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1. Novel Association of the NOTCH Pathway Regulator MIB1 Gene With the Development of Bicuspid Aortic Valve.

Author

Tessler, I., Albuisson, J., Piñeiro-Sabarís, R., Verstraeten, A., Kamber Kaya, H.E., Siguero-Álvarez, M., Goudot, G., MacGrogan, D., Luyckx, I., Shpitzen, S., Levin, G., Kelman, G., Reshef, N., Mananet, H., Holdcraft, J., Muehlschlegel, J.D., Peloso, G.M., Oppenheim, O., Cheng, C., Mazzella, J.M., Andelfinger, G., Mital, S., Eriksson, P., Billon, C., Heydarpour, M., Dietz, H.C., Jeunemaitre, X., Leitersdorf, E., Sprinzak, D., Blacklow, S.C., Body, S.C., Carmi, S., Loeys, B.L., Pompa, J.L. de la, Gilon, D., Messas, E., Durst, R., Tessler, I., Albuisson, J., Piñeiro-Sabarís, R., Verstraeten, A., Kamber Kaya, H.E., Siguero-Álvarez, M., Goudot, G., MacGrogan, D., Luyckx, I., Shpitzen, S., Levin, G., Kelman, G., Reshef, N., Mananet, H., Holdcraft, J., Muehlschlegel, J.D., Peloso, G.M., Oppenheim, O., Cheng, C., Mazzella, J.M., Andelfinger, G., Mital, S., Eriksson, P., Billon, C., Heydarpour, M., Dietz, H.C., Jeunemaitre, X., Leitersdorf, E., Sprinzak, D., Blacklow, S.C., Body, S.C., Carmi, S., Loeys, B.L., Pompa, J.L. de la, Gilon, D., Messas, E., and Durst, R.

Abstract

Contains fulltext : 295944.pdf (Publisher’s version ) (Closed access), IMPORTANCE: Nonsyndromic bicuspid aortic valve (nsBAV) is the most common congenital heart valve malformation. BAV has a heritable component, yet only a few causative genes have been identified; understanding BAV genetics is a key point in developing personalized medicine. OBJECTIVE: To identify a new gene for nsBAV. DESIGN, SETTING, AND PARTICIPANTS: This was a comprehensive, multicenter, genetic association study based on candidate gene prioritization in a familial cohort followed by rare and common association studies in replication cohorts. Further validation was done using in vivo mice models. Study data were analyzed from October 2019 to October 2022. Three cohorts of patients with BAV were included in the study: (1) the discovery cohort was a large cohort of inherited cases from 29 pedigrees of French and Israeli origin; (2) the replication cohort 1 for rare variants included unrelated sporadic cases from various European ancestries; and (3) replication cohort 2 was a second validation cohort for common variants in unrelated sporadic cases from Europe and the US. MAIN OUTCOMES AND MEASURES: To identify a candidate gene for nsBAV through analysis of familial cases exome sequencing and gene prioritization tools. Replication cohort 1 was searched for rare and predicted deleterious variants and genetic association. Replication cohort 2 was used to investigate the association of common variants with BAV. RESULTS: A total of 938 patients with BAV were included in this study: 69 (7.4%) in the discovery cohort, 417 (44.5%) in replication cohort 1, and 452 (48.2%) in replication cohort 2. A novel human nsBAV gene, MINDBOMB1 homologue MIB1, was identified. MINDBOMB1 homologue (MIB1) is an E3-ubiquitin ligase essential for NOTCH-signal activation during heart development. In approximately 2% of nsBAV index cases from the discovery and replication 1 cohorts, rare MIB1 variants were detected, predicted to be damaging, and were significantly enriched compared with populati

Published
2023

2. N-acetylneuraminate pyruvate lyase controls sialylation of muscle glycoproteins essential for muscle regeneration and function.

