Search

Your search keyword '"A Krebsova"' showing total 147 results
Start Over Author "A Krebsova"
147 results on '"A Krebsova"'

1. Genotype is associated with left ventricular reverse remodelling and early events in recent‐onset dilated cardiomyopathy

Author

Milos Kubanek, Jana Binova, Lenka Piherova, Alice Krebsova, Martin Kotrc, Hana Hartmannova, Katerina Hodanova, Dita Musalkova, Viktor Stranecky, Tomas Palecek, Anna Chaloupka, Ilga Grochova, Jan Krejci, Jana Petrkova, Vojtech Melenovsky, Stanislav Kmoch, and Josef Kautzner

Subjects
Genetics, Left ventricular reverse remodelling, Prognosis, Recent‐onset dilated cardiomyopathy, Whole‐exome sequencing, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Abstract Aims Recent‐onset dilated cardiomyopathy (RODCM) is characterized by heterogeneous aetiology and diverse clinical outcomes, with scarce data on genotype–phenotype correlates. Our aim was to correlate individual RODCM genotypes with left ventricular reverse remodelling (LVRR) and clinical outcomes. Methods and results In this prospective study, a total of 386 Czech RODCM patients with symptom duration ≤6 months underwent genetic counselling and whole‐exome sequencing (WES). The presence of pathogenic (class 5) or likely pathogenic (class 4) variants in a set of 72 cardiomyopathy‐related genes was correlated with the occurrence of all‐cause death, heart transplantation, or implantation of a ventricular assist device (primary outcome) and/or ventricular arrhythmia event (secondary outcome). LVRR was defined as an improvement of left ventricular ejection fraction to >50% or ≥10% absolute increase, with a left ventricular end‐diastolic diameter ≤33 mm/m2 or ≥10% relative decrease. Median follow‐up was 41 months. RODCM was familial in 98 (25%) individuals. Class 4–5 variants of interest (VOIs) were identified in 125 (32%) cases, with 69 (18%) having a single titin‐truncating variant (TTNtv) and 56 (14%) having non‐titin (non‐TTN) VOIs. The presence of class 4–5 non‐TTN VOIs, but not of TTNtv, heralded a lower probability of 12‐month LVRR and proved to be an independent baseline predictor both of the primary and the secondary outcome. The negative result of genetic testing was a strong protective baseline variable against occurrence of life‐threatening ventricular arrhythmias. Detection of class 4–5 VOIs in genes coding nuclear envelope proteins was another independent predictor of both study outcomes at baseline and also of life‐threatening ventricular arrhythmias after 12 months. Class 4–5 VOIs of genes coding cytoskeleton were associated with an increased risk of life‐threatening ventricular arrhythmias after baseline assessment. A positive family history of dilated cardiomyopathy alone only related to a lower probability of LVRR at 12 months and at the final follow‐up. Conclusions RODCM patients harbouring class 4–5 non‐TTN VOIs are at higher risk of progressive heart failure and life‐threatening ventricular arrhythmias. Genotyping may improve their early risk stratification at baseline assessment.

Published
2024
Full Text
View/download PDF

2. Pregnancy in women with dilated cardiomyopathy genetic variants

Author

Restrepo-Córdoba, María Alejandra, Chmielewski, Przemyslaw, Truszkowska, Grażyna, Peña-Peña, María Luisa, Kubánek, Miloš, Krebsová, Alice, Lopes, Luis R., García-Ropero, Álvaro, Merlo, Marco, Paldino, Alessia, Peters, Stacey, Jurcut, Ruxandra, Barriales-Villa, Roberto, Zorio, Esther, Hazebroek, Mark, Mogensen, Jens, and García-Pavía, Pablo

Published
2025
Full Text
View/download PDF

4. Genotype is associated with left ventricular reverse remodelling and early events in recent‐onset dilated cardiomyopathy.

Author

Kubanek, Milos, Binova, Jana, Piherova, Lenka, Krebsova, Alice, Kotrc, Martin, Hartmannova, Hana, Hodanova, Katerina, Musalkova, Dita, Stranecky, Viktor, Palecek, Tomas, Chaloupka, Anna, Grochova, Ilga, Krejci, Jan, Petrkova, Jana, Melenovsky, Vojtech, Kmoch, Stanislav, and Kautzner, Josef

Abstract

Aims: Recent‐onset dilated cardiomyopathy (RODCM) is characterized by heterogeneous aetiology and diverse clinical outcomes, with scarce data on genotype–phenotype correlates. Our aim was to correlate individual RODCM genotypes with left ventricular reverse remodelling (LVRR) and clinical outcomes. Methods and results: In this prospective study, a total of 386 Czech RODCM patients with symptom duration ≤6 months underwent genetic counselling and whole‐exome sequencing (WES). The presence of pathogenic (class 5) or likely pathogenic (class 4) variants in a set of 72 cardiomyopathy‐related genes was correlated with the occurrence of all‐cause death, heart transplantation, or implantation of a ventricular assist device (primary outcome) and/or ventricular arrhythmia event (secondary outcome). LVRR was defined as an improvement of left ventricular ejection fraction to >50% or ≥10% absolute increase, with a left ventricular end‐diastolic diameter ≤33 mm/m2 or ≥10% relative decrease. Median follow‐up was 41 months. RODCM was familial in 98 (25%) individuals. Class 4–5 variants of interest (VOIs) were identified in 125 (32%) cases, with 69 (18%) having a single titin‐truncating variant (TTNtv) and 56 (14%) having non‐titin (non‐TTN) VOIs. The presence of class 4–5 non‐TTN VOIs, but not of TTNtv, heralded a lower probability of 12‐month LVRR and proved to be an independent baseline predictor both of the primary and the secondary outcome. The negative result of genetic testing was a strong protective baseline variable against occurrence of life‐threatening ventricular arrhythmias. Detection of class 4–5 VOIs in genes coding nuclear envelope proteins was another independent predictor of both study outcomes at baseline and also of life‐threatening ventricular arrhythmias after 12 months. Class 4–5 VOIs of genes coding cytoskeleton were associated with an increased risk of life‐threatening ventricular arrhythmias after baseline assessment. A positive family history of dilated cardiomyopathy alone only related to a lower probability of LVRR at 12 months and at the final follow‐up. Conclusions: RODCM patients harbouring class 4–5 non‐TTN VOIs are at higher risk of progressive heart failure and life‐threatening ventricular arrhythmias. Genotyping may improve their early risk stratification at baseline assessment. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

6. Danon disease is an underdiagnosed cause of advanced heart failure in young female patients: a LAMP2 flow cytometric study

Author

Jiri Gurka, Lenka Piherova, Filip Majer, Anna Chaloupka, Daniela Zakova, Ondrej Pelak, Alice Krebsova, Petr Peichl, Jan Krejci, Tomas Freiberger, Vojtech Melenovsky, Josef Kautzner, Tomas Kalina, Jakub Sikora, and Milos Kubanek

Subjects
Advanced heart failure, Danon disease, Lysosomal‐associated membrane protein type 2, Screening, White blood cells, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Abstract Aims Danon disease (DD) is a rare X‐linked disorder caused by mutations in the lysosomal‐associated membrane protein type 2 gene (LAMP2). DD is difficult to distinguish from other causes of dilated or hypertrophic cardiomyopathy (HCM) in female patients. As DD female patients regularly progress into advanced heart failure (AHF) aged 20–40 years, their early identification is critical to improve patient survival and facilitate genetic counselling. In this study, we evaluated the prevalence of DD among female patients with non‐ischemic cardiomyopathy, who reached AHF and were younger than 40 years. Methods and results The study cohort comprised 60 female patients: 47 (78%) heart transplant recipients, 2 (3%) patients treated with ventricular assist device, and 11 (18%) patients undergoing pre‐transplant assessment. Aetiology of the cardiomyopathy was known in 15 patients (including two DD patients). LAMP2 expression in peripheral white blood cells (WBC) was tested by flow cytometry (FC) in the remaining 45 female patients. Whole exome sequencing was used as an alternative independent testing method to FC. Five additional female DD patients (two with different novel LAMP2 mutations) were identified by FC. The total prevalence of DD in this cohort was 12%. HCM phenotype (57% vs. 9%, *P = 0.022) and delta waves identified by electrocardiography (43% vs. 0%, **P = 0.002) were significantly more frequent in DD female patients. Conclusions Danon disease is an underdiagnosed cause of AHF in young female patients. LAMP2 expression testing in peripheral WBCs by FC can be used as an effective screening/diagnostic tool to identify DD in this patient population.

