysexecutive syndrome, Dysexecutive syndrome, Borderline intellectual functioning, Genetics, medicine, anxiety disorder, Bipolar disorder, Psychiatry, Molecular Biology, Genetics (clinical), 2p16.3 deletion, business.industry, Trastorns d'ansietat, Original Articles, medicine.disease, Penetrance, Schizophrenia, intellectual disability, Anxiety disorder, Autism, Malalts mentals, business, Anxiety disorders

Abstract

Altres ajuts: Fundació Parc Taulí - Institut Universitari UAB CIR2009/33 i CIR2010/034 Deletions in the 2p16.3 region that includes the neurexin (NRXN1) gene are associated with intellectual disability and various psychiatric disorders, in particular, autism and schizophrenia. We present three unrelated patients, two adults and one child, in whom we identified an intragenic 2p16.3 deletion within the NRXN1 gene using an oligonucleotide comparative genomic hybridization array. The three patients presented dual diagnosis that consisted of mild intellectual disability and autism and bipolar disorder. Also, they all shared a dysmorphic phenotype characterized by a long face, deep set eyes, and prominent premaxilla. Genetic analysis of family members showed two inherited deletions. A comprehensive neuropsychological examination of the 2p16.3 deletion carriers revealed the same phenotype, characterized by anxiety disorder, borderline intelligence, and dysexecutive syndrome. The cognitive pattern of dysexecutive syndrome with poor working memory and reduced attention switching, mental flexibility, and verbal fluency was the same than those of the adult probands. We suggest that in addition to intellectual disability and psychiatric disease, NRXN1 deletion is a risk factor for a characteristic cognitive and dysmorphic profile. The new cognitive phenotype found in the 2p16.3 deletion carriers suggests that 2p16.3 deletions might have a wide variable expressivity instead of incomplete penetrance.

Published

2014

38. CARE OF GIRLS AND WOMEN WITH TURNER SYNDROME: A GUIDLINE OF THE TURNER SYNDROME STUDY GROUP

Author

TURNER SYNDROME STUDY G.R.O.U.P. Bondy CA, Turner Sindrome Study Group: Turner Sindrome Consensus Study Group: Neus Baena, V. K. Bakalov, B. B. Biesecker, J. C. Carel, G. Conway, M. Davenport, C. Disteche, M. F. Karnis, J. A. Germak, C. H. Gravholt, J. Foodim, D. Gunther, O. Hovatta, A. M. Kappelgard, W. Kiess, K. Landin Wilhelmsen, A. Lin, B. Lippe, M. Loscalzo, K. Lynch, M. M. M. Mazzocco, E. McCauley, P. McDonough, S. M. P. F. de Muinck Keizer Schrama, R. W. Naeraa, C. Quigley, R. Rosenfield, D. Rosing, J. Ross, D. Roulot, K. Rubin, P. Saenger, P. Schmidt, M. Silberbach, V. Sybert, D. L. Van Dyke, A. Zinn, MAZZANTI, LAURA, TURNER SYNDROME STUDY GROUP. Bondy CA and Turner Sindrome Study Group: Turner Sindrome Consensus Study Group: Neus Baena, V. K. Bakalov, B.B. Biesecker, J.C. Carel, G.Conway, M. Davenport, C. Disteche, M. F. Karni, J. A. Germak, C.H. Gravholt, J. Foodim, D. Gunther, O. Hovatta, A.M. Kappelgard, W. Kie, K. Landin-Wilhelmsen, A. Lin, B. Lippe, M. Loscalzo, K. Lynch, L. Mazzanti, M. M. M. Mazzocco, E. McCauley, P. McDonough, S.M.P.F. de Muinck Keizer-Schrama, R. W. Naeraa, C. Quigley, R. Rosenfield, D. Rosing, J. Ro, D. Roulot, K. Rubin, P. Saenger, P. Schmidt, M. Silberbach, V. Sybert, D. L. Van Dyke, and A. Zinn.