Author

Da Silva, Afitz, Dort, J., Orfi, Z., Pan, X., Huang, S.J., Kho, I., Heckel, E., Muscarnera, G., Vliet, P.P. van, Sturiale, L., Messina, A., Romeo, D.A., Karnebeek, C.D.M. van, Wen, X.Y., Hinek, A., Molina, T., Andelfinger, G., Ellezam, B., Yamanaka, Y., Olivos, H.J., Morales, C.R., Joyal, J.S., Lefeber, D.J., Garozzo, D., Dumont, N.A., Pshezhetsky, A.V., Da Silva, Afitz, Dort, J., Orfi, Z., Pan, X., Huang, S.J., Kho, I., Heckel, E., Muscarnera, G., Vliet, P.P. van, Sturiale, L., Messina, A., Romeo, D.A., Karnebeek, C.D.M. van, Wen, X.Y., Hinek, A., Molina, T., Andelfinger, G., Ellezam, B., Yamanaka, Y., Olivos, H.J., Morales, C.R., Joyal, J.S., Lefeber, D.J., Garozzo, D., Dumont, N.A., and Pshezhetsky, A.V.

Abstract

Contains fulltext : 294352.pdf (Publisher’s version ) (Open Access), Deleterious variants in N-acetylneuraminate pyruvate lyase (NPL) cause skeletal myopathy and cardiac edema in humans and zebrafish, but its physiological role remains unknown. We report generation of mouse models of the disease: Npl(R63C), carrying the human p.Arg63Cys variant, and Npl(del116) with a 116-bp exonic deletion. In both strains, NPL deficiency causes drastic increase in free sialic acid levels, reduction of skeletal muscle force and endurance, slower healing and smaller size of newly formed myofibers after cardiotoxin-induced muscle injury, increased glycolysis, partially impaired mitochondrial function, and aberrant sialylation of dystroglycan and mitochondrial LRP130 protein. NPL-catalyzed degradation of sialic acid in the muscle increases after fasting and injury and in human patient and mouse models with genetic muscle dystrophy, demonstrating that NPL is essential for muscle function and regeneration and serves as a general marker of muscle damage. Oral administration of N-acetylmannosamine rescues skeletal myopathy, as well as mitochondrial and structural abnormalities in Npl(R63C) mice, suggesting a potential treatment for human patients.

Published
2023

3. MAPK and mTOR Inhibition Improves Childhood RASopathy-Associated Hypertrophic Cardiomyopathy

Author

Wolf, C. M., additional, Zenker, M., additional, Boleti, O., additional, Norrish, G., additional, Russell, M., additional, Meisner, J. K., additional, Peng, D. M., additional, Prendiville, T., additional, Kleinmahon, J., additional, Kantor, P., additional, Gottlieb, S. D., additional, Human, D., additional, Ewert, P., additional, Krueger, M., additional, Reber, D., additional, Donner, B., additional, Hart, C., additional, Komazec, I. O., additional, Rupp, S., additional, Hahn, A., additional, Hanser, A., additional, Draaisma, J. M., additional, Ten, C. F.E., additional, Mussa, A., additional, Ferrero, G. B., additional, Vaujois, L., additional, Raboisson, M. J., additional, Marquis, C., additional, Théoret, Y., additional, Bogarapu, S., additional, Dancea, A., additional, Moller, H. M., additional, Kemna, M., additional, Kaski, J. P., additional, Gelb, B. D., additional, and Andelfinger, G., additional

Published
2023
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4. Common Genetic Variants Contribute to Risk of Transposition of the Great Arteries

