Your search keyword '"van Tintelen, J. Peter"' showing total 65 results

1. Penetrance and Prognosis of MYH7Variant-Associated Cardiomyopathies

Author

Jansen, Mark, de Brouwer, Remco, Hassanzada, Fahima, Schoemaker, Angela E., Schmidt, Amand F., Kooijman-Reumerman, Maria D., Bracun, Valentina, Slieker, Martijn G., Dooijes, Dennis, Vermeer, Alexa M.C., Wilde, Arthur A.M., Amin, Ahmad S., Lekanne Deprez, Ronald H., Herkert, Johanna C., Christiaans, Imke, de Boer, Rudolf A., Jongbloed, Jan D.H., van Tintelen, J. Peter, Asselbergs, Folkert W., and Baas, Annette F.

Abstract

MYH7variants cause hypertrophic cardiomyopathy (HCM), noncompaction cardiomyopathy (NCCM), and dilated cardiomyopathy (DCM). Screening of relatives of patients with genetic cardiomyopathy is recommended from 10 to 12 years of age onward, irrespective of the affected gene.

Published

2024

2. Predicting personal cardiovascular disease risk based on family health history: Development of expert-based family criteria for the general population

Author

Dijkstra, Tetske, van den Heuvel, Lieke M., van Tintelen, J. Peter, van der Werf, Christian, van Langen, Irene M., and Christiaans, Imke

Abstract

In inherited and familial cardiovascular diseases (CVDs), relatives without current symptoms can still be at risk for early and preventable cardiovascular events. One way to help people evaluate their potential risk of CVD is through a risk-assessment tool based on family health history. However, family criteria including inherited CVD risk to be used by laypersons are non-existent. In this project, we employed a qualitative study design to develop expert-based family criteria for use in individual risk assessment. In the first phase of the project, we identified potential family criteria through an online focus group with physicians with expertise in monogenic and/or multifactorial CVDs. The family criteria from phase one were then used as input for a three-round Delphi procedure carried out in a larger group of expert physicians to reach consensus on appropriate criteria. This led to consensus on five family criteria that focus on cardiovascular events at young age (i.e., sudden death, any CVD, implantable cardioverter-defibrillator, aortic aneurysm) and/or an inherited CVD in one or more close relatives. We then applied these family criteria to a high-risk cohort from a clinical genetics department and demonstrated that they have substantial diagnostic accuracy. After further evaluation in a general population cohort, we decided to only use the family criteria for first-degree relatives. We plan to incorporate these family criteria into a digital tool for easy risk assessment by the public and, based on expert advice, will develop supporting information for general practitioners to act upon potential risks identified by the tool.

Published

2023

3. Programmed Ventricular Stimulation as an Additional Primary Prevention Risk Stratification Tool in Arrhythmogenic Right Ventricular Cardiomyopathy: A Multinational Study

Author

Gasperetti, Alessio, Carrick, Richard T., Costa, Sarah, Compagnucci, Paolo, Bosman, Laurens P., Chivulescu, Monica, Tichnell, Crystal, Murray, Brittney, Tandri, Harikrishna, Tadros, Rafik, Rivard, Lena, van den Berg, Maarten P., Zeppenfeld, Katja, Wilde, Arthur A.M., Pompilio, Giulio, Carbucicchio, Corrado, Dello Russo, Antonio, Casella, Michela, Svensson, Anneli, Brunckhorst, Corinna B., van Tintelen, J. Peter, Platonov, Pyotr G., Haugaa, Kristina H., Duru, Firat, te Riele, Anneline S.J.M., Khairy, Paul, Tondo, Claudio, Calkins, Hugh, James, Cynthia A., Saguner, Ardan M., and Cadrin-Tourigny, Julia

Published

2022

4. Sex-specific aspects of phospholamban cardiomyopathy: The importance and prognostic value of low-voltage electrocardiograms.

Author

de Brouwer, Remco, Meems, Laura M.G., Verstraelen, Tom E., Mahmoud, Belend, Proost, Virginnio, Wilde, Arthur A.M., Bosman, Laurens P., van Drie, Esmée, van der Zwaag, Paul A., van Tintelen, J. Peter, Houweling, Arjan C., van den Berg, Maarten P., and de Boer, Rudolf A.

Abstract

Background: A pathogenic variant in the gene encoding phospholamban (PLN), a protein that regulates calcium homeostasis of cardiomyocytes, causes PLN cardiomyopathy. It is characterized by a high arrhythmic burden and can progress to severe cardiomyopathy. Risk assessment guides implantable cardioverter-defibrillator therapy and benefits from personalization. Whether sex-specific differences in PLN cardiomyopathy exist is unknown.Objective: The purpose of this study was to improve the accuracy of PLN cardiomyopathy diagnosis and risk assessment by investigating sex-specific aspects.Methods: We analyzed a multicenter cohort of 933 patients (412 male, 521 female) with the PLN p.(Arg14del) pathogenic variant following up on a recently developed PLN risk model. Sex-specific differences in the incidence of risk model components were investigated: low-voltage electrocardiogram (ECG), premature ventricular contractions, negative T waves, and left ventricular ejection fraction.Results: Sustained ventricular arrhythmias (VAs) occurred in 77 males (18.7%) and 61 females (11.7%) (P = .004). Of the 933 cohort members, 287 (31%) had ≥1 low-voltage ECG during follow-up (180 females [63%], 107 males [37%]; P = .006). Female sex, age, age at clinical presentation, and proband status predicted low-voltage ECG during follow-up (area under the curve: 0.78). Sustained VA-free survival was lowest in males with low-voltage ECG (P <.001).Conclusion: Low-voltage ECGs predict sustained VA and are a component of the PLN risk model. Low-voltage ECGs are more common in females, yet prognostic value is greater in males. Future studies should determine the impact of this difference on the risk prediction of PLN cardiomyopathy and possibly other cardiomyopathies. [ABSTRACT FROM AUTHOR]

Published

2022

5. Phenotypic Expression, Natural History, and Risk Stratification of Cardiomyopathy Caused by Filamin C Truncating Variants

Author

Gigli, Marta, Stolfo, Davide, Graw, Sharon L., Merlo, Marco, Gregorio, Caterina, Nee Chen, Suet, Dal Ferro, Matteo, PaldinoMD, Alessia, De Angelis, Giulia, Brun, Francesca, Jirikowic, Jean, Salcedo, Ernesto E., Turja, Sylvia, Fatkin, Diane, Johnson, Renee, van Tintelen, J. Peter, Te Riele, Anneline S.J.M., Wilde, Arthur A.M., Lakdawala, Neal K., Picard, Kermshlise, Miani, Daniela, Muser, Daniele, Maria Severini, Giovanni, Calkins, Hugh, James, Cynthia A., Murray, Brittney, Tichnell, Crystal, Parikh, Victoria N., Ashley, Euan A., Reuter, Chloe, Song, Jiangping, Judge, Daniel P., McKenna, William J., Taylor, Matthew R.G., Sinagra, Gianfranco, and Mestroni, Luisa

Abstract

Supplemental Digital Content is available in the text.

Published

2021

6. The genetic architecture of Plakophilin 2 cardiomyopathy

Author

Dries, Annika M., Kirillova, Anna, Reuter, Chloe M., Garcia, John, Zouk, Hana, Hawley, Megan, Murray, Brittney, Tichnell, Crystal, Pilichou, Kalliopi, Protonotarios, Alexandros, Medeiros-Domingo, Argelia, Kelly, Melissa A., Baras, Aris, Ingles, Jodie, Semsarian, Christopher, Bauce, Barbara, Celeghin, Rudy, Basso, Cristina, Jongbloed, Jan D.H., Nussbaum, Robert L., Funke, Birgit, Cerrone, Marina, Mestroni, Luisa, Taylor, Matthew R.G., Sinagra, Gianfranco, Merlo, Marco, Saguner, Ardan M., Elliott, Perry M., Syrris, Petros, van Tintelen, J. Peter, James, Cynthia A., Haggerty, Christopher M., and Parikh, Victoria N.

Abstract

The genetic architecture of Plakophilin 2 (PKP2) cardiomyopathy can inform our understanding of its variant pathogenicity and protein function.

Published

2021

7. Clinical characteristics and determinants of the phenotype in TMEM43 arrhythmogenic right ventricular cardiomyopathy type 5.

Author

Dominguez, Fernando, Zorio, Esther, Jimenez-Jaimez, Juan, Salguero-Bodes, Rafael, Zwart, Robert, Gonzalez-Lopez, Esther, Molina, Pilar, Bermúdez-Jiménez, Francisco, Delgado, Juan F., Braza-Boïls, Aitana, Bornstein, Belen, Toquero, Jorge, Segovia, Javier, Van Tintelen, J. Peter, Lara-Pezzi, Enrique, and Garcia-Pavia, Pablo

Abstract

Background: Arrhythmogenic right ventricular cardiomyopathy type V (ARVC-5) is the most aggressive heterozygous form of ARVC. It is predominantly caused by a fully penetrant mutation (p.S358L) in the nondesmosomal gene TMEM43-endemic to Newfoundland, Canada. To date, all familial cases reported worldwide share a common ancestral haplotype. It is unknown whether the p.S358L mutation by itself causes ARVC-5 or whether the disease is influenced by genetic or environmental factors.Objective: The purpose of this study was to examine the phenotype, clinical course, and the impact of exercise on patients with p.S358L ARVC-5 without the Newfoundland genetic background.Methods: We studied 62 affected individuals and 73 noncarriers from 3 TMEM43-p.S358L Spanish families. The impact of physical activity on the phenotype was also evaluated.Results: Haplotype analysis revealed that the 3 Spanish families were unrelated to patients with ARVC-5 with the Newfoundland genetic background. Two families shared 10 microsatellite markers in a 4.9 cM region surrounding TMEM43; the third family had a distinct haplotype. The affected individuals showed a 38.7% incidence of sudden cardiac death, which was higher in men. Left ventricular involvement was common, with 40% of mutation carriers showing a left ventricular ejection fraction of <50%. Compared with noncarriers, the R-wave voltage in lead V3 was lower (3.2 ± 2.8 mV vs 7.5 ± 3.6 mV; P < .001) and QRS complex in right precordial leads wider (104.7 ± 24.0 ms vs 88.2 ± 7.7 ms; P = .001). A history of vigorous exercise showed a trend toward more ventricular arrhythmias only in women (P = .053).Conclusion: ARVC-5 is associated with a high risk of sudden cardiac death and characteristic clinical and electrocardiographic features irrespective of geographical origin and genetic background. Our data suggest that, as in desmosomal ARVC, vigorous physical activity could aggravate the phenotype of TMEM43 mutation carriers. [ABSTRACT FROM AUTHOR]