Subjects

Adult, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, media_common.quotation_subject, Clinical Biochemistry, MEDLINE, Turner Syndrome, Biochemistry, Bone and Bones, Child health, Presentation, Cognition, Neonatal Screening, Endocrinology, Multidisciplinary approach, Prenatal Diagnosis, Internal medicine, Turner syndrome, Good evidence, medicine, Humans, Child, media_common, Web site, business.industry, Liver Diseases, Estrogen Replacement Therapy, Puberty, Biochemistry (medical), Infant, Newborn, Guideline, medicine.disease, Fertility, Cardiovascular Diseases, Female, business, GROWTH-HORMONE TREATMENT, SEX-CHROMOSOME ABNORMALITIES, LERI-WEILL DYSCHONDROSTEOSIS, CARDIOVASCULAR RISK-FACTORS, CONGENITAL HEART-DISEASE, RANDOMIZED DOSE-RESPONSE, PULMONARY VENOUS RETURN, POPULATION-BASED COHORT, BONE-MINERAL DENSITY, QUALITY-OF-LIFE

Abstract

Objectives: The objective of this work is to provide updated guidelines for the evaluation and treatment of girls and women with Turner syndrome (TS). Participants: The Turner Syndrome Consensus Study Group is a multidisciplinary panel of experts with relevant clinical and research experience with TS that met in Bethesda, Maryland, April 2006. The meeting was supported by the National Institute of Child Health and unrestricted educational grants from pharmaceutical companies. Evidence: The study group used peer-reviewed published information to form its principal recommendations. Expert opinion was used where good evidence was lacking. Consensus: The study group met for 3 d to discuss key issues. Breakout groups focused on genetic, cardiological, auxological, psychological, gynecological, and general medical concerns and drafted recommendations for presentation to the whole group. Draft reports were available for additional comment on the meeting web site. Synthesis of the section reports and final revisions were reviewed by e-mail and approved by whole-group consensus. Conclusions:Wesuggest that parents receiving a prenatal diagnosis of TS be advised of the broad phenotypic spectrum and the good quality of life observed in TS in recent years. We recommend that magnetic resonance angiography be used in addition to echocardiography to evaluate the cardiovascular system and suggest that patients with defined cardiovascular defects be cautioned in regard to pregnancy and certain types of exercise. We recommend that puberty should not be delayed to promote statural growth. We suggest a comprehensive educational evaluation in early childhood to identify potential attention-deficit or nonverbal learning disorders. We suggest that caregivers address the prospect of premature ovarian failure in an open and sensitive manner and emphasize the critical importance of estrogen treatment for feminization and for bone health during the adult years. All individuals with TS require continued monitoring of hearing and thyroid function throughout the lifespan. We suggest that adults with TS be monitored for aortic enlargement, hypertension, diabetes, and dyslipidemia. (J Clin Endocrinol Metab 92: 10–25, 2007) TURNER SYNDROME (TS) affects approximately one in 2500 live-born females (1). This disorder presents the clinician with a challenging array of genetic, developmental, endocrine, cardiovascular, psychosocial, and reproductive issues. There have been important advances in each of these arenas since publication of the previous recommendations for the care of girls and women with TS (2). This paper is based on the proceedings of a multidisciplinary international conference sponsored by the National Institute of Child Health and Human Development (NICHD) in April 2006. Discussions at this conference and the ensuing recommendations have been based upon recent, peer-reviewed scientific publications. However, there are very few TS studies that would qualify as guidance for evidence-based recommendations, and hence

Published

2007

39. Prenatal detection of rare chromosomal autosomal abnormalities in Europe

Author

E. Cariati, María Rosa Caballín, Maurizio Clementi, Miriam Guitart, Claude Stoll, C. De Vigan, Neus Baena, and University of Groningen

Subjects

ANOMALIES, Pathology, medicine.medical_specialty, congenital malformation, rare chromosomal autosomal abnormalities, Prenatal diagnosis, Chromosome Disorders, MOSAICISM, Biology, ULTRASOUND FINDINGS, PHENOTYPE, Ultrasonography, Prenatal, FETUSES, Pregnancy, medicine, Humans, Genetic Testing, Genetics (clinical), Genetic testing, Genetics, Chromosome Aberrations, Fetus, prenatal diagnosis, STRUCTURAL REARRANGEMENTS, medicine.diagnostic_test, ultrasound, DELETION, Chromosome, Cystic hygroma, Congenital malformations, medicine.disease, Europe, TRISOMY-10, congenital anomaly, Cardiac defects, Female