Published
2020
Full Text
View/download PDF

9. Natural History of MYH7-Related Dilated Cardiomyopathy

Author

Fernando de Frutos, Juan Pablo Ochoa, Marina Navarro-Peñalver, Annette Baas, Jesper Vandborg Bjerre, Esther Zorio, Irene Méndez, Rebeca Lorca, Job A.J. Verdonschot, Pablo Elpidio García-Granja, Zofia Bilinska, Diane Fatkin, M. Eugenia Fuentes-Cañamero, José M. García-Pinilla, María I. García-Álvarez, Francesca Girolami, Roberto Barriales-Villa, Carles Díez-López, Luis R. Lopes, Karim Wahbi, Ana García-Álvarez, Ibon Rodríguez-Sánchez, Javier Rekondo-Olaetxea, José F. Rodríguez-Palomares, María Gallego-Delgado, Benjamin Meder, Milos Kubanek, Frederikke G. Hansen, María Alejandra Restrepo-Córdoba, Julián Palomino-Doza, Luis Ruiz-Guerrero, Georgia Sarquella-Brugada, Alberto José Perez-Perez, Francisco José Bermúdez-Jiménez, Tomas Ripoll-Vera, Torsten Bloch Rasmussen, Mark Jansen, Maria Sabater-Molina, Perry M. Elliot, Pablo Garcia-Pavia, Eva Cabrera-Romero, Marta Cobo-Marcos, Luis Escobar-Lopez, Fernando Domínguez, Esther González-López, Juan Ramón Gimeno-Blanes, Dennis Dooijes, Bernabé López Ledesma, Inés Roche Fortea, Javier Bermejo, Maria Angeles Espinosa, Ana Isabel Fernández, Silvia Vilches, Cristina Gómez, Juan Gómez, Eliecer Coto, José Julián Rodríguez Reguero, S.R.B. Heymans, H.G. Brunner, Javier López-Díaz, Grażyna Truszkowska, Rafal Ploski, Przemysław Chmielewski, Renee Johnson, Ainhoa Robles-Mezcua, Arancha Díaz-Expósito, Alejandro I. Pérez-Cabeza, Clara Jiménez-Rubio, Vicente Climent Payá, Silvia Favilli, Petros Syrris, Douglas Cannie, Clarisse Billon, Angela Lopez-Sainz, Margarita Calvo, Ángela Cacicedo Fernández de Bobadilla, Jose Juan Onaindia-Gandarias, Larraitz Gaztañaga-Arantzamendi, Estibaliz Zamarreño-Golvano, Javier Limeres, Laura Gutiérrez-García, Eduardo Villacorta, Jan Haas, Alice Krebsova, Jens Mogensen, Sergi Cesar, Oscar Campuzano, Raúl Franco Gutiérrez, Jorge Alvarez-Rubio, David Cremer-Luengos, Guido Antoniutti, Fiama Caimi-Martinez, Rosa Macías, Juan Jiménez-Jáimez, María Luisa Peña-Peña, Salvador Lucas Díez-Aja López, Tania Pino Acereda, Blanca Arnáez Corada, Jesús Piqueras-Flores, Martin Negreira-Caamaño, Jorge Martinez-del Río, María Victoria Mogollón Jiménez, Elena Villanueva, José Luis Gonzáles, Adrián Fernández, Ulises Toscanini, Lilian E. Favaloro, Carlota Hernández Díez, MUMC+: DA KG Lab Bedrijfsbureau (9), MUMC+: DA KG AIOS (9), RS: Carim - H02 Cardiomyopathy, Instituto de Salud Carlos III, Unión Europea. Fondo Europeo de Desarrollo Regional (FEDER/ERDF), Ministerio de Ciencia e Innovación (España), Fundación ProCNIC, Ministerio de Ciencia e Innovación. Centro de Excelencia Severo Ochoa (España), European Reference Network for Rare and Low Prevalence Complex Diseases of the Heart, ERA-CVD framework, Dutch Heart Foundation, Victor Chang Cardiac Research Institute, NSW Health, Clinical Academic Research Partnerships (CARP), Deutsches Zentrum für Herz-Kreislauf-Forschung (German Center for Cardiovascular Research), Informatics for Life (Klaus Tschira Foundation), Ministry of Health, Czech Republic, and Institute for Clinical and Experimental Medicine–IKEM

Subjects
Adult, Cardiomyopathy, Dilated, Heart Failure, Male, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Myocardiopathies, Adolescent, Myosin Heavy Chains, Ventricular Remodeling, Miocardiopaties, Arrhythmias, Cardiac, Middle Aged, dilated cardiomyopathy, Young Adult, Phenotype, MYH7, Genetics, Humans, Female, genetics, Cardiology and Cardiovascular Medicine, Cardiac Myosins, Genètica
Abstract

Instituto de Salud Carlos III (ISCIII), European Regional Development Fund/European Social Fund "A way to make Europe"/" Investing in your future" [PI18/0004, PI20/0320, PT17/0015/0043]; ISCIII; MCIN; Pro-CNIC Foundation; Severo Ochoa Centers of Excellence program [CEX2020-001041-S]; ISCIII [CM20/00101], Frutos F. de, Ochoa JP, Navarro-Peñalver M, Baas A, Bjerre JV, Zorio E, Méndez I, Lorca R, Verdonschot JAJ, García-Granja PE, Bilinska Z, Fatkin D, Fuentes-Cañamero ME, García-Pinilla JM, García-Álvarez MI, Girolami F, Barriales-Villa R, Díez-López C, Lopes LR, Wahbi K, García-Álvarez A, Rodríguez-Sánchez I, Rekondo-Olaetxea J, Rodríguez-Palomares JF, Gallego-Delgado M, Meder B, Kubanek M, Hansen FG, Restrepo-Córdoba MA, Palomino-Doza J, Ruiz-Guerrero L, Sarquella-Brugada G, Perez-Perez AJ, Bermúdez-Jiménez FJ, Ripoll-Vera T, Rasmussen TB, Jansen M, Sabater-Molina M, Elliot PM, Garcia-Pavia P; European Genetic Cardiomyopathies Initiative Investigators

Published
2022
Full Text
View/download PDF

10. Natural History of MYH7-Related Dilated Cardiomyopathy

Author

de Frutos, Fernando, primary, Ochoa, Juan Pablo, additional, Navarro-Peñalver, Marina, additional, Baas, Annette, additional, Bjerre, Jesper Vandborg, additional, Zorio, Esther, additional, Méndez, Irene, additional, Lorca, Rebeca, additional, Verdonschot, Job A.J., additional, García-Granja, Pablo Elpidio, additional, Bilinska, Zofia, additional, Fatkin, Diane, additional, Fuentes-Cañamero, M. Eugenia, additional, García-Pinilla, José M., additional, García-Álvarez, María I., additional, Girolami, Francesca, additional, Barriales-Villa, Roberto, additional, Díez-López, Carles, additional, Lopes, Luis R., additional, Wahbi, Karim, additional, García-Álvarez, Ana, additional, Rodríguez-Sánchez, Ibon, additional, Rekondo-Olaetxea, Javier, additional, Rodríguez-Palomares, José F., additional, Gallego-Delgado, María, additional, Meder, Benjamin, additional, Kubanek, Milos, additional, Hansen, Frederikke G., additional, Restrepo-Córdoba, María Alejandra, additional, Palomino-Doza, Julián, additional, Ruiz-Guerrero, Luis, additional, Sarquella-Brugada, Georgia, additional, Perez-Perez, Alberto José, additional, Bermúdez-Jiménez, Francisco José, additional, Ripoll-Vera, Tomas, additional, Rasmussen, Torsten Bloch, additional, Jansen, Mark, additional, Sabater-Molina, Maria, additional, Elliot, Perry M., additional, Garcia-Pavia, Pablo, additional, Cabrera-Romero, Eva, additional, Cobo-Marcos, Marta, additional, Escobar-Lopez, Luis, additional, Domínguez, Fernando, additional, González-López, Esther, additional, Gimeno-Blanes, Juan Ramón, additional, Dooijes, Dennis, additional, López Ledesma, Bernabé, additional, Roche Fortea, Inés, additional, Bermejo, Javier, additional, Espinosa, Maria Angeles, additional, Fernández, Ana Isabel, additional, Vilches, Silvia, additional, Gómez, Cristina, additional, Gómez, Juan, additional, Coto, Eliecer, additional, Rodríguez Reguero, José Julián, additional, Heymans, S.R.B., additional, Brunner, H.G., additional, López-Díaz, Javier, additional, Truszkowska, Grażyna, additional, Ploski, Rafal, additional, Chmielewski, Przemysław, additional, Johnson, Renee, additional, Robles-Mezcua, Ainhoa, additional, Díaz-Expósito, Arancha, additional, Pérez-Cabeza, Alejandro I., additional, Jiménez-Rubio, Clara, additional, Payá, Vicente Climent, additional, Favilli, Silvia, additional, Syrris, Petros, additional, Cannie, Douglas, additional, Billon, Clarisse, additional, Lopez-Sainz, Angela, additional, Calvo, Margarita, additional, Fernández de Bobadilla, Ángela Cacicedo, additional, Onaindia-Gandarias, Jose Juan, additional, Gaztañaga-Arantzamendi, Larraitz, additional, Zamarreño-Golvano, Estibaliz, additional, Limeres, Javier, additional, Gutiérrez-García, Laura, additional, Villacorta, Eduardo, additional, Haas, Jan, additional, Krebsova, Alice, additional, Mogensen, Jens, additional, Cesar, Sergi, additional, Campuzano, Oscar, additional, Gutiérrez, Raúl Franco, additional, Alvarez-Rubio, Jorge, additional, Cremer-Luengos, David, additional, Antoniutti, Guido, additional, Caimi-Martinez, Fiama, additional, Macías, Rosa, additional, Jiménez-Jáimez, Juan, additional, Peña-Peña, María Luisa, additional, Díez-Aja López, Salvador Lucas, additional, Acereda, Tania Pino, additional, Corada, Blanca Arnáez, additional, Piqueras-Flores, Jesús, additional, Negreira-Caamaño, Martin, additional, Río, Jorge Martinez-del, additional, Mogollón Jiménez, María Victoria, additional, Villanueva, Elena, additional, Gonzáles, José Luis, additional, Fernández, Adrián, additional, Toscanini, Ulises, additional, Favaloro, Lilian E., additional, and Díez, Carlota Hernández, additional

