Your search keyword '"Ho, C.Y. (Carolyn Y.)"' showing total 8 results

1. Hypertrophic cardiomyopathy in myosin-binding protein C (MYBPC3) Icelandic founder mutation carriers

Author

Adalsteinsdottir, B. (Berglind), Burke, M. (Michael), Maron, B.J. (Barry J.), Danielsen, R. (Ragnar), López, B. (Begoña), Diez, J. (Javier), Jarolim, P. (Petr), Seidman, J.G. (J.G.), Seidman, C.E. (Christine E.), Ho, C.Y. (Carolyn Y.), and Gunnarsson, G.T. (Gunnar Th)

Subjects

Echocardiography, Iceland, Genetics, Cardiomyopathy hypertrophic, Myosin-binding protein C (MYBPC3)

Abstract

Objective: The myosin-binding protein C (MYBPC3) c.927-2A>G founder mutation accounts for >90% of sarcomeric hypertrophic cardiomyopathy (HCM) in Iceland. This cross-sectional observational study explored the penetrance and phenotypic burden among carriers of this single, prevalent founder mutation. Methods: We studied 60 probands with HCM caused by MYBPC3 c.927-2A>G and 225 first-degree relatives. All participants underwent comprehensive clinical evaluation and relatives were genotyped. Results: Genetic and clinical evaluation of relatives identified 49 genotype-positive (G+) relatives with left ventricular hypertrophy (G+/LVH+), 59 G+without LVH (G+/LVH−) and 117 genotype-negative relatives (unaffected). Compared with HCM probands, G+/ LVH+ relatives were older at HCM diagnosis, had less LVH, a less prevalent diastolic dysfunction, fewer ECG abnormalities, lower serum N-terminal pro-B-type natriuretic peptide (NT-proBNP) and high-sensitivity cardiac troponin I levels, and fewer symptoms. The penetrance of HCM was influenced by age and sex; specifically, LVH was present in 39% of G+males but only 9% of G+females under age 40 years (p=0.015), versus 86% and 83%, respectively, after age 60 (p=0.89). G+/LVH− subjects had normal wall thicknesses, diastolic function and NT-proBNP levels, but subtle changes in LV geometry and more ECG abnormalities than their unaffected relatives. Conclusions: Phenotypic expression of the Icelandic MYBPC3 founder mutation varies by age, sex and proband status. Men are more likely to have LVH at a younger age, and disease manifestations were more prominent in probands than in relatives identified via family screening. G+/LVH− individuals had subtle clinical differences from unaffected relatives well into adulthood, indicating subclinical phenotypic expression of the pathogenic mutation.

Published

2020

2. A Validated Model for Sudden Cardiac Death Risk Prediction in Pediatric Hypertrophic Cardiomyopathy

Author

Miron, A. (Anastasia), Lafreniere-Roula, M. (Myriam), Steve Fan, C.-P. (Chun-Po), Armstrong, K.R. (Katey R.), Dragulescu, A. (Andreea), Papaz, T. (Tanya), Manlhiot, C. (Cedric), Kaufman, B. (Beth), Butts, R.J. (Ryan J.), Gardin, L. (Letizia), Stephenson, E.A. (Elizabeth A.), Howard, T.S. (Taylor S.), Aziz, P.F. (Pete F.), Balaji, S. (Seshadri), Ladouceur, V.B. (Virginie Beauséjour), Benson, L.N. (Lee N.), Colan, S.D. (Steven), Godown, J. (Justin), Henderson, H.T. (Heather T.), Ingles, J. (Jodie), Jeewa, A. (Aamir), Jefferies, J.L. (John L.), Lal, A.K. (Ashwin K.), Mathew, J. (Jacob), Jean-St-Michel, E. (Emilie), Michels, M. (Michelle), Nakano, S.J. (Stephanie J.), Olivotto, I. (Iacopo), Parent, J.J. (John J.), Pereira, A. (A.), Semsarian, C. (Christopher), Whitehill, R.D. (Robert D.), Wittekind, S.G. (Samuel G.), Russell, M.W. (Mark W.), Conway, J. (Jennifer), Richmond, M.E. (Marc E.), Villa, C. (Chet), Weintraub, R.G. (Robert G), Rossano, J.W. (Joseph W.), Kantor, P.F. (Paul F.), Ho, C.Y. (Carolyn Y.), Mital, S. (Seema), Miron, A. (Anastasia), Lafreniere-Roula, M. (Myriam), Steve Fan, C.-P. (Chun-Po), Armstrong, K.R. (Katey R.), Dragulescu, A. (Andreea), Papaz, T. (Tanya), Manlhiot, C. (Cedric), Kaufman, B. (Beth), Butts, R.J. (Ryan J.), Gardin, L. (Letizia), Stephenson, E.A. (Elizabeth A.), Howard, T.S. (Taylor S.), Aziz, P.F. (Pete F.), Balaji, S. (Seshadri), Ladouceur, V.B. (Virginie Beauséjour), Benson, L.N. (Lee N.), Colan, S.D. (Steven), Godown, J. (Justin), Henderson, H.T. (Heather T.), Ingles, J. (Jodie), Jeewa, A. (Aamir), Jefferies, J.L. (John L.), Lal, A.K. (Ashwin K.), Mathew, J. (Jacob), Jean-St-Michel, E. (Emilie), Michels, M. (Michelle), Nakano, S.J. (Stephanie J.), Olivotto, I. (Iacopo), Parent, J.J. (John J.), Pereira, A. (A.), Semsarian, C. (Christopher), Whitehill, R.D. (Robert D.), Wittekind, S.G. (Samuel G.), Russell, M.W. (Mark W.), Conway, J. (Jennifer), Richmond, M.E. (Marc E.), Villa, C. (Chet), Weintraub, R.G. (Robert G), Rossano, J.W. (Joseph W.), Kantor, P.F. (Paul F.), Ho, C.Y. (Carolyn Y.), and Mital, S. (Seema)