Abstract

The aim of the present study was to evaluate the prenatal detection of rare chromosomal autosomal abnormalities by ultrasound (US) examination. Data were obtained from 19 congenital malformation registries from 11 European countries, between 01/07/96 and 31/12/98. A total of 664,340 births were covered and 7,758 cases with congenital malformations were recorded. Rare autosomal abnormalities were diagnosed in 114 cases (6.6%) from a total of 1,738 chromosome abnormalities. There were a wide variety of autosomal abnormalities: the most common were deletions (33 cases), duplications (32 cases), trisomies of chromosomes 8, 9, 10, 14, 15, and 16 (23 cases), and unbalanced rearrangements (19 cases). Out of these cases, 45.6% were detected prenatally by US examination due to the presence of congenital anomaly. As for the types of chromosomal anomaly, unbalanced rearrangements and deletions were the most frequently detected by US. A high percentage of cases with balanced rearrangements were associated with severe congenital anomalies. The most frequent congenital anomalies detected by US were cystic hygroma (20.6%), central nervous system defects (17.6%), cardiac defects (13.2%), and diaphragm defects (10.3%). This large series offers useful information about prenatal diagnosis by US of congenital defects associated with rare autosomal abnormalities and it provides a valuable knowledge about outcome. Fetal anomalies detected by US that were associated with rare autosomal abnormalities were significantly more frequent than those associated with common chromosomal abnormalities (45.6 vs. 34.7%). This study indicates the need to increase the detection of congenital anomalies by US. (C) 2003 Wiley-Liss, Inc.

Published

2003

40. Detection of Congenital Anomalies by Fetal Ultrasonographic Examination across Europe

Author

Ettore Cariati, Cariati Ettore, Neus Baena, Francesco Benedicenti, Vytautas Kasiulevicius, Algirdas Utkus, and Fabrizio Bianchi

Subjects

Fetus, medicine.medical_specialty, business.industry, Ultrasound screening, Obstetrics, Primary prevention, Public Health, Environmental and Occupational Health, Medicine, Folate supplementation, Prenatal diagnosis, business, Ultrasonographic examination, Genetics (clinical)

Abstract

Objectives: Birth defects are a major health burden. Primary prevention is at present emerging, i.e. folate supplementation. When it is not possible, as is still the case for most birth defects, research is needed to determine how an optimal provision of prenatal diagnosis and use of services can be achieved. Ultrasound scans in the midtrimester of pregnancy are now a routine part of antenatal care in most European countries. The objective of this study was to evaluate the prenatal diagnosis of congenital anomalies by fetal ultrasonographic examination across Europe. Methods: Data from 20 registries of congenital malformations in 12 European countries were included. The prenatal ultrasound screening programs in the countries ranged from no routine screening to 3 fetal scans offered, including 2 for biometric purposes and 1 for search of congenital anomalies, the anomaly scan. Results: There were 8,126 cases with congenital anomalies with an overall prenatal detection rate of 44.3%. Termination of pregnancy was performed in 1,657 cases (21.8%). There was significant variation in the prenatal detection rate between regions with the lowest detection rate in registries of countries without routine fetal screening (Denmark and The Netherlands) and the highest detection rate in registries of countries with at least 1 anomaly scan (France, Germany, Italy, Spain, UK). However, there were large variations among the registries with a high detection rate. There were significant differences in the prenatal detection rate and proportion of induced abortions between isolated anomalies and associated anomalies (chromosomal aberrations, recognized syndromes, and multiple without chromosomal aberrations or recognized syndromes). Conclusions: Prenatal detection rate of congenital anomalies by fetal scan varies significantly between registries of European countries even with the same screening policy. Prenatal detection of congenital anomalies is significantly higher when associated malformations are present. The rate of induced abortions varies between registries of countries even with the same detection rate of congenital anomalies. The variation described may be due to cultural and policy differences.

Published

2002

41. Fetal and placenta chromosome constitution in 237 pregnancy losses

Author

Neus Baena, Francisco Mellado, Miriam Guitart, María Rosa Caballín, Elisabet Gabau, Josep Egozcue, Manuel Corona, and Joan Carles Ferreres

Subjects

Adult, medicine.medical_specialty, Amniotic fluid, Placenta, Chromosome Disorders, Biology, Abortion, Congenital Abnormalities, Fetus, Pregnancy, Culture Techniques, Infant Mortality, Genetics, medicine, Humans, Fetal Death, reproductive and urinary physiology, Ultrasonography, Chromosome Aberrations, Obstetrics, Infant, Newborn, Karyotype, Abortion, Induced, medicine.disease, medicine.anatomical_structure, Cartilage, Phenotype, Karyotyping, Immunology, Chromosome abnormality, Gestation, Female

Abstract

The aim of the study was to carry out cytogenetic analyses in pregnancy losses. Samples of cartilage and placenta tissue were obtained prospectively from 237 pregnancy losses of more than 16 weeks of gestation (130 stillbirths, 97 induced abortions and 10 early neonatal deaths). Cartilage culture was performed in 222 samples and placental culture was initiated in 224. The overall culture success rate was 83.5%, 72.3% in stillbirths, 97% in induced abortions and 100% in early neonatal death. An abnormal karyotype was detected in 52 cases: 6.9% in stillbirths, 43.6% in induced abortions and 20% in early neonatal deaths. The rate of discrepancy between the prenatal cytogenetic results in amniotic fluid and the post-termination karyotype was 3%. The tissue of choice for cytogenetic analysis was cartilage in induced abortions and early neonatal death, and placenta in stillbirth. The majority of cases had a chromosome abnormality: multiple congenital anomalies in 74.6%, and a single major anomaly in 9.7%.