Author

Škorić-Milosavljević, D, Tadros, R, Bosada, FM, Tessadori, F, van Weerd, JH, Woudstra, OI, Tjong, FVY, Lahrouchi, N, Bajolle, F, Cordell, HJ, Agopian, AJ, Blue, GM, Barge-Schaapveld, DQCM, Gewillig, M, Preuss, C, Lodder, EM, Barnett, P, Ilgun, A, Beekman, L, van Duijvenboden, K, Bokenkamp, R, Müller-Nurasyid, M, Vliegen, HW, Konings, TC, van Melle, JP, van Dijk, APJ, van Kimmenade, RRJ, Roos-Hesselink, JW, Sieswerda, GT, Meijboom, F, Abdul-Khaliq, H, Berger, F, Dittrich, S, Hitz, M-P, Moosmann, J, Riede, F-T, Schubert, S, Galan, P, Lathrop, M, Munter, HM, Al-Chalabi, A, Shaw, CE, Shaw, PJ, Morrison, KE, Veldink, JH, van den Berg, LH, Evans, S, Nobrega, MA, Aneas, I, Radivojkov-Blagojević, M, Meitinger, T, Oechslin, E, Mondal, T, Bergin, L, Smythe, JF, Altamirano-Diaz, L, Lougheed, J, Bouma, BJ, Chaix, M-A, Kline, J, Bassett, AS, Andelfinger, G, van der Palen, RLF, Bouvagnet, P, Clur, S-AB, Breckpot, J, Kerstjens-Frederikse, WS, Winlaw, DS, Bauer, UMM, Mital, S, Goldmuntz, E, Keavney, B, Bonnet, D, Mulder, BJ, Tanck, MWT, Bakkers, J, Christoffels, VM, Boogerd, CJ, Postma, AV, Bezzina, CR, Hubrecht Institute for Developmental Biology and Stem Cell Research, Cardiology, Cardiovascular Centre (CVC), Medical Biology, ACS - Heart failure & arrhythmias, ACS - Pulmonary hypertension & thrombosis, Human Genetics, Amsterdam Reproduction & Development (AR&D), Amsterdam Cardiovascular Sciences, General Paediatrics, Paediatric Cardiology, APH - Aging & Later Life, APH - Personalized Medicine, Epidemiology and Data Science, APH - Methodology, Pediatric surgery, and Physiology

Subjects
Genome-wide association study, Multifactorial Inheritance, congenital, hereditary, and neonatal diseases and abnormalities, Cardiac & Cardiovascular Systems, Physiology, Transposition of Great Vessels, Vascular damage Radboud Institute for Health Sciences [Radboudumc 16], ZIC3 MUTATIONS, DE-NOVO, Polymorphism, Single Nucleotide, Wnt-5a Protein, Article, Mice, OF-FUNCTION MUTATIONS, Congenital Heart Disease, Genome-wide Association Study, Single Nucleotide Polymorphism, Transposition Of Great Vessels, Animals, Humans, MALFORMATIONS, Myocytes, Cardiac, GENOME-WIDE ASSOCIATION, Transposition of great vessels, Cells, Cultured, Zebrafish, Congenital heart disease, WNT5A MUTATIONS, Science & Technology, HERITABILITY, Wnt-5a protein, Hematology, DEFECTS, Single nucleotide polymorphism, CONGENITAL HEART-DISEASE, Peripheral Vascular Disease, Cardiovascular System & Cardiology, HYPOPLASTIC LEFT-HEART, T-Box Domain Proteins, Cardiology and Cardiovascular Medicine, Life Sciences & Biomedicine
Abstract

Rationale: Dextro-transposition of the great arteries (D-TGA) is a severe congenital heart defect which affects approximately 1 in 4,000 live births. While there are several reports of D-TGA patients with rare variants in individual genes, the majority of D-TGA cases remain genetically elusive. Familial recurrence patterns and the observation that most cases with D-TGA are sporadic suggest a polygenic inheritance for the disorder, yet this remains unexplored. Objective: We sought to study the role of common single nucleotide polymorphisms (SNPs) in risk for D-TGA. Methods and Results: We conducted a genome-wide association study in an international set of 1,237 patients with D-TGA and identified a genome-wide significant susceptibility locus on chromosome 3p14.3, which was subsequently replicated in an independent case-control set (rs56219800, meta-analysis P=8.6x10 -10 , OR=0.69 per C allele). SNP-based heritability analysis showed that 25% of variance in susceptibility to D-TGA may be explained by common variants. A genome-wide polygenic risk score derived from the discovery set was significantly associated to D-TGA in the replication set (P=4x10 -5 ). The genome-wide significant locus (3p14.3) co-localizes with a putative regulatory element that interacts with the promoter of WNT5A , which encodes the Wnt Family Member 5A protein known for its role in cardiac development in mice. We show that this element drives reporter gene activity in the developing heart of mice and zebrafish and is bound by the developmental transcription factor TBX20. We further demonstrate that TBX20 attenuates Wnt5a expression levels in the developing mouse heart. Conclusions: This work provides support for a polygenic architecture in D-TGA and identifies a susceptibility locus on chromosome 3p14.3 near WNT5A . Genomic and functional data support a causal role of WNT5A at the locus.