Abstract

Background: Hypertrophic cardiomyopathy is the leading cause of sudden cardiac death (SCD) in children and young adults. Our objective was to develop and validate a SCD risk prediction model in pediatric hypertrophic cardiomyopathy to guide SCD prevention strategies. Methods: In an international multicenter observational cohort study, phenotype-positive patients with isolated hypertrophic cardiomyopathy <18 years of age at diagnosis were eligible. The primary outcome variable was the time from diagnosis to a composite of SCD events at 5-year follow-up: SCD, resuscitated sudden cardiac arrest, and aborted SCD, that is, appropriate shock following primary prevention implantable cardioverter defibrillators. Competing risk models with cause-specific hazard regression were used to identify and quantify clinical and genetic factors associated with SCD. The cause-specific regression model was implemented using boosting, and tuned with 10 repeated 4-fold cross-validations. The final model was fitted using all data with the tuned hyperparameter value that maximizes the c-statistic, and its performance was characterized by using the c-statistic for competing risk models. The final model was validated in an independent external cohort (SHaRe [Sarcomeric Human Cardiomyopathy Registry], n=285). Results: Overall, 572 patients met eligibility criteria with 2855 patient-years of follow-up. The 5-year cumulative proportion of SCD events was 9.1% (14 SCD, 25 resuscitated sudden cardiac arrests, and 14 aborted SCD). Risk predictors included age at diagnosis, documented nonsustained ventricular tachycardia, unexplained syncope, septal diameter z-score, left ventricular posterior wall diameter z score, left atrial diameter z score, peak left ventricular outflow tract gradient, and presence of a pathogenic variant. Unlike in adults, left ventricular outflow tract gradient had an inverse association, and family history of SCD had no association with SCD. Clinical and clinical/genetic mode

Published

2020

3. Sex-specific cardiac remodeling in early and advanced stages of hypertrophic cardiomyopathy

Author

Nijenkamp, L.L.A.M. (Louise), Bollen, I.A.E., Niessen, H.W.M. (Hans ), Dos Remedios, C.G. (Cris G.), Michels, M. (Michelle), Poggesi, C. (Corrado), Ho, C.Y. (Carolyn Y.), Kuster, D.W.D. (Diederik), Velden, J. (Jolanda) van der, Nijenkamp, L.L.A.M. (Louise), Bollen, I.A.E., Niessen, H.W.M. (Hans ), Dos Remedios, C.G. (Cris G.), Michels, M. (Michelle), Poggesi, C. (Corrado), Ho, C.Y. (Carolyn Y.), Kuster, D.W.D. (Diederik), and Velden, J. (Jolanda) van der

Abstract

Hypertrophic cardiomyopathy (HCM) is the most frequent genetic cardiac disease with a prevalence of 1:500 to 1:200. While most patients show obstructive HCM and a relatively stable clinical phenotype (stage II), a small group of patients progresses to end-stage HCM (stage IV) within a relatively brief