Published

2001

42. Contribution of ultrasonographic examination to the prenatal detection of chromosomal abnormalities in 19 centres across Europe

Author

C. De Vigan, Neus Baena, Claude Stoll, Maurizio Clementi, and E. Cariati

Subjects

Adult, medicine.medical_specialty, Down syndrome, Population, Aneuploidy, Turner Syndrome, Prenatal diagnosis, Trisomy, Biology, Ultrasonography, Prenatal, Pregnancy, Turner syndrome, Genetics, medicine, Humans, Abnormalities, Multiple, Registries, education, Chromosome Aberrations, education.field_of_study, Obstetrics, Pregnancy Outcome, medicine.disease, Europe, Female, Lymphangioma, Cystic, Klinefelter syndrome, Down Syndrome, Artifacts

Abstract

The objective of this study was to evaluate the prenatal detection of chromosomal abnormalities by fetal ultrasonographic examination in a large database provided by 19 Registries of Congenital Anomalies from 11 European countries. This study included 1738 cases of chromosomal abnormalities, liveborn, stillborn or termination of pregnancy regardless of maternal age from a population of 664,340 births during the period 1996 - 1998. The most frequent chromosomal anomalies were Down syndrome (n=1050), trisomy 18 (n=191), Turner syndrome (n=125), trisomy 13 (n=86), and triploidy (n=56). Fetal ultrasonographic examination resulted in the prenatal detection of 37.7% of the chromosomal abnormalities, thereby resulting in a reduction of 28.6% in their prevalence at birth due to terminations of pregnancy. The detection rate by ultrasound examination varied according to local policies of prenatal diagnosis : it was lower in countries where routine scan were not performed and higher in countries in which at least one routine anomaly scan during the second trimester of pregnancy was performed. The ultrasound detection varied according to the specific chromosomal anomaly and was lowest for Klinefelter syndrome (5.7%) and highest for triploidy (78.6%). For Down syndrome it was 26.4%. Termination of pregnancy was performed in 75.9% of the cases. Among the 655 cases detected by ultrasound, the most frequent ultrasound signs by category of chromosomal abnormalities were analysed. This study shows that ultrasound screening is an important tool in the prenatal detection of chromosomal abnormalities in Europe, leading to a significant reduction in the prevalence of livebirth children with chromosomal anomalies.

Published

2001

43. KIF6 gene as a pharmacogenetic marker for lipid-lowering effect in statin treatment

Author

Cristina Ruiz-Iruela, Jose Luis Puzo-Foncilla, Ariadna Padró-Miquel, Xavier Pintó-Sala, Assumpta Caixàs-Pedragós, Neus Baena-Díez, Rosa Navarro-Badal, Pilar Calmarza, Pedro Alía-Ramos, Beatriz Candás-Estébanez, Xavier Jusmet-Miguel, Roser Güell-Miró, and Universitat de Barcelona

Subjects

Male, Simvastatin, Heredity, Atorvastatin, lcsh:Medicine, Kinesins, 030204 cardiovascular system & hematology, Pharmacology, Biochemistry, Biomarkers, Pharmacological, chemistry.chemical_compound, 0302 clinical medicine, Medicine and Health Sciences, Medicine, 030212 general & internal medicine, Prospective Studies, Rosuvastatin Calcium, lcsh:Science, Multidisciplinary, Pharmaceutics, Anticholesteremic Agents, Drugs, Antilipemic agents, Middle Aged, Lipids, Lipid Profiles, Genetic Mapping, Cardiovascular diseases, Cholesterol, Female, lipids (amino acids, peptides, and proteins), Colesterol, medicine.drug, Research Article, Hypercholesterolemia, Motor Proteins, Mutation, Missense, Variant Genotypes, Agents antilipèmics, Lower risk, 03 medical and health sciences, Pharmacotherapy, Drug Therapy, Molecular Motors, Genetics, Humans, Rosuvastatin, business.industry, Malalties cardiovasculars, lcsh:R, Statins, Biology and Life Sciences, Proteins, nutritional and metabolic diseases, Human Genetics, Cholesterol, LDL, DNA, Cell Biology, Pharmacogenomic Testing, chemistry, KIF6, lcsh:Q, Hydroxymethylglutaryl-CoA Reductase Inhibitors, business, Pharmacogenetics