Published
2022
Full Text
View/download PDF

11. Corrigendum: Candidate Gene Resequencing in a Large Bicuspid Aortic Valve-Associated Thoracic Aortic Aneurysm Cohort: SMAD6 as an Important Contributor

Author

Elisabeth Gillis, Ajay A. Kumar, Ilse Luyckx, Christoph Preuss, Elyssa Cannaerts, Gerarda van de Beek, Björn Wieschendorf, Maaike Alaerts, Nikhita Bolar, Geert Vandeweyer, Josephina Meester, Florian Wünnemann, Russell A. Gould, Rustam Zhurayev, Dmytro Zerbino, Salah A. Mohamed, Seema Mital, Luc Mertens, Hanna M. Björck, Anders Franco-Cereceda, Andrew S. McCallion, Lut Van Laer, Judith M. A. Verhagen, Ingrid M. B. H. van de Laar, Marja W. Wessels, Emmanuel Messas, Guillaume Goudot, Michaela Nemcikova, Alice Krebsova, Marlies Kempers, Simone Salemink, Toon Duijnhouwer, Xavier Jeunemaitre, Juliette Albuisson, Per Eriksson, Gregor Andelfinger, Harry C. Dietz, Aline Verstraeten, Bart L. Loeys, and Mibava Leducq Consortium

Subjects
bicuspid aortic valve, thoracic aortic aneurysm, SMAD6, targeted gene panel, variant burden test, Physiology, QP1-981
Published
2017
Full Text
View/download PDF

12. Candidate Gene Resequencing in a Large Bicuspid Aortic Valve-Associated Thoracic Aortic Aneurysm Cohort: SMAD6 as an Important Contributor

Author

Elisabeth Gillis, Ajay A. Kumar, Ilse Luyckx, Christoph Preuss, Elyssa Cannaerts, Gerarda van de Beek, Björn Wieschendorf, Maaike Alaerts, Nikhita Bolar, Geert Vandeweyer, Josephina Meester, Florian Wünnemann, Russell A. Gould, Rustam Zhurayev, Dmytro Zerbino, Salah A. Mohamed, Seema Mital, Luc Mertens, Hanna M. Björck, Anders Franco-Cereceda, Andrew S. McCallion, Lut Van Laer, Judith M. A. Verhagen, Ingrid M. B. H. van de Laar, Marja W. Wessels, Emmanuel Messas, Guillaume Goudot, Michaela Nemcikova, Alice Krebsova, Marlies Kempers, Simone Salemink, Toon Duijnhouwer, Xavier Jeunemaitre, Juliette Albuisson, Per Eriksson, Gregor Andelfinger, Harry C. Dietz, Aline Verstraeten, Bart L. Loeys, and Mibava Leducq Consortium

Subjects
bicuspid aortic valve, thoracic aortic aneurysm, SMAD6, targeted gene panel, variant burden test, Physiology, QP1-981
Abstract

Bicuspid aortic valve (BAV) is the most common congenital heart defect. Although many BAV patients remain asymptomatic, at least 20% develop thoracic aortic aneurysm (TAA). Historically, BAV-related TAA was considered as a hemodynamic consequence of the valve defect. Multiple lines of evidence currently suggest that genetic determinants contribute to the pathogenesis of both BAV and TAA in affected individuals. Despite high heritability, only very few genes have been linked to BAV or BAV/TAA, such as NOTCH1, SMAD6, and MAT2A. Moreover, they only explain a minority of patients. Other candidate genes have been suggested based on the presence of BAV in knockout mouse models (e.g., GATA5, NOS3) or in syndromic (e.g., TGFBR1/2, TGFB2/3) or non-syndromic (e.g., ACTA2) TAA forms. We hypothesized that rare genetic variants in these genes may be enriched in patients presenting with both BAV and TAA. We performed targeted resequencing of 22 candidate genes using Haloplex target enrichment in a strictly defined BAV/TAA cohort (n = 441; BAV in addition to an aortic root or ascendens diameter ≥ 4.0 cm in adults, or a Z-score ≥ 3 in children) and in a collection of healthy controls with normal echocardiographic evaluation (n = 183). After additional burden analysis against the Exome Aggregation Consortium database, the strongest candidate susceptibility gene was SMAD6 (p = 0.002), with 2.5% (n = 11) of BAV/TAA patients harboring causal variants, including two nonsense, one in-frame deletion and two frameshift mutations. All six missense mutations were located in the functionally important MH1 and MH2 domains. In conclusion, we report a significant contribution of SMAD6 mutations to the etiology of the BAV/TAA phenotype.

Published
2017
Full Text
View/download PDF

14. Copy number variation analysis in bicuspid aortic valve-related aortopathy identifies TBX20 as a contributing gene

Author

Luyckx, I, Kumar, AA, Reyniers, E, Dekeyser, E, Vanderstraeten, K, Vandeweyer, G, Wunnemann, F, Preuss, C, Mazzella, JM, Goudot, G, Messas, E, Albuisson, J, Jeunemaitre, X, Eriksson, P, Mohamed, SA, Kempers, M, Salemink, S, Duijnhouwer, A, Andelfinger, G, Dietz, HC, Verstraeten, A (Aline), Van Laer, L, Loeys, BL, Zhurayev, R, Zerbino, D, Mital, S, Mertens, L, Franco-Cereceda, A, Verhagen, Judith, De Graaf - van de Laar, Ingrid, Wessels, Marja, Nemcikova, M, Krebsova, A, Clinical Genetics, MIBAVA Leducq Consortium, Goudot, Guillaume, University of Antwerp (UA), Centre de recherche du CHU Sainte-Justine / Research Center of the Sainte-Justine University Hospital [Montreal, Canada], Université de Montréal (UdeM)-CHU Sainte Justine [Montréal], The Jackson Laboratory [Bar Harbor] (JAX), Centre de Réféfence des Maladies Vasculaires Rares [HEGP, APHP] (CRMVR), Hôpital Européen Georges Pompidou [APHP] (HEGP), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO)-Université Paris Descartes - Paris 5 (UPD5), Karolinska Institutet [Stockholm], Karolinska University Hospital [Stockholm], University Medical Center of Schleswig–Holstein = Universitätsklinikum Schleswig-Holstein (UKSH), Kiel University, Radboud University Medical Center [Nijmegen], Howard Hughes Medical Institute (HHMI), Johns Hopkins University School of Medicine [Baltimore], and MIBAVA Leducq Consortium: Rustam Zhurayev, Dmytro Zerbino, Seema Mital, Luc Mertens, Anders Franco-Cereceda, Judith M A Verhagen, Ingrid M B H van de Laar, Marja W Wessels, Michaela Nemcikova, Alice Krebsova

Subjects
Adult, Heart Defects, Congenital, Male, Candidate gene, DNA Copy Number Variations, [SDV]Life Sciences [q-bio], Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], Population, Heart Valve Diseases, Genome-wide association study, Disease, complex mixtures, Article, 03 medical and health sciences, Aortic aneurysm, All institutes and research themes of the Radboud University Medical Center, Bicuspid aortic valve, Bicuspid Aortic Valve Disease, Databases, Genetic, parasitic diseases, Genetics, medicine, Humans, Copy-number variation, education, Biology, Genetics (clinical), 0303 health sciences, education.field_of_study, Aortic Aneurysm, Thoracic, business.industry, 030305 genetics & heredity, Middle Aged, medicine.disease, Phenotype, digestive system diseases, [SDV] Life Sciences [q-bio], Chemistry, Aortic Valve, Female, Human medicine, T-Box Domain Proteins, business, Genome-Wide Association Study, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]
Abstract