Published

2020

4. Hypertrophic Cardiomyopathy with Left Ventricular Systolic Dysfunction: Insights from the SHaRe Registry

Author

Marstrand, P. (Peter), Han, L. (Larry), Day, S.M. (Sharlene M.), Olivotto, I. (Iacopo), Ashley, E.A. (Euan A.), Michels, M. (Michelle), Pereira, A. (A.), Wittekind, S.G. (Samuel G.), Helms, A. (Adam), Saberi, S. (Sara), Jacoby, D. (Daniel), Ware, J.S. (James S.), Colan, S.D. (Steven), Semsarian, C. (Christopher), Ingles, J. (Jodie), Lakdawala, N.K. (Neal K.), Ho, C.Y. (Carolyn Y.), Marstrand, P. (Peter), Han, L. (Larry), Day, S.M. (Sharlene M.), Olivotto, I. (Iacopo), Ashley, E.A. (Euan A.), Michels, M. (Michelle), Pereira, A. (A.), Wittekind, S.G. (Samuel G.), Helms, A. (Adam), Saberi, S. (Sara), Jacoby, D. (Daniel), Ware, J.S. (James S.), Colan, S.D. (Steven), Semsarian, C. (Christopher), Ingles, J. (Jodie), Lakdawala, N.K. (Neal K.), and Ho, C.Y. (Carolyn Y.)

Abstract

Background: The term "end stage" has been used to describe hypertrophic cardiomyopathy (HCM) with left ventricular systolic dysfunction (LVSD), defined as occurring when left ventricular ejection fraction is <50%. The prognosis of HCM-LVSD has reportedly been poor, but because of its relative rarity, the natural history remains incompletely characterized. Methods: Data from 11 high-volume HCM specialty centers making up the international SHaRe Registry (Sarcomeric Human Cardiomyopathy Registry) were used to describe the natural history of patients with HCM-LVSD. Cox proportional hazards models were used to identify predictors of prognosis and incident development. Results: From a cohort of 6793 patients with HCM, 553 (8%) met the criteria for HCM-LVSD. Overall, 75% of patients with HCM-LVSD experienced clinically relevant events, and 35% met the composite outcome (all-cause death [n=128], cardiac transplantation [n=55], or left ventricular assist device implantation [n=9]). After recognition of HCM-LVSD, the median time to composite outcome was 8.4 years. However, there was substantial individual variation in natural history. Significant predictors of the composite outcome included the presence of multiple pathogenic/likely pathogenic sarcomeric variants (hazard ratio [HR], 5.6 [95% CI, 2.3-13.5]), atrial fibrillation (HR, 2.6 [95% CI, 1.7-3.5]), and left ventricular ejection fraction <35% (HR, 2.0 [95% CI, 1.3-2.8]). The incidence of new HCM-LVSD was ≈7.5% over 15 years. Significant predictors of developing incident HCM-LVSD included greater left ventricular cavity size (HR, 1.1 [95% CI, 1.0-1.3] and wall thickness (HR, 1.3 [95% CI, 1.1-1.4]), left ventricular ejection fraction of 50% to 60% (HR, 1.8 [95% CI, 1.2, 2.8]-2.8 [95% CI, 1.8-4.2]) at baseline evaluation, the presence of late gadolinium enhancement on cardiac magnetic resonance imaging (HR, 2.3 [95% CI, 1.0-4.9]), and the presence of a pathogenic/likely pathogenic sarcomeric variant, particularly in thin

Published

2020

5. Myosin Sequestration Regulates Sarcomere Function, Cardiomyocyte Energetics, and Metabolism, Informing the Pathogenesis of Hypertrophic Cardiomyopathy

Author

Toepfer, C.N. (Christopher N.), Garfinkel, A.C. (Amanda C.), Venturini, G. (Gabriela), Wakimoto, H. (Hiroko), Repetti, G. (Giuliana), Alamo, L. (Lorenzo), Sharma, A. (Arun), Agarwal, R. (Radhika), Ewoldt, J.F. (Jourdan F.), Cloonan, P. (Paige), Letendre, J. (Justin), Lun, M. (Mingyue), Olivotto, I. (Iacopo), Colan, S.D. (Steven), Ashley, E. (Euan), Jacoby, D. (Daniel), Michels, M. (Michelle), Redwood, C. (Charles), Watkins, H.C. (Hugh C.), Day, S.M. (Sharlene M.), Staples, J.F. (James F.), Padrón, R. (Raúl), Chopra, A. (Anant), Ho, C.Y. (Carolyn Y.), Chen, C.S. (Christopher S.), Pereira, A. (A.), Seidman, J.G. (Jonathan G.), Seidman, C. (Christine), Toepfer, C.N. (Christopher N.), Garfinkel, A.C. (Amanda C.), Venturini, G. (Gabriela), Wakimoto, H. (Hiroko), Repetti, G. (Giuliana), Alamo, L. (Lorenzo), Sharma, A. (Arun), Agarwal, R. (Radhika), Ewoldt, J.F. (Jourdan F.), Cloonan, P. (Paige), Letendre, J. (Justin), Lun, M. (Mingyue), Olivotto, I. (Iacopo), Colan, S.D. (Steven), Ashley, E. (Euan), Jacoby, D. (Daniel), Michels, M. (Michelle), Redwood, C. (Charles), Watkins, H.C. (Hugh C.), Day, S.M. (Sharlene M.), Staples, J.F. (James F.), Padrón, R. (Raúl), Chopra, A. (Anant), Ho, C.Y. (Carolyn Y.), Chen, C.S. (Christopher S.), Pereira, A. (A.), Seidman, J.G. (Jonathan G.), and Seidman, C. (Christine)