Abstract

Introduction The therapeutic response to statins has a high interindividual variability with respect to reductions in plasma LDL-cholesterol (c-LDL) and increases in HDL cholesterol (c-HDL). Many studies suggest that there is a relationship between the rs20455 KIF6 gene variant (c.2155T> C, Trp719Arg) and a lower risk of cardiovascular disease in patients being treated with statins. Aim The aim of this study was to investigate whether or not the c.2155T> C KIF6 gene variant modulates the hypercholesteremic effects of treatment with simvastatin, atorvastatin, or rosuvastatin. Materials and methods This was a prospective, observational and multicenter study. Three hundred and forty-four patients who had not undergone prior lipid-lowering treatment were recruited. Simvastatin, atorvastatin or rosuvastatin were administered. Lipid profiles and multiple clinical and biochemical variables were assessed before and after treatment. Results The c.2155T> C variant of the KIF6 gene was shown to influence physiological responses to treatment with simvastatin and atorvastatin. Patients who were homozygous for the c.2155T> C variant (CC genotype, ArgArg) had a 7.0% smaller reduction of LDL cholesterol levels (p = 0.015) in response to hypolipidemic treatment compared to patients with the TT (TrpTrp) or CT (TrpArg) genotype. After pharmacological treatment with rosuvastatin, patients carrying the genetic variant had an increase in c-HDL that was 21.9% lower compared to patients who did not carry the variant (p = 0.008). Conclusion Being a carrier of the c.2155T> C variant of the KIF6 gene negatively impacts patient responses to simvastatin, atorvastatin or rosuvastatin in terms of lipid lowering effect. Increasing the intensity of hypolipidemic therapy may be advisable for patients who are positive for the c.2155T> C variant.

44. Prenatal ultrasound diagnosis of congenital diaphragmatic hernia - Associated malformations, chromosomal abnormalities and pregnancy outcome

Author

Barišić, I., Garne, E., Clementi, M., Häusler, M., Gjergja, R., Stoll, C., Žužek, A., Vondraček, N., Mozetič, Z. M., Vigan, C., Vodovar, V., Alembik, Y., Dott, B., Froster, U. G., Queisser-Luft, A., Wiesel, A., Tenconi, R., Benedicenti, F., Bianca, S., Ettore, G., Cariati, E., Bianchi, F., Lithuania Kucinskas, V., Utkus, A., Walle, H. E. K., Zandwijken, G. R. J., Salvador, J., Garcia-Minaur, S., Aranguren, G., Neus Baena, Addor, M. -C, Pescia, G., Oshovska, T., Gordienko, I., Boyd, P. A., and Wellesley, D. G.

45. Origin of trisomy 21 in Down syndrome cases from a Spanish population registry

Author

Neus Baena, Josep Egozcue, Eulàlia Solsona, M.Rosa Caballín, David Gómez, Elisabeth Gabau, and Miriam Guitart

Subjects

Adult, Genetic Markers, Male, medicine.medical_specialty, Down syndrome, Chromosomes, Human, Pair 21, Offspring, Population, Aneuploidy, Biology, Congenital Abnormalities, Genomic Imprinting, Meiosis, Pregnancy, Prevalence, Genetics, medicine, Humans, Registries, education, Gynecology, education.field_of_study, Meiosis II, Infant, Newborn, Chromosome Mapping, Abortion, Induced, medicine.disease, Spain, Female, Down Syndrome, Trisomy, Chromosome 21, Maternal Age, Microsatellite Repeats

Abstract

We have carried out a population-based study on the origin of the extra chromosome 21 in 38 families with Down syndrome (DS) offspring in El Valles (Spain). From 1991 to 1994, a higher prevalence of DS (22.7/10000 live births, stillbirths and induced abortions) was found compared to the majority of EUROCAT registries. The distribution of trisomy 21 by origin was 88% maternal (90.6% meiosis I, 6.2% meiosis II, 3.1% maternal mosaicism), 5.6% paternal (50% meiosis I, 50% meiosis II) and 5.6% mitotic. The percentage of parental mosaicism was 2.7%. These percentages are similar to those previously reported. Recombination study revealed a maternal meiosis I genetic map of 32.68 cM (approximately one-half the length of the normal female map). Mean maternal age among non-recombinant cases involving MI errors was significantly lower (31.1 years) than among those cases showing one observable crossover (36.1 years) (P