International audience; Bicuspid aortic valve (BAV) is the most common congenital heart defect (CHD), affecting 1-2% of the population. BAV is associated with thoracic aortic aneurysms (TAAs). Deleterious copy number variations (CNVs) were found previously in up to 10% of CHD cases. This study aimed at unravelling the contribution of deleterious deletions or duplications in 95 unrelated BAV/TAA patients. Seven unique or rare CNVs were validated, harbouring protein-coding genes with a role in the cardiovascular system. Based on the presence of overlapping CNVs in patients with cardiovascular phenotypes in the DECIPHER database, the identification of similar CNVs in whole-exome sequencing data of 67 BAV/TAA patients and suggested topological domain involvement from Hi-C data, supportive evidence was obtained for two genes (DGCR6 and TBX20) of the seven initially validated CNVs. A rare variant burden analysis using next-generation sequencing data from 637 BAV/TAA patients was performed for these two candidate genes. This revealed a suggestive genetic role for TBX20 in BAV/TAA aetiology, further reinforced by segregation of a rare TBX20 variant with the phenotype within a BAV/TAA family. To conclude, our results do not confirm a significant contribution for deleterious CNVs in BAV/TAA as only one potentially pathogenic CNV (1.05%) was identified. We cannot exclude the possibility that BAV/TAA is occasionally attributed to causal CNVs though, or that certain CNVs act as genetic risk factors by creating a sensitised background for BAV/TAA. Finally, accumulative evidence for TBX20 involvement in BAV/TAA aetiology underlines the importance of this transcription factor in cardiovascular disease.

Published
2019
Full Text
View/download PDF

15. Mutation in a non-desmosomal gene is associated with poor outcome of endo-epicardial ventricular tachycardia ablation in patients with nonischaemic cardiomyopathy

Author

Milan Macek, Patricia Norambuena, Stanislav Kmoch, Lenka Piherová, Viktor Stranecky, A Krebsova, D Wichterle, J Kautzner, Petr Peichl, and Robert Cihak

Subjects
medicine.medical_specialty, Ventricular tachycardia ablation, business.industry, Internal medicine, Mutation (genetic algorithm), medicine, Cardiomyopathy, Cardiology, In patient, Cardiology and Cardiovascular Medicine, medicine.disease, business, Gene
Abstract

Background Nonischaemic cardiomyopathy (NICM) represents a heterogenic disorder with a variable arrhythmogenic substrate. Its location is often epicardial and catheter ablation in this location proved to be an effective therapeutic modality in NICM patients with recurrent ventricular tachycardias (VTs). Purpose To determine the impact of the type of genetic mutation on the long-term outcome of endo-epicardial ablation in patients with NICM. Methods We investigated 82 patients (age 47±15 years, 10 women) with NICM who underwent endo-epicardial ablation for frequent VTs. Of them, 59% had a history of failed endocardial ablation. Patients had a left ventricular ejection fraction of 44±14% and all were implanted with cardioverter-defibrillator. One hundred candidate genes were examined using the new generation sequencing technique. Results Mutation in genes coding desmosomal complex (genes: PKP2, DSC, DSP, and DSG) was found in 30% of patients (“desmosomal” group). In 23% of patients, other gene mutations (genes: LMNA/C, MYH7, DES, TTN, RYR2, TPM1, MYPN, FLNC, and SCN5A) were detected (“non-desmosomal” group). In 46% of subjects no pathogenic mutation could be identified (“none” group). During a mean follow up of 34±33 months, patients in the “non-desmosomal” group were at significantly higher risk of VT recurrence and death/heart transplant compared to patients in the “desmosomal” group (Figure 1). Conclusion Potentially pathogenic mutation can be detected in about half of patients with NICM undergoing endo-epicardial VT ablation. Most commonly, mutations can be found in genes coding desmosomal complex and the endo-epicardial ablation is then associated with a satisfactory low VT recurrence rate and excellent survival in the long-term. On the other hand, patients with a mutation in non-desmosomal genes have poor outcomes despite endo-epicardial ablation. Funding Acknowledgement Type of funding sources: Public grant(s) – National budget only. Main funding source(s): Supported by Ministry of Health of the Czech Republic, grant nr. NV18-02-00237 Figure 1

Published
2021
Full Text
View/download PDF

18. Concealed cardiomyopathy as a frequent cause of idiopathic ventricular fibrillation in a representative Czech cohort of survivors of sudden cardiac arrest (SCA)

Author

Peter Kubuš, Milan Macek, V Zoubkova, Vlastimil Vančura, Petr Peichl, J Kautzner, M Segetova, Marek Sramko, T Tavacova, Jan Janoušek, J Haskova, Tomáš Roubíček, P Peldova, A Krebsova, and P Votypka

Subjects
medicine.medical_specialty, Scn5a gene, biology, business.industry, Cardiomyopathy, Cardiac arrhythmia, Sudden cardiac arrest, medicine.disease, Sudden cardiac death, Physiology (medical), Internal medicine, Cohort, medicine, Cardiology, biology.protein, KvLQT1, medicine.symptom, Idiopathic ventricular fibrillation, Cardiology and Cardiovascular Medicine, business
Abstract

Funding Acknowledgements Type of funding sources: Public grant(s) – National budget only. Main funding source(s): Ministry of Health of the Czech Republic Introduction The complex diagnostic work up in SCA survivors often does not yield a concrete cardiological diagnosis. Moreover, there is conflicting evidence whether genetic testing could support or guide clinical diagnostics. Purpose To assess the molecular architecture of idiopathic ventricular fibrillation in cases without apparent evidence of specific structural or arrhythmic cardiac disease at initial diagnostic work up in a representative Czech cohort. Patients and Methods Between 2013 - 2020 we have ascertained 100 SCA survivors (54 M / 46 F; age range at cardiac arrest 5-69 years). Genetic counselling was followed by massively parallel DNA sequencing using custom-made panels comprising 100 cardiac conditions-related genes. Subsequently, thorough cardiological screening examinations in first degree relatives were carried out. Presence of pathogenic variants was validated by Sanger DNA sequencing and through family segregation analyses. Results Highly likely or certain molecular aetiology (i.e. based on the presence of Class 4 or 5 variants) was disclosed in 20/100 (20%) in PKP2 (3x), SCN5A (4x), RYR2 (3x), TTN (2x), PLN, FLNC, PRKAG2, KCNH2, KCNQ1, SLC4A, TNNT2, and DSP. Interestingly, the KCNE1 p.Asp85Asn (LQT 5 lite) variant, was detected in further 3/100 cases, representing a recognized risk factor for ventricular arrhythmias. Conclusions Genetic testing facilitates stratification of the cause of arrhythmia in a substantial portion of SCA survivors. The utility of positive outcomes of genetic testing was substantiated in 10/20 gene positive patients, where the genetic stratification led to diagnosis of concealed arrhythmogenic cardiomyopathy, whose extent of morphological changes was under the diagnostic sensibility of imaging modalities or ECG. Our results enable individualized care in SCA survivors and assure targeted preventive approaches in their relatives.

Published
2021
Full Text
View/download PDF

19. Outcomes of post mortem genetic diagnosis in SCD victims and primary prevention of cardiac arrest in relatives: a nationwide multidisciplinary and multicentric collaboration in the Czechia

Author

Martin Dobiáš, J Kautzner, J Petrkova, Milan Macek, P Tomasek, P Votypka, A Pilin, Jan Janoušek, M Kulvajtova, T Tavacova, S Pohlova Kucerova, A Krebsova, K Rucklova, A Gregorova, and P Peldova

Subjects
medicine.medical_specialty, Epidemiology, business.industry, Genetic counseling, Hypertrophic cardiomyopathy, Autopsy, medicine.disease, Sudden cardiac death, Transforming growth factor beta receptor I, Multidisciplinary approach, Primary prevention, Emergency medicine, Medicine, Cardiology and Cardiovascular Medicine, business, Genetic diagnosis
Abstract