Published

2020

8. Shared genetic pathways contribute to risk of hypertrophic and dilated cardiomyopathies with opposite directions of effect

Author

Tadros, Rafik, Francis, Catherine, Xu, Xiao, Vermeer, Alexa M. C., Harper, Andrew R., Huurman, Roy, Kelu Bisabu, Ken, Walsh, Roddy, Hoorntje, Edgar T., te Rijdt, Wouter P., Buchan, Rachel J., van Velzen, Hannah G., van Slegtenhorst, Marjon A., Vermeulen, Jentien M., Offerhaus, Joost Allard, Bai, Wenjia, de Marvao, Antonio, Lahrouchi, Najim, Beekman, Leander, Karper, Jacco C., Veldink, Jan H., Kayvanpour, Elham, Pantazis, Antonis, Baksi, A. John, Whiffin, Nicola, Mazzarotto, Francesco, Sloane, Geraldine, Suzuki, Hideaki, Schneider-Luftman, Deborah, Elliott, Paul, Richard, Pascale, Ader, Flavie, Villard, Eric, Lichtner, Peter, Meitinger, Thomas, Tanck, Michael W. T., van Tintelen, J. Peter, Thain, Andrew, McCarty, David, Hegele, Robert A., Roberts, Jason D., Amyot, Julie, Dubé, Marie-Pierre, Cadrin-Tourigny, Julia, Giraldeau, Geneviève, L’Allier, Philippe L., Garceau, Patrick, Tardif, Jean-Claude, Boekholdt, S. Matthijs, Lumbers, R. Thomas, Asselbergs, Folkert W., Barton, Paul J. R., Cook, Stuart A., Prasad, Sanjay K., O’Regan, Declan P., van der Velden, Jolanda, Verweij, Karin J. H., Talajic, Mario, Lettre, Guillaume, Pinto, Yigal M., Meder, Benjamin, Charron, Philippe, de Boer, Rudolf A., Christiaans, Imke, Michels, Michelle, Wilde, Arthur A. M., Watkins, Hugh, Matthews, Paul M., Ware, James S., and Bezzina, Connie R.

Abstract

The heart muscle diseases hypertrophic (HCM) and dilated (DCM) cardiomyopathies are leading causes of sudden death and heart failure in young, otherwise healthy, individuals. We conducted genome-wide association studies and multi-trait analyses in HCM (1,733 cases), DCM (5,521 cases) and nine left ventricular (LV) traits (19,260 UK Biobank participants with structurally normal hearts). We identified 16 loci associated with HCM, 13 with DCM and 23 with LV traits. We show strong genetic correlations between LV traits and cardiomyopathies, with opposing effects in HCM and DCM. Two-sample Mendelian randomization supports a causal association linking increased LV contractility with HCM risk. A polygenic risk score explains a significant portion of phenotypic variability in carriers of HCM-causing rare variants. Our findings thus provide evidence that polygenic risk score may account for variability in Mendelian diseases. More broadly, we provide insights into how genetic pathways may lead to distinct disorders through opposing genetic effects.

Published

2021

9. A tailored approach to informing relatives at risk of inherited cardiac conditions: results of a randomised controlled trial

Author

van den Heuvel, Lieke M., Hoedemaekers, Yvonne M., Baas, Annette F., Baars, Marieke J. H., van Tintelen, J. Peter, Smets, Ellen M. A., and Christiaans, Imke

Abstract

If undetected, inherited cardiac conditions can lead to sudden cardiac death, while treatment options are available. Predictive DNA testing is therefore advised for at-risk relatives, and probands are currently asked to inform relatives about this. However, fewer than half of relatives attend genetic counselling. In this trial, we compared a tailored approach to informing relatives, in which probands were asked whether they preferred relatives to be informed by themselves or by the genetic counsellor, with current practice. Our primary outcome was uptake of genetic counselling in relatives in the first year after test result disclosure. Secondary outcomes were evaluation of the approach and impact on psychological/family functioning measured 3 (T1) and 9 (T2) months post-disclosure via telephone interviews and questionnaires. We included 96 probands; 482 relatives were eligible for counselling and genetic testing. We observed no significant difference in uptake of genetic counselling between the control (38%) and the intervention (37%) group (p= 0.973). Nor were there significant differences between groups in impact on family/psychological functioning. Significantly more probands in the tailored group were satisfied (p= 0.001) and felt supported (p= 0.003) by the approach, although they also felt somewhat coerced to inform relatives (p< 0.001)and perceived room for improvement (p< 0.001). To conclude, we observed no differences in uptake and impact on family/psychological functioning between the current and tailored approach, but probands in the tailored group more often felt satisfied. Further research on barriers to relatives attending genetic counselling and on how to optimize the provision of a tailored approach is needed.

Published

2021

10. Long-Term Follow-Up Study on the Uptake of Genetic Counseling and Predictive DNA Testing in Inherited Cardiac Conditions

Author

van den Heuvel, Lieke M., van Teijlingen, Maxiem O., van der Roest, Wilma, van Langen, Irene M., Smets, Ellen M.A., van Tintelen, J. Peter, and Christiaans, Imke

Abstract

Supplemental Digital Content is available in the text.

Published

2020

11. Transethnic Genome-Wide Association Study Provides Insights in the Genetic Architecture and Heritability of Long QT Syndrome

Author

Lahrouchi, Najim, Tadros, Rafik, Crotti, Lia, Mizusawa, Yuka, Postema, Pieter G., Beekman, Leander, Walsh, Roddy, Hasegawa, Kanae, Barc, Julien, Ernsting, Marko, Turkowski, Kari L., Mazzanti, Andrea, Beckmann, Britt M., Shimamoto, Keiko, Diamant, Ulla-Britt, Wijeyeratne, Yanushi D., Kucho, Yu, Robyns, Tomas, Ishikawa, Taisuke, Arbelo, Elena, Christiansen, Michael, Winbo, Annika, Jabbari, Reza, Lubitz, Steven A., Steinfurt, Johannes, Rudic, Boris, Loeys, Bart, Shoemaker, M. Ben, Weeke, Peter E., Pfeiffer, Ryan, Davies, Brianna, Andorin, Antoine, Hofman, Nynke, Dagradi, Federica, Pedrazzini, Matteo, Tester, David J., Bos, J. Martijn, Sarquella-Brugada, Georgia, Campuzano, Óscar, Platonov, Pyotr G., Stallmeyer, Birgit, Zumhagen, Sven, Nannenberg, Eline A., Veldink, Jan H., van den Berg, Leonard H., Al-Chalabi, Ammar, Shaw, Christopher E., Shaw, Pamela J., Morrison, Karen E., Andersen, Peter M., Müller-Nurasyid, Martina, Cusi, Daniele, Barlassina, Cristina, Galan, Pilar, Lathrop, Mark, Munter, Markus, Werge, Thomas, Ribasés, Marta, Aung, Tin, Khor, Chiea C., Ozaki, Mineo, Lichtner, Peter, Meitinger, Thomas, van Tintelen, J. Peter, Hoedemaekers, Yvonne, Denjoy, Isabelle, Leenhardt, Antoine, Napolitano, Carlo, Shimizu, Wataru, Schott, Jean-Jacques, Gourraud, Jean-Baptiste, Makiyama, Takeru, Ohno, Seiko, Itoh, Hideki, Krahn, Andrew D., Antzelevitch, Charles, Roden, Dan M., Saenen, Johan, Borggrefe, Martin, Odening, Katja E., Ellinor, Patrick T., Tfelt-Hansen, Jacob, Skinner, Jonathan R., van den Berg, Maarten P., Olesen, Morten Salling, Brugada, Josep, Brugada, Ramón, Makita, Naomasa, Breckpot, Jeroen, Yoshinaga, Masao, Behr, Elijah R., Rydberg, Annika, Aiba, Takeshi, Kääb, Stefan, Priori, Silvia G., Guicheney, Pascale, Tan, Hanno L., Newton-Cheh, Christopher, Ackerman, Michael J., Schwartz, Peter J., Schulze-Bahr, Eric, Probst, Vincent, Horie, Minoru, Wilde, Arthur A., Tanck, Michael W.T., and Bezzina, Connie R.

Abstract

Supplemental Digital Content is available in the text.

Published

2020

12. Homozygous damaging SOD2 variant causes lethal neonatal dilated cardiomyopathy

Author

Almomani, Rowida, Herkert, Johanna C, Posafalvi, Anna, Post, Jan G, Boven, Ludolf G, van der Zwaag, Paul A, Willems, Peter H G M, van Veen-Hof, Ingrid H, Verhagen, Judith M A, Wessels, Marja W, Nikkels, Peter G J, Wintjes, Liesbeth T, van den Berg, Maarten P, Sinke, Richard J, Rodenburg, Richard J, Niezen-Koning, Klary E, van Tintelen, J Peter, and Jongbloed, Jan D H

Abstract

BackgroundIdiopathic dilated cardiomyopathy (DCM) is recognised to be a heritable disorder, yet clinical genetic testing does not produce a diagnosis in >50% of paediatric patients. Identifying a genetic cause is crucial because this knowledge can affect management options, cardiac surveillance in relatives and reproductive decision-making. In this study, we sought to identify the underlying genetic defect in a patient born to consanguineous parents with rapidly progressive DCM that led to death in early infancy.Methods and resultsExome sequencing revealed a potentially pathogenic, homozygous missense variant, c.542G>T, p.(Gly181Val), in SOD2. This gene encodes superoxide dismutase 2 (SOD2) or manganese-superoxide dismutase, a mitochondrial matrix protein that scavenges oxygen radicals produced by oxidation-reduction and electron transport reactions occurring in mitochondria via conversion of superoxide anion (O2–·) into H2O2. Measurement of hydroethidine oxidation showed a significant increase in O2−·levels in the patient’s skin fibroblasts, as compared with controls, and this was paralleled by reduced catalytic activity of SOD2 in patient fibroblasts and muscle. Lentiviral complementation experiments demonstrated that mitochondrial SOD2 activity could be completely restored on transduction with wild type SOD2.ConclusionOur results provide evidence that defective SOD2 may lead to toxic increases in the levels of damaging oxygen radicals in the neonatal heart, which can result in rapidly developing heart failure and death. We propose SOD2 as a novel nuclear-encoded mitochondrial protein involved in severe human neonatal cardiomyopathy, thus expanding the wide range of genetic factors involved in paediatric cardiomyopathies.