Published
2022
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5. MAPK AND AKT/MTOR INHIBITION IMPROVES CHILDHOOD RASOPATHY-ASSOCIATED CARDIOMYOPATHY

Author

Andelfinger, G., primary, Zenker, M., additional, Norrish, G., additional, Russell, M., additional, Meisner, J., additional, Peng, D., additional, Prendiville, T., additional, Kleinmahon, J., additional, Kantor, P., additional, Sen, D Gottlieb, additional, Human, D., additional, Ewert, P., additional, Krueger, M., additional, Reber, D., additional, Donner, B., additional, Hart, C., additional, Odri-Komazec, I., additional, Rupp, S., additional, Hahn, A., additional, Hanser, A., additional, Hofbeck, M., additional, Draaisma, J., additional, Udink ten Cate, F., additional, Mussa, A., additional, Ferrero, G., additional, Vaujois, L., additional, Raboisson, M., additional, Delrue, M., additional, Marquis, C., additional, Théorêt, Y., additional, Kaski, J., additional, Gelb, B., additional, and Wolf, C., additional

Published
2022
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7. Common Genetic Variants Contribute to Risk of Transposition of the Great Arteries

Author

Škorić-Milosavljević, D., Tadros, R., Bosada, F.M., Tessadori, F., Weerd, J.H. van, Woudstra, O.I., Tjong, F.V.Y., Lahrouchi, N., Bajolle, F., Cordell, H.J., Agopian, A.J., Blue, G.M., Barge-Schaapveld, D., Gewillig, M., Preuss, C., Lodder, E.M., Barnett, P., Ilgun, A., Beekman, L., Duijvenboden, K. van, Bokenkamp, R., Müller-Nurasyid, M., Vliegen, H.W., Konings, T.C., Melle, J.P. van, Dijk, A.P.J. van, Kimmenade, R.R.J. van, Roos-Hesselink, J.W., Sieswerda, G.T., Meijboom, F., Abdul-Khaliq, H., Berger, F, Dittrich, S., Hitz, M.P., Moosmann, J., Riede, F.T., Schubert, S., Galan, P., Lathrop, M., Munter, H.M., Al-Chalabi, A., Shaw, C.E., Shaw, P.J., Morrison, K.E., Veldink, J.H., Berg, L.H. van den, Evans, S., Nobrega, M.A., Aneas, I., Radivojkov-Blagojević, M., Meitinger, T., Oechslin, E., Mondal, T., Bergin, L., Smythe, J.F., Altamirano-Diaz, L., Lougheed, J., Bouma, B.J., Chaix, M.A., Kline, J., Bassett, A.S., Andelfinger, G., Palen, R.L.F. van der, Bouvagnet, P., Clur, S.B., Breckpot, J., Kerstjens-Frederikse, W.S., Winlaw, D.S., Bauer, U.M.M., Mital, S., Goldmuntz, E., Keavney, B., Bonnet, D., Mulder, B. J. M., Tanck, M.W.T., Bakkers, J., Christoffels, V.M., Boogerd, C.J., Postma, A.V., Bezzina, C.R., Škorić-Milosavljević, D., Tadros, R., Bosada, F.M., Tessadori, F., Weerd, J.H. van, Woudstra, O.I., Tjong, F.V.Y., Lahrouchi, N., Bajolle, F., Cordell, H.J., Agopian, A.J., Blue, G.M., Barge-Schaapveld, D., Gewillig, M., Preuss, C., Lodder, E.M., Barnett, P., Ilgun, A., Beekman, L., Duijvenboden, K. van, Bokenkamp, R., Müller-Nurasyid, M., Vliegen, H.W., Konings, T.C., Melle, J.P. van, Dijk, A.P.J. van, Kimmenade, R.R.J. van, Roos-Hesselink, J.W., Sieswerda, G.T., Meijboom, F., Abdul-Khaliq, H., Berger, F, Dittrich, S., Hitz, M.P., Moosmann, J., Riede, F.T., Schubert, S., Galan, P., Lathrop, M., Munter, H.M., Al-Chalabi, A., Shaw, C.E., Shaw, P.J., Morrison, K.E., Veldink, J.H., Berg, L.H. van den, Evans, S., Nobrega, M.A., Aneas, I., Radivojkov-Blagojević, M., Meitinger, T., Oechslin, E., Mondal, T., Bergin, L., Smythe, J.F., Altamirano-Diaz, L., Lougheed, J., Bouma, B.J., Chaix, M.A., Kline, J., Bassett, A.S., Andelfinger, G., Palen, R.L.F. van der, Bouvagnet, P., Clur, S.B., Breckpot, J., Kerstjens-Frederikse, W.S., Winlaw, D.S., Bauer, U.M.M., Mital, S., Goldmuntz, E., Keavney, B., Bonnet, D., Mulder, B. J. M., Tanck, M.W.T., Bakkers, J., Christoffels, V.M., Boogerd, C.J., Postma, A.V., and Bezzina, C.R.