Funding Acknowledgements Type of funding sources: Public grant(s) – National budget only. Main funding source(s): Supported by Ministry of Health of the Czech Republic Introduction Post mortem genetic analysis in sudden cardiac death (SCD) represents an important diagnostic tool for the primary prevention of cardiac arrest in victim´s relatives. Purpose To assess the underlying molecular pathogenesis of SCD in a representative Czech cohort and to evaluate the effects of primary prevention of SCD in genetic relatives. Patients and Methods Between 2016 and 2020 we have ascertained 100 SCD cases (29 females/71 males; age range 0-52 years). According to autopsy protocols, cases with SCD were divided into categories of sudden arrhythmic death (SADS), sudden unexplained death (in infants; SUD/SUDI), thoracic aortic aneurysm/dissection and cardiomyopathy hypertrophic, arrhythmic, dilated (HCM, ACM, DCM) and sudden infant death syndrome (SIDS). DNA was isolated from post mortem biopsies / relatives blood and subjected to massively parallel sequencing (Illumina, USA) comprising custom-made candidate gene panel (100 genes). Genetic counselling and cardiological examinations were carried out in 245 family members. Results According to post mortem-established diagnosis, we identified 20 victims with SADS and SUD/SUDI, 11 with HCM and DCM, 19 with ACMG, 8 SIDS cases and 9 acute dissection cases. Most of victims died at sleep or at rest, while only 10/100 victims died during strenuous sport activities. About 50% of SCD victims did not report any apparent cardiac complaints. Highly likely or certain molecular etiology (i.e. based on presence of ACMG.net Class 4 to 5 variants) was disclosed in 19/100 (19%) in RYR2, KCNH2, SCN5A, FLNC (stop), TTN, RBM 20, LMNA/C, PRKAG2, MYBPC3, DSC2, FHL1, TGFBR1 and Col3A1 genes (see Tab). Finally, we identified 52/241 phenotype/genotype positive family members who are at risk of cardiac arrest and were offered corresponding cardiological care. Conclusion Multidisciplinary cooperation, together with centralized and standardized molecular genetic testing, enables the primary prevention of cardiac arrest in relatives of SCD victims. Results of post mortem genetic analysis Post mortem diagnosis Nr. Gender Age (years) Nr. of positive cases (DNA variant class IV or V) Gene Nr. examined relatives/phenotype or genotype positive cases SADS 20 8 females12 males 3-52 5/20 (25%) KCNH2 3x RYR2RANGFR 56/11 SUD/SUDI 20 5 females, 15 males 0-50 1/18 (5%, 2 non informative cases) RYR2 45/9 HCM 11 0 females11 males 14-52 3/11 (27%) MYBPC3FHL1PRKAG2 26/9 DCM 11 3 females8 males 8-48 4/11 (36%) TTN (3x)RBM 20FLNC (stop) 24/7 ACM 19 9 females10 males 17 - 49 4/19 (21%) SCN5AFLNC (stop)DSC2LMNA/C 58/9 SIDS 8 3 females5 males < 1 0/8 - 12/0 Acute dissection 9 1 female8 males 16-49 2/9 (22%) TGFBR1Col3A1 24/7

Published
2021
Full Text
View/download PDF

20. Novel LOX Variants in Five Families with Aortic/Arterial Aneurysm and Dissection with Variable Connective Tissue Findings

Author

Van Gucht, Ilse, primary, Krebsova, Alice, additional, Diness, Birgitte Rode, additional, Laga, Steven, additional, Adlam, Dave, additional, Kempers, Marlies, additional, Samani, Nilesh J., additional, Webb, Tom R., additional, Baranowska, Ania A., additional, Van Den Heuvel, Lotte, additional, Perik, Melanie, additional, Luyckx, Ilse, additional, Peeters, Nils, additional, Votypka, Pavel, additional, Macek, Milan, additional, Meester, Josephina, additional, Van Laer, Lut, additional, Verstraeten, Aline, additional, and Loeys, Bart L., additional

Published
2021
Full Text
View/download PDF

22. Novel lox variants in five families with aortic/arterial aneurysm and dissection with variable connective tissue findings

Author

Van Gucht, Ilse, Krebsova, Alice, Diness, Birgitte Rode, Laga, Steven, Adlam, Dave, Kempers, Marlies, Samani, Nilesh J., Webb, Tom R., Baranowska, Ania A., Van Den Heuvel, Lotte, Perik, Melanie, Luyckx, Ilse, Peeters, Nils, Votypka, Pavel, Macek, Milan, Meester, Josephina, Van Laer, Lut, Verstraeten, Aline, Loeys, Bart L., Van Gucht, Ilse, Krebsova, Alice, Diness, Birgitte Rode, Laga, Steven, Adlam, Dave, Kempers, Marlies, Samani, Nilesh J., Webb, Tom R., Baranowska, Ania A., Van Den Heuvel, Lotte, Perik, Melanie, Luyckx, Ilse, Peeters, Nils, Votypka, Pavel, Macek, Milan, Meester, Josephina, Van Laer, Lut, Verstraeten, Aline, and Loeys, Bart L.

Abstract

Thoracic aortic aneurysm and dissection (TAAD) is a major cause of cardiovascular morbidity and mortality. Loss-of-function variants in LOX, encoding the extracellular matrix crosslinking enzyme lysyl oxidase, have been reported to cause familial TAAD. Using a next-generation TAAD gene panel, we identified five additional probands carrying LOX variants, including two missense variants affecting highly conserved amino acids in the LOX catalytic domain and three truncating variants. Connective tissue manifestations are apparent in a substantial fraction of the variant carriers. Some LOX variant carriers presented with TAAD early in life, while others had normal aortic diam-eters at an advanced age. Finally, we identified the first patient with spontaneous coronary artery dissection carrying a LOX variant. In conclusion, our data demonstrate that loss-of-function LOX variants cause a spectrum of aortic and arterial aneurysmal disease, often combined with connective tissue findings.

Published
2021

23. Concealed cardiomyopathy as a frequent cause of idiopathic ventricular fibrillation in a representative Czech cohort of survivors of sudden cardiac arrest (SCA)

Author

Krebsova, A, primary, Votypka, P, additional, Peldova, P, additional, Haskova, J, additional, Tavacova, T, additional, Peichl, P, additional, Segetova, M, additional, Roubicek, T, additional, Vancura, V, additional, Kubus, P, additional, Sramko, M, additional, Macek Jr, M, additional, Zoubkova, V, additional, Janousek, J, additional, and Kautzner, J, additional

Published
2021
Full Text
View/download PDF

24. Outcomes of post mortem genetic diagnosis in SCD victims and primary prevention of cardiac arrest in relatives: a nationwide multidisciplinary and multicentric collaboration in the Czechia

Author

Krebsova, A, primary, Votypka, P, additional, Peldova, P, additional, Rucklova, K, additional, Kulvajtova, M, additional, Pohlova -Kucerova, S, additional, Pilin, A, additional, Gregorova, A, additional, Tavacova, T, additional, Petrkova, J, additional, Dobias, M, additional, Tomasek, P, additional, Macek Jr, M, additional, Janousek, J, additional, and Kautzner, J, additional

Published
2021
Full Text
View/download PDF

25. Comparison of variant detection rate in genes between two cohorts of Czech living patients versus victims of sudden cardiac death with clinical / post mortem diagnosis of non-ischemic cardiomyopathy

Author

A Krebsova, K Rucklova, Milos Kubanek, S Pohlova Kucerova, P Tomasek, Jan Janoušek, T Tavacova, Milan Macek, P Votypka, J Kautzner, M Kulvajtova, Martin Dobiáš, J Petrkova, A Pilin, and E Borisincova

Subjects
Czech, medicine.medical_specialty, business.industry, Non ischemic cardiomyopathy, medicine.disease, language.human_language, Sudden cardiac death, Internal medicine, language, Cardiology, Medicine, cardiovascular diseases, Detection rate, Cardiology and Cardiovascular Medicine, business
Abstract

Introduction Hereditary cardiomyopathy is associated with an increased risk of ventricular arrhythmia and sudden cardiac death (SCD). Genetic stratification substantiates risk assessment and enables the primary prevention of SCD in relatives at risk. We have analyzed the genetic aetiology of SCD in a representative Czech cohort with post mortem diagnosis of various forms of cardiomyopathy and compared it to living cases with these cardiac disorders. Patients and methods Between 2018 and 2019, altogether 47 victims of SCD with post mortem diagnosis of hypertrophic- (HCM; 18/47), arrhythmogenic- (ACM; 19/47) and dilated cardiomyopathy (DCM; 10/47) were identified. Concurrently, genetic testing was performed in 114 living patients (HCM 54/114, ACM 22/114, DCM 38/114). Genetic counselling and cardiologic examination had been carried out in first-degree relatives in all patients/SCD victims. Massively parallel sequencing (MiSeq platform; Illumina.com) was utilized for a custom-made panel comprising 100 candidate genes (Sophia Genetics, Switzerland). The presence of pathogenic variants was validated by Sanger DNA sequencing and through family segregation analyses. Results The causative detection rate (according to ACMG.net classes 4 or 5) in SCD victims with DCM was 60% (6/10) and in living patients with DCM 47.4% (18/38). Variants in TTN, RBM20, DES and FLNC (mainly truncating variants) prevailed in both groups. The detection rate in ACM was 5% (1/19 in SCN5A gene) in SCD victims and 31.8% (7/22) in living patients. Interestingly, the most prevalent mutated gene PKP2 in living patients was not detected in SCD victims. The detection rate in SCD victims with post mortem diagnosis of HCM was 16% (3/18) and in living patients 35% (19/54). The most prevalent gene was MYBPC3 in both groups, while PRKAG2 was detected in one SCD victim and in one living case who survived cardiac arrest. Conclusion Post-mortem genetic analysis in DCM yields a high detection rate and allows potentially effective primary prevention of SCD in relatives at risk. In contrast, the molecular autopsy of HCM and ACM renders a much lower yield which is below the mutation detection rate in living phenotype positive individuals. The results help to improve the genetic counselling in affected families in Czech Republic. Funding Acknowledgement Type of funding source: Public grant(s) – National budget only. Main funding source(s): Ministry of Health of the Czech Republic