Published

2020

13. Predicting arrhythmic risk in arrhythmogenic right ventricular cardiomyopathy: A systematic review and meta-analysis.

Author

Bosman, Laurens P., Sammani, Arjan, James, Cynthia A., Cadrin-Tourigny, Julia, Calkins, Hugh, van Tintelen, J. Peter, Hauer, Richard N.W., Asselbergs, Folkert W., te Riele, Anneline S.J.M., and teRiele, Anneline S J M

Abstract

While many studies evaluate predictors of ventricular arrhythmias in arrhythmogenic right ventricular cardiomyopathy (ARVC), a systematic review consolidating this evidence is currently lacking. Therefore, we searched MEDLINE and Embase for studies analyzing predictors of ventricular arrhythmias (sustained ventricular tachycardia/fibrillation (VT/VF), appropriate implantable cardioverter-defibrillator therapy, or sudden cardiac death) in patients with definite ARVC, patients with borderline ARVC, and ARVC-associated mutation carriers. In the case of multiple publications on the same cohort, the study with the largest population was included. This yielded 45 studies with a median cohort size of 70 patients (interquartile range 60 patients) and a median follow-up of 5.0 years (interquartile range 3.3 - 6.7 years). The average proportion of arrhythmic events observed was 10.6%/y in patients with definite ARVC, 10.0%/y in patients with borderline ARVC, and 3.7%/y with mutation carriers. Predictors of ventricular arrhythmias were population dependent: consistently predictive risk factors in patients with definite ARVC were male sex, syncope, T-wave inversion in lead >V3, right ventricular dysfunction, and prior (non)sustained VT/VF; in patients with borderline ARVC, 2 additional predictors-inducibility during electrophysiology study and strenuous exercise-were identified; and with mutation carriers, all aforementioned predictors as well as ventricular ectopy, multiple ARVC-related pathogenic mutations, left ventricular dysfunction, and palpitations/presyncope determined arrhythmic risk. Most evidence originated from small observational cohort studies, with a moderate quality of evidence. In conclusion, the average risk of ventricular arrhythmia ranged from 3.7 to 10.6%/y depending on the population with ARVC. Male sex, syncope, T-wave inversion in lead >V3, right ventricular dysfunction, and prior (non)sustained VT/VF consistently predict ventricular arrhythmias in all populations with ARVC. [ABSTRACT FROM AUTHOR]

Published

2018

14. Informing relatives at risk of inherited cardiac conditions: experiences and attitudes of healthcare professionals and counselees

Author

van den Heuvel, Lieke M., Huisinga, Mette J., Hoedemaekers, Yvonne M., Baas, Annette F., Plantinga, Mirjam, Henneman, Lidewij, van Tintelen, J. Peter, Smets, Ellen M. A., and Christiaans, Imke

Abstract

Inherited cardiac conditions (ICCs) can lead to sudden cardiac death at young age, even without previous symptoms, yet often remain undetected. To prevent sudden cardiac death, cardiac monitoring and/or predictive DNA testing is advised for at-risk relatives. Probands in whom a causal variant is detected are asked to inform their relatives about the possibility of testing, often supported by a family letter. This qualitative study investigates experiences with and attitudes toward this family-mediated approach in ICCs and explores whether and how improvements can be made. Two online focus groups were conducted with 28 healthcare professionals (HCPs) from various disciplines, as were 25 face-to-face semi-structured interviews with counselees (10 probands; 15 relatives). Data were analysed by two researchers independently using a thematic approach. Participants, both HCPs and counselees, preferred that probands inform relatives about genetic risks in ICCs, but both groups struggled with the dependency on and burden on probands to inform their relatives. To overcome this, HCPs do see a more active role for themselves in informing relatives, but prefer uniformity in procedures in order to maintain their workload. Counselees, on the other hand, prefer a tailored information provision strategy adjusted to family dynamics and the personality characteristics of relatives. In conclusion, although it is generally preferred that probands inform relatives themselves, a more active role of HCPs could be considered to overcome the dependency and burden on probands. Further research is needed to study how HCPs can engage more actively in informing at-risk relatives in current clinical genetic practise.

Published

2019

15. Large Genomic Rearrangements of Desmosomal Genes in Italian Arrhythmogenic Cardiomyopathy Patients.

Author

Pilichou, Kalliopi, Lazzarini, Elisabetta, Rigato, Ilaria, Celeghin, Rudy, De Bortoli, Marzia, Perazzolo Marra, Marina, Cason, Marco, Jongbloed, Jan, Calore, Martina, Rizzo, Stefania, Regazzo, Daniela, Poloni, Giulia, Iliceto, Sabino, Daliento, Luciano, Delise, Pietro, Corrado, Domenico, Van Tintelen, J. Peter, Thiene, Gaetano, Rampazzo, Alessandra, and Basso, Cristina

Abstract

Background: Arrhythmogenic cardiomyopathy (AC) is an inherited heart muscle disease associated with point mutations in genes encoding for cardiac desmosome proteins. Conventional mutation screening is positive in ≈50% of probands. Copy number variations (CNVs) have recently been linked to AC pointing to the need to determine the prevalence of CNVs in desmosomal genes and to evaluate disease penetrance by cosegregation analysis in family members.Methods and Results: A total of 160 AC genotype-negative probands for 5 AC desmosomal genes by conventional mutation screening underwent multiplex ligation-dependent probe amplification. Nine heterozygous CNVs were identified in 11 (6.9%) of the 160 probands. Five carried a deletion of the entire plakophilin-2 (PKP2) gene, 2 a deletion of only PKP2 exon 4, 1 a deletion of the PKP2 exons 6 to 11, 1 a PKP2 duplication of 5' untranslated region till exon 1, 1 the desmocollin-2 (DSC2) duplication of exons 7 to 9, and 1 a large deletion of chromosome 18 comprising both DSC2 and desmoglein-2 genes. All probands were affected by moderate-severe forms of the disease, whereas 10 (32%) of the 31 family members carrying one of these deletions fulfilled the diagnostic criteria.Conclusions: Genomic rearrangements were detected in ≈7% of AC probands negative for pathogenic point mutations in desmosomal genes, highlighting the potential of CNVs analysis to substantially increase the diagnostic yield of genetic testing. Genotype-phenotype correlation demonstrated the presence of the disease in about one third of family members carrying the CNV, underlying the role of other factors in the development and progression of the disease. [ABSTRACT FROM AUTHOR]

Published

2017

16. Burden of Recurrent and Ancestral Mutations in Families With Hypertrophic Cardiomyopathy.

Author

Barratt Ross, Samantha, Bagnall, Richard D., Ingles, Jodie, Van Tintelen, J. Peter, and Semsarian, Christopher

Abstract

Background—Hypertrophic cardiomyopathy is a genetically heterogeneous myocardial disease with >1000 causal variants identified. Nonunique variants account for disease in many families. We sought to characterize nonunique variants in Australian families and determine whether they arise from common ancestral mutations or recurrent mutation events. Methods and Results—Genetic test results of 467 index patients from apparently unrelated families with hypertrophic cardiomyopathy were evaluated. Causal variants were found in 185 of 467 (40%) families. Nonunique variants accounted for 122 of 185 (66%) families. The most common single genetic cause of hypertrophic cardiomyopathy is the recurrent MYBPC3 (myosin-binding protein-C) variant c.1504C>T, p.Arg502Trp, which was found in 13 of 185 (7%) families with a causal variant identified. Thirteen variants in MYBPC3 and MYH7 (myosin heavy chain 7) were each identified >3 times and accounted for 78 of 185 (42%) hypertrophic cardiomyopathy families with a causal variant. Haplotype analysis of these 13 variants was performed on 126 individuals from 70 Australian families, and 11 variants arose through recurrent mutation events. Two variants, MYBPC3 c.1928-2A>G and MYH7 c.2681A>G, p.Glu894Gly, were found on 1 haplotype in 6 families each, supportive of a single mutation event inherited from a common ancestor. Conclusions—The majority of families with a causal variant identified have a nonunique variant. Discovery of the genetic origins of human disease forms a fundamental basis for improved understanding of disease pathogenesis and phenotype development. [ABSTRACT FROM AUTHOR]

Published

2017

17. Cardiac phenotype and long-term prognosis of arrhythmogenic right ventricular cardiomyopathy/dysplasia patients with late presentation.

Author

Bhonsale, Aditya, te Riele, Anneline S.J.M., Sawant, Abhishek C., Groeneweg, Judith A., James, Cynthia A., Murray, Brittney, Tichnell, Crystal, Mast, Thomas P., van der Pols, Michelle J., Cramer, Maarten J.M., Dooijes, Dennis, van der Heijden, Jeroen F., Tandri, Harikrishna, van Tintelen, J. Peter, Judge, Daniel P., Hauer, Richard N.W., and Calkins, Hugh

Abstract

Background: The clinical profile of arrhythmogenic right ventricular cardiomyopathy/dysplasia (ARVC/D) patients with late presentation is unknown.Objective: The purpose of this study was to characterize the genotype, cardiac phenotype, and long-term outcomes of ARVC/D patients with late presentation (age ≥50 years at diagnosis).Methods: Five hundred two patients with an ARVC/D diagnosis from Johns Hopkins and Utrecht Registries were studied and long-term clinical outcomes ascertained.Results: Late presentation was seen in 104 patients (21%; 38% PKP2 carriers); 3% were ≥65 years at diagnosis. Sustained ventricular tachycardia was the major (43%) mode of presentation in patients with late presentation, whereas cardiac syncope was infrequent (P <.001). Those with late presentation were significantly less likely to harbor a known pathogenic mutation (53%; P = .005), have less precordial T-wave repolarization changes (P <.001), and have lower ventricular ectopy burden (P = .026). Over median 6-year follow-up, 68 patients with late presentation (65%) experienced sustained ventricular arrhythmias, with similar arrhythmia-free survival at 5-year follow up (P = .48). Left ventricular dysfunction and heart failure were seen in 24 (32%) and 15 patients (14%), respectively, without need for cardiac transplantation. In the late presentation cohort, male sex, pathogenic mutation, right ventricular structural disease, lack of family history, and electrophysiologic study inducibility were associated with increased arrhythmic risk.Conclusion: One-fifth of all ARVC/D patients present after age 50 years, often with sustained ventricular tachycardia, and are less likely to have prior syncope, ECG changes, ventricular ectopy, or identifiable pathogenic mutation. In ARVC/D, late presentation does not confer a benign prognosis and is associated with high arrhythmic risk. [ABSTRACT FROM AUTHOR]

Published

2017

18. Influence of Panel Selection on Yield of Clinically Useful Variants in Arrhythmogenic Right Ventricular Cardiomyopathy Families

Author

Murray, Brittney, Tichnell, Crystal, Tandri, Harikrishna, Calkins, Hugh, van Tintelen, J. Peter, Judge, Daniel P., and James, Cynthia A.