Abstract

Item does not contain fulltext, RATIONALE: Dextro-transposition of the great arteries (D-TGA) is a severe congenital heart defect which affects approximately 1 in 4,000 live births. While there are several reports of D-TGA patients with rare variants in individual genes, the majority of D-TGA cases remain genetically elusive. Familial recurrence patterns and the observation that most cases with D-TGA are sporadic suggest a polygenic inheritance for the disorder, yet this remains unexplored. OBJECTIVE: We sought to study the role of common single nucleotide polymorphisms (SNPs) in risk for D-TGA. METHODS AND RESULTS: We conducted a genome-wide association study in an international set of 1,237 patients with D-TGA and identified a genome-wide significant susceptibility locus on chromosome 3p14.3, which was subsequently replicated in an independent case-control set (rs56219800, meta-analysis P=8.6x10(-10), OR=0.69 per C allele). SNP-based heritability analysis showed that 25% of variance in susceptibility to D-TGA may be explained by common variants. A genome-wide polygenic risk score derived from the discovery set was significantly associated to D-TGA in the replication set (P=4x10(-5)). The genome-wide significant locus (3p14.3) co-localizes with a putative regulatory element that interacts with the promoter of WNT5A, which encodes the Wnt Family Member 5A protein known for its role in cardiac development in mice. We show that this element drives reporter gene activity in the developing heart of mice and zebrafish and is bound by the developmental transcription factor TBX20. We further demonstrate that TBX20 attenuates Wnt5a expression levels in the developing mouse heart. CONCLUSIONS: This work provides support for a polygenic architecture in D-TGA and identifies a susceptibility locus on chromosome 3p14.3 near WNT5A. Genomic and functional data support a causal role of WNT5A at the locus.

Published
2022

10. AKT/mTOR and MAPK Inhibition Improves Childhood RASopathic Cardiomyopathy

Author

Wolf, C. M., additional, Zenker, M., additional, Norrish, G., additional, Russell, M., additional, Meisner, J. K., additional, Peng, D. M., additional, Prendiville, T., additional, Kleinmahon, J., additional, Kantor, P. F., additional, Sen, D. Gottlieb, additional, Human, D. G., additional, Ewert, P., additional, Krueger, M., additional, Reber, D., additional, Donner, B. C., additional, Hart, C., additional, Odri-Komazec, I., additional, Rupp, S., additional, Hahn, A., additional, Hanser, A., additional, Hofbeck, M., additional, Draaisma, J. M., additional, Cate, F.E.A. Udink Ten, additional, Mussa, A., additional, Ferrero, G. B., additional, Marquis, C., additional, Théoret, Y., additional, Kaski, J. P., additional, Gelb, B. D., additional, and Andelfinger, G., additional

Published
2022
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11. 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
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13. Integrative analysis of genomic variants reveals new associations of candidate haploinsufficient genes with congenital heart disease