Published
2020
Full Text
View/download PDF

26. P1107First results of molecular autopsy examinations in sudden cardiac death drawn from nationwide multidisciplinary and multicentric collaboration in the Czech Republic

Author

A Krebsova, P Votypka, P Peldova, K Rucklova, A Pilin, M Kulvajtova, S Pohlova -Kucerova, A Blankova, T Tavacova, J Petrkova, P Tomasek, M Macek Sr, M Macek Jr, J Janousek, and J Kautzner

Subjects
Czech, medicine.medical_specialty, business.industry, General surgery, Autopsy, medicine.disease, language.human_language, Sudden cardiac death, Multidisciplinary approach, Physiology (medical), Primary prevention, language, Molecular autopsy, Medicine, Cardiology and Cardiovascular Medicine, business, Sudden infant death
Abstract

Funding Acknowledgements Supported by Ministry of Health of the Czech Republic, grant nr. NV18-02-00237. All rights reserved." Introduction "Molecular autopsy" in sudden cardiac death (SCD) is an important diagnostic tool for primary prevention of cardiac arrest in victim´s relatives and requires multicentric and multidisciplinary collaboration. Purpose To establish a national network for SCD diagnostics, to assess the acceptance of genetic testing in at risk relatives and to elucidate the genetic etiology of SCD in a representative Czech cohort aged below 45 years. Patients and Methods Between 2016 and 2019 we ascertained 70 SCD (50 M / 20 F), with positive family history for cardiac arrest in 8/70 cases. Only one family did not agree with molecular autopsy. Genetic counselling and cardiological screening examination was carried out in first degree relatives of SCD survivors accompanied by custom-made targeted panel massively parallel DNA sequencing comprising 100 cardiac conditions-related genes. Presence of pathogenic variants was validated by Sanger DNA sequencing and through family segregation analyses. Results According to post-mortem diagnosis most victims died of HCM (17/70), ACM (16/70), no structural heart disease was found in 15/70 cases, DCM/LVNC in 9/70, 6/70 were SIDS cases, other rare diagnoses comprised aortic dissection, or myocarditis. Most of victims died at sleep, only 9/70 victims died during strenuous activities. About 50% of SCD victims did not have cardiac complaints before death. Very likely or certain molecular etiology (i.e. based on presence of ACMG.net Class 4 to 5 variants) was disclosed in 12/70 (17%) in RYR2, FLNC, TTN, KCNH2 and KCNQ1 genes, whilst potentially causative DNA variants (Classes 3-4) were observed in 13/70 (18%) cases. In SIDS we did not find any pathogenic variants. Interestingly, the KCNE1 p.Asp85Asn (LQT 5 lite) variant, was detected in 3/70 cases as a recognized risk factor for ventricular arrhythmias. Conclusion The multidisciplinary cooperation in Czech Republic has been established, family survivors are willing to receive genetic and cardiological care, while centralised molecular genetic analysis enables reliable results which are in accordance with other multicentric studies. The molecular autopsy should, especially in SIDS, be expanded to whole exome sequencing.

Published
2020
Full Text
View/download PDF

28. Association of human aging with a functional variant of lotho

Author

Arking, Dan E., Krebsova, Alice, Macek, Milan, Sr., Macek, Milan, Jr., Arking, Albert, Mian, I. Saira, Fried, Linda, Hamosh, Ada, Dey, Srabani, McIntosh, Iain, and Dietz, Harry C.

Subjects
Aging -- Genetic aspects, Gene expression -- Physiological aspects, Amino acids -- Physiological aspects, Nucleotides -- Analysis, Phenotype -- Genetic aspects, Genetic research -- Analysis, Science and technology
Abstract

Mice deficient in Klotho gene expression exhibit a syndrome resembling premature human aging. To determine whether variation in the human KLOTHO locus contributes to survival, we applied two newly characterized polymorphic microsatellite markers flanking the gene in a population-based association study. In a cohort chosen for its homogeneity, Bohemian Czechs, we demonstrated significant differences in selected marker allele frequencies between newborn and elderly individuals (P < 0.05). These results precipitated a search for functional variants of klotho. We identified an allele, termed KL-VS, containing six sequence variants in complete linkage disequilibrium, two of which result in amino acid substitutions F352V and C370S. Homozygous elderly individuals were underrepresented in three distinct populations: Bohemian Czechs, Baltimore Caucasians, and Baltimore African-Americans [combined odds ratio (OR) = 2.59, P < 0.0023]. In a transient transfection assay, secreted levels of klotho harboring V352 are reduced 6-fold, whereas extracellular levels of the S370 form are increased 2.9-fold. The V352/S370 double mutant exhibits an intermediate phenotype (1.6-fold increase), providing a rare example of intragenic complementation in cis by human single nucleotide polymorphisms. The remarkable conservation of F352 among homologous proteins suggests that it is functionally important. The corresponding substitution, F289V, in the closest human klotho paralog with a known substrate, cBGL1, completely eliminates its ability to cleave p-nitrophenyl-[beta]-D-glucoside. These results suggest that the KL-VS allele influences the trafficking and catalytic activity of klotho, and that variation in klotho function contributes to heterogeneity in the onset and severity of human age-related phenotypes.

Published
2002

29. Comparison of variant detection rate in genes between two cohorts of Czech living patients versus victims of sudden cardiac death with clinical / post mortem diagnosis of non-ischemic cardiomyopathy

Author

Borisincova, E, primary, Votypka, P, additional, Rucklova, K, additional, Pilin, A, additional, Kulvajtova, M, additional, Pohlova Kucerova, S, additional, Tavacova, T, additional, Kubanek, M, additional, Petrkova, J, additional, Dobias, M, additional, Tomasek, P, additional, Macek Jr, M, additional, Janousek, J, additional, Krebsova, A, additional, and Kautzner, J, additional

Published
2020
Full Text
View/download PDF

30. Danon disease is an underdiagnosed cause of advanced heart failure in young female patients: a LAMP2 flow cytometric study

Author

Gurka, Jiri, primary, Piherova, Lenka, additional, Majer, Filip, additional, Chaloupka, Anna, additional, Zakova, Daniela, additional, Pelak, Ondrej, additional, Krebsova, Alice, additional, Peichl, Petr, additional, Krejci, Jan, additional, Freiberger, Tomas, additional, Melenovsky, Vojtech, additional, Kautzner, Josef, additional, Kalina, Tomas, additional, Sikora, Jakub, additional, and Kubanek, Milos, additional

Published
2020
Full Text
View/download PDF

31. Pigmentary retinopathy can indicate the presence of pathogenic LAMP2 variants even in somatic mosaic carriers with no additional signs of Danon disease

Author

Kousal, Bohdan, primary, Majer, Filip, additional, Vlaskova, Hana, additional, Dvorakova, Lenka, additional, Piherova, Lenka, additional, Meliska, Martin, additional, Langrova, Hana, additional, Palecek, Tomas, additional, Kubanek, Milos, additional, Krebsova, Alice, additional, Gurka, Jiri, additional, Stara, Veronika, additional, Michaelides, Michel, additional, Kalina, Tomas, additional, Sikora, Jakub, additional, and Liskova, Petra, additional

Published
2020
Full Text
View/download PDF

32. P1107First results of molecular autopsy examinations in sudden cardiac death drawn from nationwide multidisciplinary and multicentric collaboration in the Czech Republic

Author

Krebsova, A, primary, Votypka, P, additional, Peldova, P, additional, Rucklova, K, additional, Pilin, A, additional, Kulvajtova, M, additional, Pohlova -Kucerova, S, additional, Blankova, A, additional, Tavacova, T, additional, Petrkova, J, additional, Tomasek, P, additional, Macek Sr, M, additional, Macek Jr, M, additional, Janousek, J, additional, and Kautzner, J, additional

Published
2020
Full Text
View/download PDF

33. 5162Novel insights into desminopathy in the era of next generation sequencing

Author

A Krebsova, Milos Kubanek, T Schimerova, Milan Macek, Josef Zamecnik, Josef Houstek, Lenka Piherová, Viktor Stranecky, Stanislav Kmoch, Vojtech Melenovsky, Josef Kautzner, P Ridzon, Jiří Zeman, Tomáš Paleček, and Hana Hansikova