Published

2020

19. Adaptation and validation of the ACMG/AMP variant classification framework for MYH7-associated inherited cardiomyopathies: recommendations by ClinGen’s Inherited Cardiomyopathy Expert Panel

Author

Kelly, Melissa A, Caleshu, Colleen, Morales, Ana, Buchan, Jillian, Wolf, Zena, Harrison, Steven M, Cook, Stuart, Dillon, Mitchell W, Garcia, John, Haverfield, Eden, Jongbloed, Jan D H, Macaya, Daniela, Manrai, Arjun, Orland, Kate, Richard, Gabriele, Spoonamore, Katherine, Thomas, Matthew, Thomson, Kate, Vincent, Lisa M, Walsh, Roddy, Watkins, Hugh, Whiffin, Nicola, Ingles, Jodie, van Tintelen, J Peter, Semsarian, Christopher, Ware, James S, Hershberger, Ray, and Funke, Birgit

Abstract

PurposeIntegrating genomic sequencing in clinical care requires standardization of variant interpretation practices. The Clinical Genome Resource has established expert panels to adapt the American College of Medical Genetics and Genomics/Association for Molecular Pathology classification framework for specific genes and diseases. The Cardiomyopathy Expert Panel selected MYH7, a key contributor to inherited cardiomyopathies, as a pilot gene to develop a broadly applicable approach.MethodsExpert revisions were tested with 60 variants using a structured double review by pairs of clinical and diagnostic laboratory experts. Final consensus rules were established via iterative discussions.ResultsAdjustments represented disease-/gene-informed specifications (12) or strength adjustments of existing rules (5). Nine rules were deemed not applicable. Key specifications included quantitative frameworks for minor allele frequency thresholds, the use of segregation data, and a semiquantitative approach to counting multiple independent variant occurrences where fully controlled case-control studies are lacking. Initial inter-expert classification concordance was 93%. Internal data from participating diagnostic laboratories changed the classification of 20% of the variants (n = 12), highlighting the critical importance of data sharing.ConclusionThese adapted rules provide increased specificity for use in MYH7-associated disorders in combination with expert review and clinical judgment and serve as a stepping stone for genes and disorders with similar genetic and clinical characteristics.

Published

2018

20. QRS prolongation after premature stimulation is associated with polymorphic ventricular tachycardia in nonischemic cardiomyopathy: Results from the Leiden Nonischemic Cardiomyopathy Study.

Author

Piers, Sebastiaan R.D., Askar, Saïd F.A., Venlet, Jeroen, Androulakis, Alexander F.A.A., Kapel, Gijsbert F.L., de Riva Silva, Marta, Jongbloed, Jan J.D.H., van Tintelen, J. Peter, Schalij, Martin J., Pijnappels, Daniël A., and Zeppenfeld, Katja

Abstract

Background: Progressive activation delay after premature stimulation has been associated with ventricular fibrillation in nonischemic cardiomyopathy (NICM).Objectives: The objectives of this study were (1) to investigate prolongation of the paced QRS duration (QRSd) after premature stimulation as a marker of activation delay in NICM, (2) to assess its relation to induced ventricular arrhythmias, and (3) to analyze its underlying substrate by late gadolinium enhancement cardiac magnetic resonance imaging (LGE-CMR) and endomyocardial biopsy.Methods: Patients with NICM were prospectively enrolled in the Leiden Nonischemic Cardiomyopathy Study and underwent a comprehensive evaluation including LGE-CMR, electrophysiology study, and endomyocardial biopsy. Patients without structural heart disease served as controls for electrophysiology study.Results: Forty patients with NICM were included (mean age 57 ± 14 years; 33 men [83%]; left ventricular ejection fraction 30% ± 13%). After the 400-ms drive train and progressively premature stimulation, the maximum increase in QRSd was larger in patients with NICM than in controls (35 ± 18 ms vs. 23 ± 12 ms; P = .005) and the coupling interval window with QRSd prolongation was wider (47 ± 23 ms vs. 31 ± 14 ms; P = .005). The maximum paced QRSd exceeded the ventricular effective refractory period, allowing for pacing before the offset of the QRS complex in 20 of 39 patients with NICM vs. 1 of 20 controls (P < .001). In patients with NICM, QRSd prolongation was associated with the inducibility of polymorphic ventricular tachycardia (16 of 39 patients) and was related to long, thick strands of fibrosis in biopsies, but not to focal enhancement on LGE-CMR.Conclusion: QRSd is a simple parameter used to quantify activation delay after premature stimulation, and its prolongation is associated with the inducibility of polymorphic ventricular tachycardia and with the pattern of myocardial fibrosis in biopsies. [ABSTRACT FROM AUTHOR]

Published

2016

21. Follow-up care by a genetic counsellor for relatives at risk for cardiomyopathies is cost-saving and well-appreciated: a randomised comparison

Author

Nieuwhof, Karin, Birnie, Erwin, van den Berg, Maarten P, de Boer, Rudolf A, van Haelst, Paul L, van Tintelen, J Peter, and van Langen, Irene M

Abstract

Increasing numbers of patient relatives at risk of developing dilated or hypertrophic cardiomyopathy (DCM/HCM) are being identified and followed up by cardiologists according to the ACC/ESC guidelines. However, given limited healthcare resources, good-quality low-cost alternative approaches are needed. Therefore, we have compared conventional follow-up by a cardiologist with that provided at a cardiogenetic clinic (CGC) led by a genetic counsellor. Phenotype-negative first-degree relatives at risk for DCM/HCM were randomly assigned to see either a cardiologist or to attend a CGC. Uptake and resource use were recorded. For 189 participants, we evaluated quality of care experienced, patient satisfaction and perceived personal control (PPC) using validated questionnaires and estimated the average cost difference of these two modes of care. Maximum patient satisfaction scores were achieved more frequently at the CGC (86% vs 45%, P<0.01). In terms of follow-up care provided, the genetic counsellor did not perform worse than the cardiologist (95% vs 59%, P<0.01). The genetic counsellor more often enquired about the relative-at risk’s health (100% vs 65%, P<0.01) and family health (97% vs 33%, P<0.01), measured blood pressure (98% vs 29%, P<0.01) and gave disease-specific information (77% vs 52%, P<0.01). Although PPC scores were equal in both groups, the average cost per patient of CGC follow-up was 25% lower. Follow-up of phenotype-negative relatives at risk for DCM/HCM at a CGC led to greater patient satisfaction and is well-appreciated at lower cost. CGC care is a good alternative to conventional cardiological follow-up for this growing group of patients.

Published

2017

22. B-PO04-170 SEX DIFFERENCES IN PATIENTS WITH ARRHYTHMOGENIC CARDIOMYOPATHY WITH RESPECT TO VENTRICULAR TACHYCARDIA MORPHOLOGY.

Author

Laredo, Mikael, Belhassen, Bernard, Roudijk, Rob, Peretto, Giovanni, Zahavi, Guy, Sen-Chowdhry, Srijita, Badenco, Nicolas, te Riele, Anneline S.J., Sala, Simone, Duthoit, Guillaume, van Tintelen, J. Peter, Sellal, Jean-Marc, Gasperetti, Alessio, Arbelo, Elena, Andorin, Antoine, Ninni, Sandro, Rollin, Anne, Peichl, Petr, Waintraub, Xavier, and Bosman, Laurens P.

Published

2021

23. Evaluation of Genes Encoding for the Transient Outward Current (Ito) Identifies the KCND2 Gene as a Cause of J-Wave Syndrome Associated With Sudden Cardiac Death.

Author

Perrin, Mark J., Adler, Arnon, Green, Sharon, Al-Zoughool, Foad, Doroshenko, Petro, Orr, Nathan, Uppal, Shaheen, Healey, Jeff S., Birnie, David, Sanatani, Shubhayan, Gardner, Martin, Champagne, Jean, Simpson, Chris, Ahmad, Kamran, van den Berg, Maarten P., Chauhan, Vijay, Backx, Peter H., van Tintelen, J. Peter, Krahn, Andrew D., and Gollob, Michael H.

Subjects

GENETIC code, CARDIAC arrest, POTASSIUM channels, MUTAGENESIS, PATIENTS

Abstract

The article presents a study that investigates and determines the genetic mutation frequency of the gene encoding of the transient outward current (Ito) of patients who died of sudden cardiac arrest in Canada. Researchers carried out different types of tests, including mutation analysis, mutagenesis and cloning, of 51 patients who had J-wave syndrome. Moreover, they found that the potassium voltage-gated channel (KCND2) gene is the prime cause of the J-wave syndrome and death of patients.

Published

2014

24. Functional assessment of potential splice site variants in arrhythmogenic right ventricular dysplasia/cardiomyopathy.