Author

Audain, E, primary, Wilsdon, A, additional, Breckpot, J, additional, Izarzugaza, JMG, additional, Fitzgerald, TW, additional, Kahlert, AK, additional, Sifrim, A, additional, Wünnemann, F, additional, Perez-Riverol, Y, additional, Abdul-Khaliq, H, additional, Bak, M, additional, Bassett, AS, additional, Belmont, JW, additional, Benson, DW, additional, Berger, F, additional, Daehnert, I, additional, Devriendt, K, additional, Dittrich, S, additional, Daubeney, P, additional, Garg, V, additional, Hackmann, K, additional, Hoff, K, additional, Hofmann, P, additional, Dombrowsky, G, additional, Pickardt, T, additional, Bauer, U, additional, Keavney, BD, additional, Klaassen, S, additional, Kramer, HH, additional, Marshall, CR, additional, Milewicz, DM, additional, Lemaire, SA, additional, Coselli, J, additional, Mitchell, ME, additional, Tomita-Mitchell, A, additional, Prakash, SK, additional, Stamm, K, additional, Stewart, AFR, additional, Silversides, CK, additional, Siebert, R, additional, Stiller, B, additional, Rosenfeld, JA, additional, Vater, I, additional, Postma, AV, additional, Caliebe, A, additional, Brook, JD, additional, Andelfinger, G, additional, Hurles, ME, additional, Thienpont, B, additional, Larsen, LA, additional, and Hitz, MP, additional

Published
2020
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21. Candidate Gene Resequencing in a Large Bicuspid Aortic Valve-Associated Thoracic Aortic Aneurysm Cohort: SMAD6 as an Important Contributor

Author

Gillis, E., Kumar, A.A., Luyckx, I., Preuss, C., Cannaerts, E., Beek, G. van de, Wieschendorf, B., Alaerts, M., Bolar, N., Vandeweyer, G., Meester, J. de, Wunnemann, F., Gould, R.A., Zhurayev, R., Zerbino, D., Mohamed, S.A., Mital, S., Mertens, L., Bjorck, H.M., Franco-Cereceda, A., McCallion, A.S., Laer, L. Van, Verhagen, J.M.A., Laar, I. van de, Wessels, M.W., Messas, E., Goudot, G., Nemcikova, M., Krebsova, A., Kempers, M.J.E., Salemink, S., Duijnhouwer, T., Jeunemaitre, X., Albuisson, J., Eriksson, P., Andelfinger, G., Dietz, H.C., Verstraeten, A., Loeys, B.L., Gillis, E., Kumar, A.A., Luyckx, I., Preuss, C., Cannaerts, E., Beek, G. van de, Wieschendorf, B., Alaerts, M., Bolar, N., Vandeweyer, G., Meester, J. de, Wunnemann, F., Gould, R.A., Zhurayev, R., Zerbino, D., Mohamed, S.A., Mital, S., Mertens, L., Bjorck, H.M., Franco-Cereceda, A., McCallion, A.S., Laer, L. Van, Verhagen, J.M.A., Laar, I. van de, Wessels, M.W., Messas, E., Goudot, G., Nemcikova, M., Krebsova, A., Kempers, M.J.E., Salemink, S., Duijnhouwer, T., Jeunemaitre, X., Albuisson, J., Eriksson, P., Andelfinger, G., Dietz, H.C., Verstraeten, A., and Loeys, B.L.

Abstract

Contains fulltext : 176973.pdf (publisher's version ) (Open Access), 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

22. Candidate gene resequencing in a large bicuspid aortic valve-associated thoracic aortic aneurysm cohort: SMAD6 as an important contributor

Author

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

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
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23. Corrigendum: Candidate gene resequencing in a large bicuspid aortic valve-associated thoracic aortic aneurysm cohort: SMAD6 as an important contributor [Front. Physiol, 8, (2017) (400)] doi: 10.3389/fphys.2017.00400