Subjects
business.industry, Medicine, Computational biology, Cardiology and Cardiovascular Medicine, business, DNA sequencing
Abstract

Aims The pleomorphic clinical presentation makes the diagnosis of desminopathy difficult. This disease of intermediate filaments causes not only a contractile dysfunction in cardiomyopathy and skeletal myopathy, but also a secondary mitochondrial dysfunction. We aimed to describe prevalence, phenotypic expression and mitochondrial function in desmin mutation carriers identified in a large cohort of patients with unexplained cardiomyopathy. Methods and results A representative cohort of 327 Czech patients with unexplained cardiomyopathy underwent whole exome sequencing. The cohort consisted of cases with familial and sporadic dilated cardiomyopathy (81%), left ventricular noncompaction cardiomyopathy (LVNC) (13%), and less frequently of restrictive (3%) or arrhythmogenic cardiomyopathy (3%). Clinical and laboratory data of desmin mutation carriers were collected. Morphology, desmin expression and mitochondrial function were studied in available myocardial and skeletal muscle specimens. Rare, conserved and possibly pathogenic desmin variants were identified in 6 (1.8%) probands. Two desmin mutations previously classified as variants of uncertain significance (p.K43E, p.S57L), one novel desmin variant (p.A210D) and two known pathogenic desmin mutations (p.R406W, p.R454W) were in affected individuals associated with characteristic pathological desmin aggregates in myocardial and/or skeletal biopsy samples. The individual with the novel desmin variant p.Q364H had decreased myocardial expression of desmin with absent desmin aggregates in myocardial/skeletal biopsy and presented with familial left ventricular non-compaction cardiomyopathy, a novel phenotype of desminopathy. Assessment of mitochondrial function in four carriers of desmin mutations with fresh-frozen skeletal and/or myocardial muscle specimens confirmed decreased metabolic capacity of mitochondrial respiratory chain complexes, which was in case of myocardial succinate respiration more profound than in end-stage heart failure of other etiologies. Genetic testing corrected an inappropriate clinical diagnosis in two probands previously diagnosed with mitochondrial disease and inflammatory cardiomyopathy. During a median follow-up of 56 months, 5 (83%) probands developed end-stage heart failure. Conclusions Desminopathy is a rare cause of cardiomyopathy and/or skeletal muscle myopathy with a pleomorphic clinical presentation and poor prognosis. The presence of desminopathy should be considered also in individuals with left ventricular non-compaction cardiomyopathy, and in the differential diagnosis of mitochondrial diseases and inflammatory cardiomyopathy. Acknowledgement/Funding Research grant of the Ministry of Health, Czech Republic [MZ 15-27682A], No. 00023001 (IKEM, Prague, CZ), the Czech Science Foundation [14-36804G].

Published
2019
Full Text
View/download PDF

34. P5610Inflammatory response after ExoVasc personalized external aortic root support (PEARS) procedure in patients with Marfan syndrome or non-Marfan genetic aortopathy

Author

Marek Laboš, Radka Kockova, J Maly, Jan Pirk, and A Krebsova

Subjects
Marfan syndrome, medicine.medical_specialty, business.industry, Inflammatory response, Aortic root, medicine.disease, Chest pain, Aortic disease, Hospital records, Internal medicine, medicine, Cardiology, In patient, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Fibrillin
Abstract

Background External aortic root support (PEARS) is a novel prophylactic aortic root surgery. Purpose The study aimed to determine the severity of inflammatory response after the personalized external aortic root support (PEARS) procedure in comparison to after the standard prophylactic aortic root surgery (SPARS). Materials and methods The study was a single-centre, retrospective, based on hospital record analysis of patients who underwent the PEARS procedure (PEARS group) or SPARS (SPARS group) during 1998–2017. C-reactive protein (CRP), white blood count (WBC), and echocardiography were routinely obtained. Fever was defined as body temperature ≥38°C. Diagnosis of pericarditis included a minimum of three signs from chest pain, pericardial effusion, ST elevation, elevated CRP, and body temperature. Results PEARS and SPARS groups consisted of 13 and 14 patients, respectively, scheduled for prophylactic aortic root surgery. A majority of patients in both groups had Marfan syndrome with causal mutation in the fibrillin 1 (FBN1) gene (62% vs 79%). Patient baseline characteristics were similar in the two groups, except aortic root was significantly larger in the SPARS group than in the PEARS group (60±12 mm vs 48±5 mm; P=0.003). All surgical procedures were successful and without major complications. The peak values of CRP and WBC were significantly higher in the PEARS group (264.5±84.4 mg/L vs 184.6±89.6 mg/L; P=0.034 and 15.2±3.8 109/L vs 11.9±3.3 109/L; P=0.029). Early and recurrent fever requiring hospital readmission was significantly more frequent in the PEARS group (77% vs 36%; P=0.032 and 46% vs 7%; P=0.020). Early and recurrent pericarditis requiring hospital readmission was also more frequent in the PEARS group (31% vs 0%; P=0.024 and 31% vs 0%; P=0.024). Inflammatory characteristics Postprocedural inflammatory characteristics PEARS group SPARS group P value (N=13) (N=14) Peak level of CRP (mg/L) 264.5±84.4 184.6±89.6 0.034 Peak WBC (109/L) 15.2±3.8 11.9±3.3 0.029 ST elevation (N) 11 (85) 6 (43) 0.024 Early fever (N) 10 (77) 5 (36) 0.032 Recurrent fever (N) 6 (46) 1 (7) 0.020 Early pericarditis (N) 4 (31) 0 (0) 0.024 Recurrent pericarditis (N) 4 (31) 0 (0) 0.024 CRP, C-reactive protein; WBC, white blood count. Echocardiography-signs of inflammation Conclusions The PEARS procedure is an extremely promising surgical technique, but the postoperative inflammatory response occurs frequently and more severely in comparison to SPARS. Clearly, these findings warrant further investigation.

Published
2019
Full Text
View/download PDF

35. Alu-mediated Xq24 deletion encompassing CUL4B, LAMP2, ATP1B4, TMEM255A, and ZBTB33 genes causes Danon disease in a female patient

Author

Filip, Majer, Bohdan, Kousal, Petr, Dusek, Lenka, Piherova, Martin, Reboun, Romana, Mihalova, Jiri, Gurka, Alice, Krebsova, Hana, Vlaskova, Lenka, Dvorakova, Jana, Krihova, Petra, Liskova, Stanislav, Kmoch, Tomas, Kalina, Milos, Kubanek, and Jakub, Sikora

Subjects
Adult, Male, DNA Copy Number Variations, Myocardium, Exons, Cullin Proteins, Glycogen Storage Disease Type IIb, Alu Elements, Loss of Function Mutation, X Chromosome Inactivation, Lysosomal-Associated Membrane Protein 2, Mental Retardation, X-Linked, Humans, Female, Chromosome Deletion, Sodium-Potassium-Exchanging ATPase, Cardiomyopathies, Transcription Factors
Abstract

Cullin 4B (CUL4B), lysosomal-associated membrane protein Type 2 (LAMP2), ATP1B4, TMEM255A, and ZBTB33 are neighboring genes on Xq24. Mutations in CUL4B result in Cabezas syndrome (CS). Male CS patients present with dysmorphic, neuropsychiatric, genitourinary, and endocrine abnormalities. Heterozygous CS females are clinically asymptomatic. LAMP2 mutations cause Danon disease (DD). Cardiomyopathy is a dominant feature of DD present in both males and heterozygous females. No monogenic phenotypes have been associated with mutations in ATP1B4, TMEM255A, and ZBTB33 genes. To facilitate diagnostics and counseling in CS and DD families, we present a female DD patient with a de novo Alu-mediated Xq24 rearrangement causing a deletion encompassing CUL4B, LAMP2, and also the other three neighboring genes. Typical to females heterozygous for CUL4B mutations, the patient was CS asymptomatic, however, presented with extremely skewed X-chromosome inactivation (XCI) ratios in peripheral white blood cells. As a result of the likely selection against CUL4B deficient clones, only minimal populations (~3%) of LAMP2 deficient leukocytes were identified by flow cytometry. On the contrary, myocardial LAMP2 protein expression suggested random XCI. We demonstrate that contiguous CUL4B and LAMP2 loss-of-function copy number variations occur and speculate that male patients carrying similar defects could present with features of both CS and DD.

Published
2019

36. Genotype/phenotype correlation in autosomal recessive lamellar ichthyosis

Author

Hennies, Hans Christian, Kuster, Wolfgang, Wiebe, Victor, Krebsova, Alice, and Reis, Andre

Subjects
Ichthyosis -- Genetic aspects, Keratinization -- Genetic aspects, Biological sciences
Abstract

Correlation between genotype and phenotype has been examined in 14 families with autosomal recessive lamellar ichthyosis. The results show no consistent correlation between genetic and clinical classifications, suggesting that existing clinical criteria do not discriminate between the different molecular forms of the disease. Three loci have been associated with lamellar ichthyosis. In families with mutations on the TGM1 gene, seven different missense mutations and one splice mutation have been found.