Author

Groeneweg, Judith A., Ummels, Amber, Mulder, Marcel, Bikker, Hennie, van der Smagt, Jasper J., van Mil, Anneke M., Homfray, Tessa, Post, Jan G., Elvan, Arif, van der Heijden, Jeroen F., Houweling, Arjan C., Jongbloed, Jan D.H., Wilde, Arthur A.M., van Tintelen, J. Peter, Hauer, Richard N., and Dooijes, Dennis

Abstract

Background Interpretation of genetic screening results in arrhythmogenic right ventricular dysplasia/cardiomyopathy (ARVD/C) often is difficult. Pathogenicity of variants with uncertain clinical significance may be predicted by software algorithms. However, functional assessment can unambiguously demonstrate the effect of such variants. Objective The purpose of this study was to perform functional analysis of potential splice site variants in ARVD/C patients. Methods Nine variants in desmosomal ( PKP2 , JUP , DSG2 , DSC2 ) genes with potential RNA splicing effect were analyzed. The variants were found in patients who fulfilled 2010 ARVD/C Task Force Criteria (n = 7) or had suspected ARVD/C (n = 2). Total RNA was isolated from fresh blood samples and subjected to reverse transcriptase polymerase chain reaction. Results An effect on splicing was predicted by software algorithms for all variants. Of the 9 variants, 5 were intronic and 4 exonic. RNA analysis showed a functional effect on mRNA splicing by exon skipping, generation of new splice sites, or activation of cryptic sites in 6 variants. All 5 intronic variants tested severely impaired splicing. Only 1 of 4 exonic potential splice site variants was shown to have a deleterious effect on splicing. The remaining 3 exonic variants had no detectable effect on splicing, and heterozygous presence in mRNA confirmed biallelic expression. Conclusion Six variants of uncertain clinical significance in the PKP2 , JUP , and DSG2 genes showed a deleterious effect on mRNA splicing, indicating these are ARVD/C–related pathogenic splice site mutations. These results highlight the importance of functional assessment of potential splice site variants to improve patient care and facilitate cascade screening. [ABSTRACT FROM AUTHOR]

Published

2014

25. Outcome in Phospholamban R14del Carriers.

Author

van Rijsingen, Ingrid A.W., van der Zwaag, Paul A., Groeneweg, Judith A., Nannenberg, Eline A., Jongbloed, Jan D.H., Zwinderman, Aeilko H., Pinto, Yigal M., dit Deprez, Ronald H. Lekanne, Post, Jan G., Tan, Hanno L., de Boer, Rudolf A., Hauer, Richard N.W., Christiaans, Imke, van den Berg, Maarten P., van Tintelen, J. Peter, and Wilde, Arthur A.M.

Abstract

The pathogenic phospholamban R14del mutation causes dilated and arrhythmogenic right ventricular cardiomyopathies and is associated with an increased risk of malignant ventricular arrhythmias and end-stage heart failure. We performed a multicentre study to evaluate mortality, cardiac disease outcome, and risk factors for malignant ventricular arrhythmias in a cohort of phospholamban R14del mutation carriers.Using the family tree mortality ratio method in a cohort of 403 phospholamban R14del mutation carriers, we found a standardized mortality ratio of 1.7 (95% confidence interval, 1.4-2.0) with significant excess mortality starting from the age of 25 years. Cardiological data were available for 295 carriers. In a median follow-up period of 42 months, 55 (19%) individuals had a first episode of malignant ventricular arrhythmias and 33 (11%) had an end-stage heart failure event. The youngest age at which a malignant ventricular arrhythmia occurred was 20 years, whereas for an end-stage heart failure event this was 31 years. Independent risk factors for malignant ventricular arrhythmias were left ventricular ejection fraction <45% and sustained or nonsustained ventricular tachycardia with hazard ratios of 4.0 (95% confidence interval, 1.9-8.1) and 2.6 (95% confidence interval, 1.5-4.5), respectively.Phospholamban R14del mutation carriers are at high risk for malignant ventricular arrhythmias and end-stage heart failure, with left ventricular ejection fraction <45% and sustained or nonsustained ventricular tachycardia as independent risk factors. High mortality and a poor prognosis are present from late adolescence. Genetic and cardiac screening is, therefore, advised from adolescence onwards. [ABSTRACT FROM AUTHOR]

Published

2014

26. Generation of human induced pluripotent stem cell (iPSC) lines derived from five patients carrying the pathogenic phospholamban-R14del (PLN-R14del) variant and three non-carrier family members.

Author

Mittal, Nishka, Dave, Jaydev, Harakalova, Magdalena, van Tintelen, J. Peter., Asselbergs, Folkert W., Doevendans, Pieter A., Costa, Kevin D., Turnbull, Irene C., and Stillitano, Francesca

Abstract

The R14del pathogenic variant in the phospholamban (PLN) gene (PLN-R14del), has been identified in families with hereditary cardiomyopathy, including dilated and arrhythmogenic cardiomyopathies. Here we have generated human iPSC lines from five PLN-R14del carriers and three non-carrier family members. Peripheral blood mononuclear cells (PBMC) were obtained from the eight individuals and reprogrammed using Sendai viral vector system carrying the Yamanaka factors. All eight lines show typical iPSC morphology, normal karyotype, high expression of pluripotency markers, and possess the ability to differentiate into all three germ layers. These lines represent valuable resources for studying the pathophysiological mechanisms of PLN-R14del associated cardiomyopathy. [ABSTRACT FROM AUTHOR]

Published

2022

27. Arrhythmogenic Right Ventricular Dysplasia/Cardiomyopathy in the Pediatric Population

Author

te Riele, Anneline S.J.M., James, Cynthia A., Sawant, Abhishek C., Bhonsale, Aditya, Groeneweg, Judith A., Mast, Thomas P., Murray, Brittney, Tichnell, Crystal, Dooijes, Dennis, van Tintelen, J. Peter, Judge, Daniel P., van der Heijden, Jeroen F., Crosson, Jane, Hauer, Richard N.W., Calkins, Hugh, and Tandri, Harikrishna

Abstract

The aims of this study were to determine the clinical characteristics and outcomes of pediatric-onset arrhythmogenic right ventricular dysplasia/cardiomyopathy (ARVD/C) and to compare these with those of adult-onset ARVD/C.

Published

2015

28. Clinical Presentation, Long-Term Follow-Up, and Outcomes of 1001 Arrhythmogenic Right Ventricular Dysplasia/Cardiomyopathy Patients and Family Members

Author

Groeneweg, Judith A., Bhonsale, Aditya, James, Cynthia A., te Riele, Anneline S., Dooijes, Dennis, Tichnell, Crystal, Murray, Brittney, Wiesfeld, Ans C.P., Sawant, Abhishek C., Kassamali, Bina, Atsma, Douwe E., Volders, Paul G., de Groot, Natasja M., de Boer, Karin, Zimmerman, Stefan L., Kamel, Ihab R., van der Heijden, Jeroen F., Russell, Stuart D., Jan Cramer, Maarten, Tedford, Ryan J., Doevendans, Pieter A., van Veen, Toon A., Tandri, Harikrishna, Wilde, Arthur A., Judge, Daniel P., van Tintelen, J. Peter, Hauer, Richard N., and Calkins, Hugh

Abstract

Supplemental Digital Content is available in the text.

Published

2015

29. Left-dominant arrhythmogenic cardiomyopathy in a large family: Associated desmosomal or nondesmosomal genotype?

Author

Groeneweg, Judith A., van der Zwaag, Paul A., Jongbloed, Jan D.H., Cox, Moniek G.P.J., Vreeker, Arnold, de Boer, Rudolf A., van der Heijden, Jeroen F., van Veen, Toon A.B., McKenna, William J., van Tintelen, J. Peter, Dooijes, Dennis, and Hauer, Richard N.W.

Abstract

Background: Arrhythmogenic cardiomyopathy (AC) is considered a predominantly right ventricular (RV) desmosomal disease. However, left-dominant forms due to desmosomal gene mutations, including PKP2 variant c.419C>T, have been described. Recently, a nondesmosomal phospholamban (PLN) mutation (c.40_42delAGA) has been identified, causing dilated cardiomyopathy and arrhythmias. Objective: To gain more insight into pathogenicity of the PKP2 variant c.419C>T by cosegregation analysis of the PKP2 variant c.419C>T vs the PLN mutation c.40_42delAGA. Methods: A Dutch family (13 family members, median age 49 years, range 34–71 years) with ventricular tachycardia underwent (1) meticulous phenotypic characterization and (2) screening of 5 desmosomal genes (PKP2, DSC2, DSG2, DSP, JUP) and PLN. Results: Six family members fulfilled 2010 AC Task Force Criteria. Seven had signs of left ventricular (LV) involvement (inverted T waves in leads V4–V6, LV wall motion abnormalities and late enhancement, and reduced LV ejection fraction), including 6 family members with proven AC. The PKP2 variant c.419C>T was found as a single variant in 3 family members, combined with the PLN mutation c.40_42delAGA in 3 others. PLN mutation was found in 9 family members, including the 6 with AC and all 7 with LV involvement. The PLN mutation c.40_42delAGA was found as a single mutation in 6, combined with the PKP2 variant c.419C>T in 3 others. A low-voltage electrocardiogram was seen in 4 of 9 PLN mutation-positive subjects. None of the family members with the single PKP2 variant showed any sign of RV or LV involvement. Conclusions: The PLN mutation c.40_42delAGA cosegregates with AC and with electrocardiographic and structural LV abnormalities. In this family, there was no evidence of disease-causing contribution of the PKP2 variant c.419C>T. [ABSTRACT FROM AUTHOR]

Published

2013

30. Familial Evaluation in Catecholaminergic Polymorphic Ventricular Tachycardia.

Author

van der Werf, Christian, Nederend, Ineke, Hofman, Nynke, van Geloven, Nan, Ebink, Cornd, Frohn-Mulder, Ingrid M. E., Alings, A. Marco W., Bosker, Hans A., Bracke, Frank A., den Heuvel, Freek van, Waalewijn, Reinier A., Bikker, Hennie, van Tintelen, J. Peter, Bhuiyan, Zahurul A., den Berg, Maarten P. van, and Wilde, Arthur A. M.

Subjects

COHORT analysis, RYANODINE receptors, HEART disease genetics, VENTRICULAR tachycardia, HEART disease prognosis, CARDIOVASCULAR diseases

Abstract

The article discusses a study which evaluated a cohort of 116 relatives carrying the cardiac ryanodine receptor gene (RYR2) mutation which causes catecholaminergic polymorphic ventricular tachycardia (CPVT). The clinical and electrocardiographic variables of disease penetrance and expression, genotype-phenotype correlations, and prognosis are explored. Results showed a marked phenotypic diversity among the relatives and most of them lack signs of supraventricular disease manifestations.