Author

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

Abstract

In the original article, we noted two mutation annotation errors. The correction of these two mistakes does not change the scientific conclusions in any way. The authors apologize for these nomenclature errors. Please find below the corrected annotations of those two mutations: (1) The correct RNA and protein annotations of the SMAD6 variant in P99 are c.455_461del and p.Pro152Profs*27, and not c.454_461del and p.Gly166Valfs*23. (2) The correct RNA and protein annotations of the SMAD6 variant in P128 are c.74_79del and p.Ser27_Gly28del, and not c.73_79del and p.Gly26_Ser27del. As a consequence, a correction has been made to RESULTS, Paragraphs 5 and 6: The SMAD6 c.726del variant leads to a frameshift (p.Lys242Asnfs*300) and a predicted protein with a C-terminal extension due to loss of the intended stop codon. The c.455_461del frameshift variant (p.Pro152Profs*27) causes the introduction of a premature stop codon, most likely resulting in haploinsufficiency due to nonsense-mediated mRNA decay (NMD). Also the two nonsense variants (p.Tyr279* and p.Tyr288*) are predicted to lead to NMD. All of the missense variants cluster in the functionally important MH1 and MH2 domains (Makkar et al., 2009) (amino acids 148-275 and 331-496, respectively), which is not the case for the sole missense variant (p.Ser130Leu) found in a control individual (Figure 2). All but one (p.Arg443His) of the identified variants were absent in the ExAC control cohort (v0.3.1; Supplementary Table 2). Moreover, the missense variants in the patient cohort (7/7) are enriched in the MH1 and MH2 domains when compared to ExAC controls (n = 228/430; p = 0.02).

Published
2017
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24. Candidate Gene Resequencing in a Large Bicuspid Aortic Valve-Associated Thoracic Aortic Aneurysm Cohort: SMAD6 as an Important Contributor

Author

Gillis, E, Kumar, AA, Luyckx, I, Preuss, C, Cannaerts, E, van de Beek, G, Wieschendorf, B, Alaerts, M, Bolar, N, Vandeweyer, G, Meester, J, Wunnemann, F, Gould, RA, Zhurayev, R, Zerbino, D, Mohamed, SA, Mital, S, Mertens, L, Bjorck, HM, Franco-Cereceda, A, McCallion, AS, Van Laer, L, Verhagen, Judith, De Graaf - van de Laar, Ingrid, Wessels, Marja, Messas, E, Goudot, G, Nemcikova, M, Krebsova, A, Kempers, M, Salemink, S, Duijnhouwer, T, Jeunemaitre, X, Albuisson, J, Eriksson, P, Andelfinger, G, Dietz, HC, Verstraeten, A (Aline), Loeys, BL, Gillis, E, Kumar, AA, Luyckx, I, Preuss, C, Cannaerts, E, van de Beek, G, Wieschendorf, B, Alaerts, M, Bolar, N, Vandeweyer, G, Meester, J, Wunnemann, F, Gould, RA, Zhurayev, R, Zerbino, D, Mohamed, SA, Mital, S, Mertens, L, Bjorck, HM, Franco-Cereceda, A, McCallion, AS, Van Laer, L, Verhagen, Judith, De Graaf - van de Laar, Ingrid, Wessels, Marja, Messas, E, Goudot, G, Nemcikova, M, Krebsova, A, Kempers, M, Salemink, S, Duijnhouwer, T, Jeunemaitre, X, Albuisson, J, Eriksson, P, Andelfinger, G, Dietz, HC, Verstraeten, A (Aline), and Loeys, BL

Published
2017

25. Erratum: Polymorphisms of ABCC5 and NOS3 genes influence doxorubicin cardiotoxicity in survivors of childhood acute lymphoblastic leukemia

Author

Krajinovic, M, primary, Elbared, J, additional, Drouin, S, additional, Bertout, L, additional, Rezgui, A, additional, Ansari, M, additional, Raboisson, M-J, additional, Lipshultz, S E, additional, Silverman, L B, additional, Sallan, S E, additional, Neuberg, D S, additional, Kutok, J L, additional, Laverdière, C, additional, Sinnett, D, additional, and Andelfinger, G, additional

Published
2016
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32. Polymorphisms of ABCC5 and NOS3 genes influence doxorubicin cardiotoxicity in survivors of childhood acute lymphoblastic leukemia