Published
1998

38. Copy number variation analysis in bicuspid aortic valve-related aortopathy identifies TBX20 as a contributing gene

Author

Luyckx, I., Kumar, A.A., Reyniers, Edwin, Dekeyser, Emily, Vanderstraeten, Kathleen, Vandeweyer, G., Kempers, M.J.E., Duijnhouwer, A.L., Loeys, B.L., Nemcikova, M., Krebsova, A., Luyckx, I., Kumar, A.A., Reyniers, Edwin, Dekeyser, Emily, Vanderstraeten, Kathleen, Vandeweyer, G., Kempers, M.J.E., Duijnhouwer, A.L., Loeys, B.L., Nemcikova, M., and Krebsova, A.

Abstract

Item does not contain fulltext

Published
2019

40. P1817Non-truncating Filamin C variants represent disease-causing mutations in dilated cardiomyopathy

Author

Jakub Sikora, Tomas Palecek, Stanislav Kmoch, Jan Krejčí, Vojtech Melenovsky, A Krebsova, Anna Chaloupka, Lenka Piherová, Josef Kautzner, T Nedvedova, Milos Kubanek, and I Grochova

Subjects
Pathology, medicine.medical_specialty, business.industry, Medicine, Dilated cardiomyopathy, Disease, Cardiology and Cardiovascular Medicine, business, Filamin, medicine.disease
Published
2018
Full Text
View/download PDF

41. Alu ‐mediated Xq24 deletion encompassing CUL4B , LAMP2 , ATP1B4 , TMEM255A , and ZBTB33 genes causes Danon disease in a female patient

Author

Majer, Filip, primary, Kousal, Bohdan, additional, Dusek, Petr, additional, Piherova, Lenka, additional, Reboun, Martin, additional, Mihalova, Romana, additional, Gurka, Jiri, additional, Krebsova, Alice, additional, Vlaskova, Hana, additional, Dvorakova, Lenka, additional, Krihova, Jana, additional, Liskova, Petra, additional, Kmoch, Stanislav, additional, Kalina, Tomas, additional, Kubanek, Milos, additional, and Sikora, Jakub, additional

Published
2019
Full Text
View/download PDF

43. 5162Novel insights into desminopathy in the era of next generation sequencing

Author

Kubanek, M, primary, Schimerova, T, additional, Piherova, L, additional, Krebsova, A, additional, Hansikova, H, additional, Zeman, J, additional, Palecek, T, additional, Houstek, J, additional, Zamecnik, J, additional, Macek Jr, M, additional, Ridzon, P, additional, Stranecky, V, additional, Kmoch, S, additional, Melenovsky, V, additional, and Kautzner, J, additional

Published
2019
Full Text
View/download PDF

45. Pigmentary retinopathy can indicate the presence of pathogenic LAMP2 variants even in somatic mosaic carriers with no additional signs of Danon disease.

Author

Kousal, Bohdan, Majer, Filip, Vlaskova, Hana, Dvorakova, Lenka, Piherova, Lenka, Meliska, Martin, Langrova, Hana, Palecek, Tomas, Kubanek, Milos, Krebsova, Alice, Gurka, Jiri, Stara, Veronika, Michaelides, Michel, Kalina, Tomas, Sikora, Jakub, and Liskova, Petra

Subjects
OPTICAL coherence tomography, RHODOPSIN, BIOFLUORESCENCE, RETINAL degeneration, VISUAL fields, PROLIFERATIVE vitreoretinopathy
Abstract

Purpose: Danon disease (DD) is a rare X‐linked disorder caused by pathogenic variants in LAMP2. DD primarily manifests as a severe cardiomyopathy. An early diagnosis is crucial for patient survival. The aim of the study was to determine the usefulness of ocular examination for identification of DD. Methods: Detailed ocular examination in 10 patients with DD (3 males, 7 females) and a 45‐year‐old asymptomatic female somatic mosaic carrier of a LAMP2 disease‐causing variant. Results: All patients with manifest cardiomyopathy had pigmentary retinopathy with altered autofluorescence and diffuse visual field loss. Best corrected visual acuity (BCVA) was decreased (<0.63) in 8 (40%) out of 20 eyes. The severity of retinal pathology increased with age, resulting in marked cone‐rod involvement overtime. Spectral‐domain optical coherence tomography in younger patients revealed focal loss of photoreceptors, disruption and deposition at the retinal pigment epithelium/Bruch's membrane layer (corresponding to areas of marked increased autofluorescence), and hyperreflective foci in the outer nuclear layer. Cystoid macular oedema was seen in one eye. In the asymptomatic female with somatic mosaicism, the BCVA was 1.0 bilaterally. An abnormal autofluorescence pattern in the left eye was present; while full‐field electroretinography was normal. Conclusions: Detailed ocular examination may represent a sensitive and quick screening tool for the identification of carriers of LAMP2 pathogenic variants, even in somatic mosaicism. Hence, further investigation should be undertaken in all patients with pigmentary retinal dystrophy as it may be a sign of a life‐threatening disease. [ABSTRACT FROM AUTHOR]

Published
2021
Full Text
View/download PDF

46. 3946Comparison of genetic signature of isolated left ventricular non-compaction cardiomyopathy and familial dilated cardiomyopathy as assessed by whole exome sequencing

Author

A Krebsova, Milan Macek, Lenka Piherová, Stanislav Kmoch, Milos Kubanek, Filip Málek, Viktor Stranecky, R. Kockova, Josef Kautzner, Vojtech Melenovsky, and Tomas Palecek

Subjects
Genetic signature, medicine.medical_specialty, business.industry, Internal medicine, Familial dilated cardiomyopathy, Cardiology, Medicine, Left Ventricular Non-Compaction Cardiomyopathy, Cardiology and Cardiovascular Medicine, business, Exome sequencing
Published
2017
Full Text
View/download PDF

49. Alu‐mediated Xq24 deletion encompassing CUL4B, LAMP2, ATP1B4, TMEM255A, and ZBTB33 genes causes Danon disease in a female patient.

Author

Majer, Filip, Kousal, Bohdan, Dusek, Petr, Piherova, Lenka, Reboun, Martin, Mihalova, Romana, Gurka, Jiri, Krebsova, Alice, Vlaskova, Hana, Dvorakova, Lenka, Krihova, Jana, Liskova, Petra, Kmoch, Stanislav, Kalina, Tomas, Kubanek, Milos, and Sikora, Jakub

Abstract

Cullin 4B (CUL4B), lysosomal‐associated membrane protein Type 2 (LAMP2), ATP1B4, TMEM255A, and ZBTB33 are neighboring genes on Xq24. Mutations in CUL4B result in Cabezas syndrome (CS). Male CS patients present with dysmorphic, neuropsychiatric, genitourinary, and endocrine abnormalities. Heterozygous CS females are clinically asymptomatic. LAMP2 mutations cause Danon disease (DD). Cardiomyopathy is a dominant feature of DD present in both males and heterozygous females. No monogenic phenotypes have been associated with mutations in ATP1B4, TMEM255A, and ZBTB33 genes. To facilitate diagnostics and counseling in CS and DD families, we present a female DD patient with a de novo Alu‐mediated Xq24 rearrangement causing a deletion encompassing CUL4B, LAMP2, and also the other three neighboring genes. Typical to females heterozygous for CUL4B mutations, the patient was CS asymptomatic, however, presented with extremely skewed X‐chromosome inactivation (XCI) ratios in peripheral white blood cells. As a result of the likely selection against CUL4B deficient clones, only minimal populations (~3%) of LAMP2 deficient leukocytes were identified by flow cytometry. On the contrary, myocardial LAMP2 protein expression suggested random XCI. We demonstrate that contiguous CUL4B and LAMP2 loss‐of‐function copy number variations occur and speculate that male patients carrying similar defects could present with features of both CS and DD. [ABSTRACT FROM AUTHOR]

Published
2020
Full Text
View/download PDF

50. LAMP2 exon-copy number variations in Danon disease heterozygote female probands: Infrequent or underdetected?

Author

Majer, Filip, primary, Piherova, Lenka, additional, Reboun, Martin, additional, Stara, Veronika, additional, Pelak, Ondrej, additional, Norambuena, Patricia, additional, Stranecky, Viktor, additional, Krebsova, Alice, additional, Vlaskova, Hana, additional, Dvorakova, Lenka, additional, Kmoch, Stanislav, additional, Kalina, Tomas, additional, Kubanek, Milos, additional, and Sikora, Jakub, additional

Published
2018
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results