Published

2012

31. Desmin mutations as a cause of right ventricular heart failure affect the intercalated disks.

Author

Otten, Ellen, Asimaki, Angeliki, Maass, Alexander, van Langen, Irene M., van der Wal, Allard, de Jonge, Nicolaas, van den Berg, Maarten P., Saffitz, Jeffrey E., Wilde, Arthur A.M., Jongbloed, Jan D.H., and van Tintelen, J. Peter

Abstract

Background: Mutations in the gene encoding desmin (DES), an intermediate filament protein, underlie a heterogeneous phenotype, which is referred to as desmin-related myopathy (DRM). Right ventricular involvement including an arrhythmogenic right ventricular cardiomyopathy (ARVC)(-like) phenotype has occasionally been described in DES mutation-carrying patients. Objective: To determine the effects of a DES missense mutation on the structure of different intercalated disk proteins, to evaluate right ventricular involvement in DES mutation carriers, and to establish the role of DES mutations in ARVC(-like) phenotypes. Methods: We evaluated the clinical phenotype in two families carrying two different DES mutations. One family was diagnosed with DRM, with an ARVC(-like) phenotype in one patient, while the other family presented with a severe biventricular cardiomyopathy. Additional immunohistochemistry of desmosomal proteins was performed in myocardial tissue from two patients of the last family. The DES gene was screened for mutations in 50 ARVC(-like) patients. Results: Except for two different DES mutations (p.N342D and p.R454W) in two families with DRM and severe biventricular cardiomyopathy, respectively, we did not find additional DES mutations in ARVC(-like) patients. In addition to desmin aggregates, immunohistochemistry demonstrated a decreased amount of desmoplakin and plakophilin-2 at the intercalated disk in p.R454W mutation carriers. Conclusions: We confirmed that either an ARVC-like phenotype or a severe cardiomyopathy with right ventricular involvement are possible, yet infrequent, cardiac phenotypes in DRM. Moreover, we demonstrated that the DES mutation p.R454W affects the localization of desmoplakin and plakophilin-2 at the intercalated disk, suggesting a link between desmosomal cardiomyopathies (mainly affecting the right ventricle) and cardiomyopathies caused by DES mutations. [Copyright &y& Elsevier]

Published

2010

32. Arrhythmogenic Right Ventricular Dysplasia/Cardiomyopathy Diagnostic Task Force Criteria.

Author

Cox, Moniek G. P. J., Van Der Smagt, Jasper J., Noorman, Maartje, Wiesfeld, Arts C., Volders, Paul G. A., Van Langen, Irene M., Atsma, Douwe E., Dooijes, Dennis, Houweling, Arjan C., Loh, Peter, Jordaens, Luc, Arens, Yvonne, Cramer, Maarten J., Doevendans, Pieter A., Van Tintelen, J. Peter, Wilde, Arthur A. M., and Hauer, Richard N. W.

Subjects

DYSPLASIA, CARDIOMYOPATHIES, VENTRICULAR tachycardia, MEDICAL genetics, BUNDLE-branch block, DIAGNOSIS

Abstract

The article focuses on a study which compared arrhythmogenic right ventricular dysplasia/cardiomyopathy (ARVD/C) Diagnostic Task Force Criteria (TFC) in 1994 and a new proposed criteria. The newly proposed criteria contains terminal activation duration of QRS, ventricular tachycardia with left bundle-branch block morphology and superior axis and genetic criteria. Study authors concluded that the new TFC affects the increasing diagnostic yield of ARVD/C.

Published

2010

33. Severe cardiac phenotype with right ventricular predominance in a large cohort of patients with a single missense mutation in the DES gene.

Author

van Tintelen, J. Peter, Van Gelder, Isabelle C., Asimaki, Angeliki, Suurmeijer, Albert J.H., Wiesfeld, Ans C.P., Jongbloed, Jan D.H., van den Wijngaard, Arthur, Kuks, Jan B.M., van Spaendonck-Zwarts, Karin Y., Notermans, Nicolette, Boven, Ludolf, van den Heuvel, Freek, Veenstra-Knol, Hermine E., Saffitz, Jeffrey E., Hofstra, Robert M.W., and van den Berg, Maarten P.

Abstract

Background: Desmin-related myopathy is a clinically heterogenous group of disorders encompassing myopathies, cardiomyopathies, conduction disease, and combinations of these disorders. Mutations in the gene encoding desmin (DES), a major intermediate filament protein, can underlie this phenotype. Objective: The purpose of this study was to investigate the clinical and pathologic characteristics of 27 patients from five families with an identical mutation in the head domain region (p.S13F) of desmin. Methods/Results: All 27 carriers or obligate carriers of a p.S13F DES founder mutation demonstrated a fully penetrant yet variable phenotype. All patients demonstrated cardiac involvement characterized by high-grade AV block at young ages and important right ventricular (RV) involvement. RV predominance was demonstrated by the presence of right bundle branch block in 10 patients (sometimes as a first manifestation) and by RV heart failure in 6 patients, including 2 patients who fulfilled the diagnostic criteria for arrhythmogenic RV cardiomyopathy. Because of this clinical overlap with desmosome cardiomyopathies, we also studied the organization of the intercalated disks, particularly the distribution of desmosomal proteins. Normal amounts of the major desmosomal proteins were found, but the intercalated disks were more convoluted and elongated and had a zigzag appearance. Conclusion: In this largest series to date of individuals with a single head domain DES mutation, patients show a variable yet predominantly cardiologic phenotype characterized by conduction disease at an early age and RV involvement including right bundle branch block and/or RV tachycardias and arrhythmogenic RV cardiomyopathy phenocopies. A localized effect of desmin on the structure of the cardiac intercalated disks might contribute to disease pathogenesis. [Copyright &y& Elsevier]

Published

2009

34. Desmoglein-2 and Desmocollin-2 Mutations in Dutch Arrhythmogenic Right Ventricular Dysplasia/Cardiomypathy Patients.

Author

Bhuiyan, Zahurul A., Jongbloed, Jan D. H., Van der Smagt, Jasper, Lombardi, Paola M., Wiesfeld, Ans C. P., Nelen, Marcel, Schouten, Meyke, Jongbloed, Roselie, Cox, Moniek G. P. J., Van Wolferen, Marleen, Rodriguez, Luz M., Van Gelder, Isabelle C., Bikker, Hennie, Suurmeijer, Albert J. H., van den Berg, Maarten P., Mannens, Marcel M. A. M., Hauer, Richard N. W., Wilde, Arthur A. M., and van Tintelen, J. Peter

Subjects

DYSPLASIA, CELL transformation, CELLULAR pathology, FIBROCYSTIC breast disease, BRONCHOPULMONARY dysplasia, CARDIOMYOPATHIES

Abstract

The article discusses a study on Desmoglein-2 (DSG2) and Desmocollin-2 (DSC2) mutations in arrythmogenic right ventricular dysplasia/cardiomypathy (ARVD/C) patients in the Netherlands. ARVD/C is a disease characterized by progressive fibrofatty replacement of the right ventricular (RV) myocardium. The Task Force Criteria (TFC) was used to analyze the genes of 57 patients. Results show that DSG2 and DSC2 are less prevalent than PKP2 mutations.

Published

2009

35. New ECG Criteria in Arrhythmogenic Right Ventricular Dysplasia/Cardiomyopathy.

Author

Cox, Moniek G. P. J., van der Smagt, Jasper J., Wilde, Arthur A. M., Wiesfeld, Ans C. P., Atsma, Douwe E., Nelen, Marcel R., Rodriguez, Luz-Maria, Loh, Peter, Cramer, Maarten J., Doevendans, Pieter A., van Tintelen, J. Peter, de Bakker, Jacques M. T., and Hauer, Richard N. W.

Subjects

ELECTROCARDIOGRAPHY, VENTRICULAR tachycardia, MEDICAL imaging systems, CARDIOMYOPATHIES, DYSPLASIA, PATIENTS, DIAGNOSIS

Abstract

The article presents a research study about the diagnostic value of new electrocardiography (ECG) criteria on ventricular tachycardia (VT) and activation delay to enhance the identification of individuals with arrthythmogenic right ventricular dysplasia/cardiomyopathy (ARVD/C). The study showed that the recognition of individuals was improved through the addition of ECG criteria to current task force criteria (TFC) for ARVD/C. It notes that the result was independent of outcome of DNA analyses.

Published

2009

36. Identification and Functional Characterization of Cardiac Troponin I As a Novel Disease Gene in Autosomal Dominant Dilated Cardiomyopathy.

Author

Carballo, Sebastian, Robinson, Paul, Otway, Robyn, Fatkin, Diane, Jongbloed, Jan D. H., de Jonge, Nicolaas, Blair, Edward, Van Tintelen, J. Peter, Redwood, Charles, and Watkins, Hugh

Subjects

CARDIOMYOPATHIES, GENETIC mutation, EXONS (Genetics), NUCLEOTIDE sequence, HEMOGLOBIN polymorphisms, GENETICS

Abstract

The article presents a study which aims to examine the TNN13 as a candidate gene through the analysis of 96 probands with dilated cardiomyopathy (DCM). The researchers isolated genomic DNA and screened TNN13 exons using heteroduplex analysis. Accordingly, DNA sequencing was applied to exons with aberrant profiles, while the variants were assessed using the segregation analysis. The results have supported the discovery that TNN13 missense mutations can cause diseases that can lead to DCM.

Published

2009

37. Integrating Exercise Into Personalized Ventricular Arrhythmia Risk Prediction in Arrhythmogenic Right Ventricular Cardiomyopathy.