Author

Krajinovic, M, primary, Elbared, J, additional, Drouin, S, additional, Bertout, L, additional, Rezgui, A, additional, Ansari, M, additional, Raboisson, M-J, additional, Lipshultz, S E, additional, Silverman, L B, additional, Sallan, S E, additional, Neuberg, D S, additional, Kutok, J L, additional, Laverdière, C, additional, Sinnett, D, additional, and Andelfinger, G, additional

Published
2015
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44. Polymorphisms of ABCC5and NOS3genes influence doxorubicin cardiotoxicity in survivors of childhood acute lymphoblastic leukemia

Author

Krajinovic, M, Elbared, J, Drouin, S, Bertout, L, Rezgui, A, Ansari, M, Raboisson, M-J, Lipshultz, S E, Silverman, L B, Sallan, S E, Neuberg, D S, Kutok, J L, Laverdière, C, Sinnett, D, and Andelfinger, G

Abstract

Anthracyclines are efficient chemotherapy agents. However, their use is limited by anthracycline-induced cardiotoxicity (CT). We investigated the influence of polymorphisms in doxorubicin metabolic and functional pathways on late-onset CT as estimated by echocardiography in 251 childhood acute lymphoblastic leukemia (cALL) patients. Association analyses revealed a modulating effect of two variants: A-1629?T in ABCC5, an ATP-binding cassette transporter, and G894T in the NOS3endothelial nitric oxide synthase gene. Individuals with the ABCC5 TT-1629 genotype had an average of 8–12% reduction of ejection (EF) and shortening fractions (SF; EF: P<0.0001, and SF: P=0.001, respectively). A protective effect of the NOS3TT894 genotype on EF was seen in high-risk patients (P=0.02), especially in those who did not receive dexrazoxane (P=0.002). Analysis of an additional cohort of 44 cALL patients replicated the ABCC5association but was underpowered for NOS3. In summary, we identified two biomarkers that may contribute to cALL anthracycline CT risk stratification.

Published
2016
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49. A New Source of Iodine for Salt Blocks

Author

Kuhajek, E. J. and Andelfinger, G. F.

Abstract

The nutritional availability, physical availability and oral toxicity of pentacalcium orthoperiodate (PCOP) have been investigated. Eight-week diet studies with rats showed that the iodine in PCOP is as nutritionally available as iodide (sodium iodide) and iodate (calcium iodate). When salt blocks containing PCOP at a level of 0.008% iodine were fed to cattle, adequate iodine was found to be continuously available at the surface of these blocks. Both acute and subacute oral toxicity tests with rats demonstrated that PCOP is a safe source of supplemental iodine.

Published
1970
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50. Partitioning of copy-number genotypes in pedigrees

Author

Andelfinger Gregor U, Perreault Louis-Philippe, Asselin Géraldine, and Dubé Marie-Pierre

Subjects
Computer applications to medicine. Medical informatics, R858-859.7, Biology (General), QH301-705.5
Abstract

Abstract Background Copy number variations (CNVs) and polymorphisms (CNPs) have only recently gained the genetic community's attention. Conservative estimates have shown that CNVs and CNPs might affect more than 10% of the genome and that they may be at least as important as single nucleotide polymorphisms in assessing human variability. Widely used tools for CNP analysis have been implemented in Birdsuite and PLINK for the purpose of conducting genetic association studies based on the unpartitioned total number of CNP copies provided by the intensities from Affymetrix's Genome-Wide Human SNP Array. Here, we are interested in partitioning copy number variations and polymorphisms in extended pedigrees for the purpose of linkage analysis on familial data. Results We have developed CNGen, a new software for the partitioning of copy number polymorphism using the integrated genotypes from Birdsuite with the Affymetrix platform. The algorithm applied to familial trios or extended pedigrees can produce partitioned copy number genotypes with distinct parental alleles. We have validated the algorithm using simulations on a complex pedigree structure using frequencies calculated from a real dataset of 300 genotyped samples from 42 pedigrees segregating a congenital heart defect phenotype. Conclusions CNGen is the first published software for the partitioning of copy number genotypes in pedigrees, making possible the use CNPs and CNVs for linkage analysis. It was implemented with the Python interpreter version 2.5.2. It was successfully tested on current Linux, Windows and Mac OS workstations.

Published
2010
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