Author

Bosman, Laurens P., Wang, Weijia, Lie, Oyvind H., van Lint, Freyja H.M., Rootwelt-Norberg, Christine, Murray, Brittney MS, Tichnell, Crystal MGC, Cadrin-Tourigny, Julia, van Tintelen, J. Peter, Asselbergs, Folkert W., Calkins, Hugh, te Riele, Anneline S.J.M., Haugaa, Kristina H., James, Cynthia A., Lie, Øyvind H, Murray, Brittney, and Tichnell, Crystal

Subjects

ARRHYTHMIA diagnosis, RESEARCH, PREDICTIVE tests, TIME, RESEARCH methodology, SELF-evaluation, ARRHYTHMOGENIC right ventricular dysplasia, DISEASE incidence, RETROSPECTIVE studies, PROGNOSIS, EVALUATION research, RISK assessment, COMPARATIVE studies, EXERCISE, DECISION making, RESEARCH funding, ARRHYTHMIA, LONGITUDINAL method, HEALTH self-care

Abstract

Background: Exercise is associated with sustained ventricular arrhythmias (VA) in Arrhythmogenic Right Ventricular Cardiomyopathy (ARVC) but is not included in the ARVC risk calculator (arvcrisk.com). The objective of this study is to quantify the influence of exercise at diagnosis on incident VA risk and evaluate whether the risk calculator needs adjustment for exercise.Methods: We interviewed ARVC patients without sustained VA at diagnosis about their exercise history. The relationship between exercise dose 3 years preceding diagnosis (average METh/wk) and incident VA during follow-up was analyzed with time-to-event analysis. The incremental prognostic value of exercise to the risk calculator was evaluated by Cox models.Results: We included 176 patients (male, 43.2%; age, 37.6±16.1 years) from 3 ARVC centers, of whom 53 (30.1%) developed sustained VA during 5.4 (2.7-9.7) years of follow-up. Exercise at diagnosis showed a dose-dependent nonlinear relationship with VA, with no significant risk increase <15 to 30 METh/wk. Athlete status, using 3 definitions from literature (>18, >24, and >36 METh/wk), was significantly associated with VA (hazard ratios, 2.53-2.91) but was also correlated with risk factors currently in the risk calculator model. Thus, adding athlete status to the model did not change the C index of 0.77 (0.71-0.84) and showed no significant improvement (Akaike information criterion change, <2).Conclusions: Exercise at diagnosis was dose dependently associated with risk of sustained VA in ARVC patients but only above 15 to 30 METh/wk. Exercise does not appear to have incremental prognostic value over the risk calculator. The ARVC risk calculator can be used accurately in athletic patients without modification. [ABSTRACT FROM AUTHOR]

Published

2022

38. Familial disease with a risk of sudden death: A longitudinal study of the psychological consequences of predictive testing for long QT syndrome.

Author

Hendriks, Karin S.W.H., Hendriks, Margriet M.W.B., Birnie, Erwin, Grosfeld, Frans J.M., Wilde, Arthur A.M., van den Bout, Jan, Smets, Ellen M.A., van Tintelen, J. Peter, ten Kroode, Herman F.J., and van Langen, Irene M.

Abstract

Background: Since 1996, in the Netherlands, cardiac and molecular screening has been performed in families with the long QT syndrome, a potentially life-threatening but treatable cardiac arrhythmia syndrome. The psychological consequences of predictive cardiac and molecular screening in these families are relatively unknown. Objective: A psychological study was initiated to investigate the extent and course of distress caused by this new form of predictive genetic testing. Methods: We carried out a prospective study to assess the extent and course of disease-related anxiety and depression, caused by predictive genetic testing, in applicants and their partners from the time of first consultation until 18 months after the disclosure of the result of genetic testing. Results: Seventy-seven applicants and 57 partners were investigated for measures of distress in 3 assessments. Those individuals who received an uncertain electrocardiogram result seemed especially vulnerable for distress, at least in the short term. The distress levels in the whole group of applicants were largely restored within 18 months. However, the disease-related anxiety scores in carriers remained relatively increased at long term. As compared with partners of noncarriers, partners of mutation carriers had higher levels of disease-related anxiety at all 3 assessments. Conclusion: Predictive testing for long QT syndrome consisting of cardiologic testing followed by molecular testing leads to distress, especially in carriers with an uncertain electrocardiogram and their partners at first visit. These distress levels return to normal at long term. However, for carriers with an uncertain electrocardiogram, the incidence of clinically relevant distress was high, most probably also caused by the consequences of having the disease. [Copyright &y& Elsevier]

Published

2008

39. High yield of LMNA mutations in patients with dilated cardiomyopathy and/or conduction disease referred to cardiogenetics outpatient clinics.

Author

van Tintelen, J. Peter, Hofstra, Robert M.W., Katerberg, Hilga, Rossenbacker, Tom, Wiesfeld, Ans C.P., du Marchie Sarvaas, Gideon J., Wilde, Arthur A.M., van Langen, Irene M., Nannenberg, Eline A., van der Kooi, Anneke J., Kraak, Marian, van Gelder, Isabelle C., van Veldhuisen, Dirk Jan, Vos, Yvonne, and van den Berg, Maarten P.

Subjects

CARDIOMYOPATHIES, GENETIC mutation, PATIENTS, GENETIC engineering

Abstract

Background: Among the most frequently encountered mutations in dilated cardiomyopathy (DCM) are those in the lamin A/C (LMNA) gene. Our goal was to analyze the LMNA gene in patients with DCM and/or conduction disease referred to the cardiogenetics outpatient clinic and to evaluate the prevalence of LMNA mutations and their clinical expression. Methods and Results: The LMNA gene was screened in 61 index patients. Eleven mutations (including 6 novel) were identified, mainly in the subgroup of familial DCM with cardiac conduction disease (3/10 index patients) and in patients with DCM and Emery-Dreifuss, Limb-Girdle, or unclassified forms of muscular dystrophy (7/8 index patients). In addition, a mutation was identified in 1 of 4 families with only cardiac conduction disease. We did not identify any large deletions or duplications. Genotype-phenotype relationships revealed a high rate of sudden death and cardiac transplants in carriers of the p.N195K mutation. Our study confirmed that the p.R225X mutation leads to cardiac conduction disease with late or no development of DCM, underscoring the importance of this mutation in putative familial “lone conduction disease.” Nearly one third of LMNA mutation carriers had experienced a thromboembolic event. Conclusions: This study highlights the role of LMNA mutations in DCM and related disorders. A severe phenotype in p.N195K mutation carriers and preferential cardiac conduction disease in p.R225X carriers was encountered. Because of the clinical variability, including the development of associated symptoms in time, LMNA screening should be considered in patients with DCM or familial lone conduction disease. [Copyright &y& Elsevier]

Published

2007

40. A family with Andersen-Tawil syndrome and dilated cardiomyopathy.

Author

Schoonderwoerd, Bas A., Wiesfeld, Ans C.P., Wilde, Arthur A.M., van den Heuvel, Freek, Van Tintelen, J. Peter, van den Berg, Maarten P., Van Veldhuisen, Dirk J., and Van Gelder, Isabelle C.

Subjects

AMBULATORY electrocardiography, BIOPSY, DISEASE susceptibility, GENEALOGY, GENETIC techniques, HEART ventricles, HEART beat, GENETIC mutation, POTASSIUM, ANDERSEN syndrome, DILATED cardiomyopathy, DISEASE complications

Published

2006

41. Evaluation of Genes Encoding for the Transient Outward Current (Ito) Identifies the KCND2Gene as a Cause of J-Wave Syndrome Associated With Sudden Cardiac Death

Author

Perrin, Mark J., Adler, Arnon, Green, Sharon, Al-Zoughool, Foad, Doroshenko, Petro, Orr, Nathan, Uppal, Shaheen, Healey, Jeff S., Birnie, David, Sanatani, Shubhayan, Gardner, Martin, Champagne, Jean, Simpson, Chris, Ahmad, Kamran, van den Berg, Maarten P., Chauhan, Vijay, Backx, Peter H., van Tintelen, J. Peter, Krahn, Andrew D., and Gollob, Michael H.

Abstract

Supplemental Digital Content is available in the text.

Published

2014

42. New clinical molecular diagnostic methods for congenital and inherited heart disease

Author

Jongbloed, Jan DH, Pósafalvi, Anna, Kerstjens-Frederikse, Wilhelmina S, Sinke, Richard J, and van Tintelen, J Peter

Abstract

Importance of the field:For patients with congenital and inherited heart disorders, causative mutations are often not identified owing to limitations of current screening techniques. Identifying the mutation is of major importance for genetic counseling of patients and families, facilitating the diagnosis in people at risk and directing clinical management. Next-generation sequencing (NGS) provides unprecedented opportunities to maximize mutation yields and improve clinical management, genetic counseling and monitoring of patients.Areas covered in this review:Recent NGS applications are reviewed, focusing on methods relevant for molecular diagnostics in cardiogenetics. Requirements for reliable implementation in clinical practice and challenges that clinicians, bioinfomaticians and molecular diagnosticians must deal with in analyzing resulting data are discussed.What the reader will gain:Readers will be introduced to recent developments, techniques and applications in NGS. They will learn about possibilities of using it in clinical diagnostics. They will become acquainted with difficulties and challenges in interpreting the data and considerations around communicating these issues to patients and the community.Take home message:Although several obstacles are still to be overcome and there is much still to learn, NGS will revolutionize clinical molecular diagnostics of inherited and congenital cardiac diseases, maximizing mutation yields and leading to optimized diagnostic and clinical care.

Published

2011

43. Arrhythmogenic Right Ventricular Dysplasia/Cardiomyopathy Diagnostic Task Force Criteria

Author

Cox, Moniek G.P.J., van der Smagt, Jasper J., Noorman, Maartje, Wiesfeld, Ans C., Volders, Paul G.A., van Langen, Irene M., Atsma, Douwe E., Dooijes, Dennis, Houweling, Arjan C., Loh, Peter, Jordaens, Luc, Arens, Yvonne, Cramer, Maarten J., Doevendans, Pieter A., van Tintelen, J. Peter, Wilde, Arthur A.M., and Hauer, Richard N.W.

Abstract

Arrhythmogenic Right Ventricular Dysplasia/Cardiomyopathy (ARVD/C) Diagnostic Task Force Criteria (TFC) proposed in 1994 are highly specific but lack sensitivity. A new international task force modified criteria to improve diagnostic yield. A comparison of diagnosis by 1994 TFC versus newly proposed criteria in 3 patient groups was conducted.

Published

2010

44. The importance of the family history in caring for families with long QT syndrome and dilated cardiomyopathyHow to cite this article: Ruiter JS, BerkenboschNieuwhof K, van den Berg MP, van Dijk R, Middel B, van Tintelen JP. 2010. The importance of the family history in caring for families with long QT syndrome and dilated cardiomyopathy. Am J Med Genet Part A 152A:607–612.Jolien S. Ruiter and Karin BerkenboschNieuwhof contributed equally to this work.

Author

Ruiter, Jolien S., BerkenboschNieuwhof, Karin, van den Berg, Maarten P., van Dijk, Rene, Middel, Berrie, and van Tintelen, J. Peter

Abstract

In potentially inherited cardiac diseases, the family history is of great importance. We looked at the way cardiologists take a family history in patients with idiopathic dilated cardiomyopathy DCM or long QT syndrome LQTS and whether this led to screening of relatives or other followup. We performed retrospective crosssectional analyses of adult index patients with DCM or LQTS in a general hospital GH or a University Medical Center UMC. We identified 82 index patients with DCM 34 GH; 48 UMC and 20 with LQTS all UMC between 1996 and 2005. Mean followup was 58 months. A family history was recorded in 90 of both LQTS and DCM patients most of the cases restricted to firstdegree family members. The genetic aspects, counseling and screening of family members was discussed significantly more often with LQTS than DCM patients all P < 0.05. Also followup screening of family members, DNA analysis and referral was performed significantly more often in LQTS than DCM patients. Cardiologists in the UMC referred DCM index patients for genetic counseling more often than those in the GH 25 vs. 6; P < 0.05. Only a few index patients with DCM were referred to a clinical genetics department. Onethird of DCM cases and nearly all LQTS cases are familial. Since early recognition and treatment may reduce morbidity and mortality we recommend cardiologists take a more thorough family history and always consider referring to a clinical genetics department in such index patients. © 2010 WileyLiss, Inc.

Published

2010

45. Family letters are an effective way to inform relatives about inherited cardiac disease

Author

van der Roest, Wilma P., Pennings, José M., Bakker, Marian, van den Berg, Maarten P., and van Tintelen, J. Peter

Abstract

Increasing numbers of individuals are being referred to cardiogenetics outpatient clinics with potentially inherited arrhythmia ARR or cardiomyopathy CM. To inform relatives atrisk, we ask index patients to distribute “family letters” containing information on the risks, possible genetic and other screenings, and preventive options. We assessed the responses to these letters in terms of referrals to a cardiologist andor clinical geneticist. Fiftysix index patients were asked to distribute 249 family letters: 85 in the ARR group and 164 in the CM group. Within a mean followup period of 2 years range 1–5 years the number of relatives actually referred to the clinical geneticist andor cardiologist was 57 142 of 249. There was a significant difference P < 0.01 between the ARR 80 and CM groups 45.1. To verify the results obtained from our files at the cardiogenetics department we sent a questionnaire to 52 index patients response 50. This showed that 2326 88 index patients had distributed the letters to their relatives and that for 1923 index patients one or more relatives had been screened. This is comparable with our files, which showed that 57 of relatives of index patients with a potentially inherited cardiac disease underwent screening, particularly in the ARR group. The actual response was underestimated because some relatives were investigated elsewhere or may still decide to be screened in the future. We conclude that distributing family letters is an effective way to inform and encourage relatives to undergo screening for highrisk inherited cardiac disease. Am. J. Med. Genet. © 2009 WileyLiss, Inc.

Published

2009

46. The influence of coping styles and perceived control on emotional distress in persons at risk for a hereditary heart diseaseHow to cite this article: Hoedemaekers E, Jaspers JPC, Van Tintelen JP. 2007. The influence of coping styles and perceived control on emotional distress in persons at risk for a hereditary heart disease. Am J Med Genet Part A 143A:1997–2005.

Author

Hoedemaekers, Elly, Jaspers, Jan P.C., and Van Tintelen, J. Peter

Abstract

This prospective study investigates the influence of two coping styles (monitoring and blunting) and perceived control (health locus of control and mastery) on emotional distress in persons at risk of a hereditary cardiac disease. Emotional distress in people at risk for a hereditary cardiac disease does not differ from the normal population, neither before nor after disclosure of the DNA‐or clinical test results. Less monitoring reflects less emotional distress before the results of the DNA‐test or clinical investigations are known, while a stronger feeling of mastery reflects less emotional distress both before and after the results of the tests are known. These results indicate that the negative effect of monitoring is temporary. Mastery is a more powerful predictor than health locus of control in this situation. © 2007 Wiley‐Liss, Inc.

Published

2007

47. Correction to: The genetic architecture of Plakophilin 2 cardiomyopathy

Author

Dries, Annika M., Kirillova, Anna, Reuter, Chloe M., Garcia, John, Zouk, Hana, Hawley, Megan, Murray, Brittney, Tichnell, Crystal, Pilichou, Kalliopi, Protonotarios, Alexandros, Medeiros-Domingo, Argelia, Kelly, Melissa A., Baras, Aris, Ingles, Jodie, Semsarian, Christopher, Bauce, Barbara, Celeghin, Rudy, Basso, Cristina, Jongbloed, Jan D.H., Nussbaum, Robert L., Funke, Birgit, Cerrone, Marina, Mestroni, Luisa, Taylor, Matthew R.G., Sinagra, Gianfranco, Merlo, Marco, Saguner, Ardan M., Elliott, Perry M., Syrris, Petros, van Tintelen, J. Peter, James, Cynthia A., Haggerty, Christopher M., and Parikh, Victoria N.

Published

2021

48. Epicardial differentiation drives fibro-fatty remodeling in arrhythmogenic cardiomyopathy

Author

Kohela, Arwa, van Kampen, Sebastiaan J., Moens, Tara, Wehrens, Martijn, Molenaar, Bas, Boogerd, Cornelis J., Monshouwer-Kloots, Jantine, Perini, Ilaria, Goumans, Marie José, Smits, Anke M., van Tintelen, J. Peter, and van Rooij, Eva

Abstract

Description

Published

2021

49. Arrhythmogenic Right Ventricular Cardiomyopathy-Associated Desmosomal Variants Are Rarely De Novo: Segregation and Haplotype Analysis of a Multinational Cohort.

Author

van Lint, Freyja H.M., Murray, Brittney, Tichnell, Crystal, Zwart, Rob, Amat, Nuria, Lekanne Deprez, Ronald H., Dittmann, Sven, Stallmeyer, Birgit, Calkins, Hugh, van der Smagt, Jasper J., van den Wijngaard, Arthur, Dooijes, Dennis, van der Zwaag, Paul A., Schulze-Bahr, Eric, Judge, Daniel P., Jongbloed, Jan D.H., van Tintelen, J. Peter, and James, Cynthia A.

Abstract

Supplemental Digital Content is available in the text. Background: Arrhythmogenic right ventricular cardiomyopathy (ARVC) is associated with pathogenic/likely pathogenic (P/LP) variants in genes encoding the cardiac desmosomal proteins. Origin of these variants, including de novo mutation rate and extent of founder versus recurrent variants has implications for variant adjudication and clinical care, yet this has never been systematically investigated. Methods: We identified arrhythmogenic right ventricular cardiomyopathy probands who met 2010 Task Force Criteria and had undergone genotyping that included sequencing of the desmosomal genes (PKP2 , DSP , DSG2 , DSC2 , and JUP) from 3 arrhythmogenic right ventricular cardiomyopathy registries in America and Europe. We classified the desmosomal variants, defined the contribution of unique versus nonunique (ie, not family-specific) P/LP variants, and identified the frequency and characteristics of de novo variants. Next, we haplotyped nonunique variants to determine how often they likely represent a single mutation event in a common ancestor (implied by shared haplotypes) versus multiple mutation events at the same genetic location. Results: Of 501 arrhythmogenic right ventricular cardiomyopathy probands, 322 (64.3%) carried 327 desmosomal P/LP variants. Most variants (n=247, 75.6%, in 245 patients) were identified in more than one proband and, therefore, considered nonunique. For 212/327 variants (64.8%) genetic cascade screening was performed extensively enough to identify the parental origin of the P/LP variant. Only 3 variants were de novo, 2 of which were whole gene deletions. For 24 nonunique P/LP PKP2 variants, haplotyping was conducted in 183 available families. For all 24 variants, multiple seemingly unrelated families sharing identical haplotypes were identified, suggesting that these variants originate from common founders. Conclusions: Most desmosomal P/LP variants are inherited, nonunique, and originate from ancient founders. Two of 3 de novo variants were large deletions. These observations inform genetic testing, cascade screening, and variant adjudication. [ABSTRACT FROM AUTHOR]

Published

2019

50. Effect of Ascertainment Bias on Estimates of Patient Mortality in Inherited Cardiac Diseases.

Author

Nannenberg, Eline A., van Rijsingen, Ingrid A.W., van der Zwaag, Paul A., van den Berg, Maarten P., van Tintelen, J. Peter, Tanck, Michael W.T., Ackerman, Michael J., Wilde, Arthur A.M., and Christiaans, Imke

Abstract

Supplemental Digital Content is available in the text. Background: Accurate estimates of survival are indispensable for cardiologists, clinical geneticists, and genetic counselors dealing with families with an inherited cardiac disease. However, a bias towards a more severe disease with a worse outcome in the first publications may not accurately represent the actual survival forecast. We, therefore, evaluated the effect of ascertainment bias on survival in 3 different inherited cardiac diseases (idiopathic ventricular fibrillation, SCN5A overlap syndrome, and arrhythmogenic cardiomyopathy) caused by a founder mutation. Methods: We collected mortality data from mutation-positive subjects with either DPP6 -associated idiopathic ventricular fibrillation, SCN5A overlap syndrome, and PLN -R14del-mediated arrhythmogenic cardiomyopathy >2 to 10 years of ongoing clinical/cascade genetic screening. Results: The median age of survival in DPP6 mutation-positive subjects increased from 44.6 years in the original cohort from 2008 (n=60; 95% CI, 36.8–52.4 years) to 68.2 years in the extended cohort from 2012 (n=235; 95% CI, 64.6–71.7 years; P <0.001). In the SCN5A overlap syndrome, survival increased from 56.1 years in 1999 (n=86; 95% CI, 48.0–64.2 years) to 69.7 years in 2009 (n=197; 95% CI, 61.3–78.2 years; P =0.049). In PLN -R14del positive patients, the median age of survival increased from 63.5 years in 2010 (n=89; 95% CI, 59.1–68.0 years) to 65.2 years in 2012 (n=370; 95% CI, 62.0–68.3 years; P =0.046). Conclusions: The median age of survival in 3 different inherited cardiac diseases with an established pathogenic substrate significantly increased once genetic testing and cascade screening extended, after the first publication that elucidated the discovery of the disease-susceptibility gene/mutation. This underscores the direct and negative influence of ascertainment bias on survival forecasts and the importance of ongoing clinical/genetic follow-up to establish the most accurate disease prognosis for genetically mediated heart diseases. [ABSTRACT FROM AUTHOR]

Published

2018