Abstract

BACKGROUND: Hypertrophic cardiomyopathy (HCM) is caused by pathogenic variants in sarcomere protein genes that evoke hypercontractility, poor relaxation, and increased energy consumption by the heart and increased patient risks for arrhythmias and heart failure. Recent studies show that pathogenic missense variants in myosin, the molecular motor of the sarcomere, are clustered in residues that participate in dynamic conformational states of sarcomere proteins. We hypothesized that these conformations are essential to adapt contractile output for energy conservation and that pathophysiology of HCM results from destabilization of these conformations. METHODS: We assayed myosin ATP binding to define the proportion of myosins in the super relaxed state (SRX) conformation or the disordered relaxed state (DRX) conformation in healthy rodent and human hearts, at baseline and in response to reduced hemodynamic demands of hibernation or pathogenic HCM variants. To determine the relationships between myosin conformations, sarcomere function, and cell biology, we assessed contractility, relaxation, and cardiomyocyte morphology and metabolism, with and without an allosteric modulator of myosin ATPase activity. We then tested whether the positions of myosin variants of unknown clinical significance that were identified in patients with HCM, predicted functional consequences and associations with heart failure and arrhythmias. RESULTS: Myosins undergo physiological shifts between the SRX conformation that maximizes energy conservation and the DRX conformation that enables cross-bridge formation with greater ATP consumption. Systemic hemodynamic requirements, pharmacological modulators of myosin, and pathogenic myosin missense mutations influenced the proportions of these conformations. Hibernation increased the proportion of myosins in the SRX conformation, whereas pathogenic variants destabilized these and increased the proportion of myosins in the DRX conformation, which enhanc

Published

2020

6. Genotype and Lifetime Burden of Disease in Hypertrophic Cardiomyopathy: Insights from the Sarcomeric Human Cardiomyopathy Registry (SHaRe)

Author

Ho, C.Y. (Carolyn Y.), Day, S.M. (Sharlene M.), Ashley, E.A. (Euan A.), Michels, M. (Michelle), Pereira, A.C. (Alexandre C.), Jacoby, D. (Daniel), Cirino, A.L. (Allison L.), Fox, J.C. (Jonathan C.), Lakdawala, N.K. (Neal K.), Ware, J.S. (James S.), Caleshu, C.A. (Colleen A.), Helms, A.S. (Adam S.), Colan, S.D. (Steven), Girolami, F. (Francesca), Cecchi, F. (Franco), Seidman, C. (Christine), Sajeev, G. (Gautam), Signorovitch, J. (James), Green, E.M. (Eric M.), Olivotto, I. (Iacopo), Ho, C.Y. (Carolyn Y.), Day, S.M. (Sharlene M.), Ashley, E.A. (Euan A.), Michels, M. (Michelle), Pereira, A.C. (Alexandre C.), Jacoby, D. (Daniel), Cirino, A.L. (Allison L.), Fox, J.C. (Jonathan C.), Lakdawala, N.K. (Neal K.), Ware, J.S. (James S.), Caleshu, C.A. (Colleen A.), Helms, A.S. (Adam S.), Colan, S.D. (Steven), Girolami, F. (Francesca), Cecchi, F. (Franco), Seidman, C. (Christine), Sajeev, G. (Gautam), Signorovitch, J. (James), Green, E.M. (Eric M.), and Olivotto, I. (Iacopo)

Abstract

Background: A better understanding of the factors that contribute to heterogeneous outcomes and lifetime disease burden in hypertrophic cardiomyopathy (HCM) is critically needed to improve patient management and outcomes. The Sarcomeric Human Cardiomyopathy Registry (SHaRe) was established to provide the scale of data required to address these issues, aggregating longitudinal datasets curated by eight international HCM specialty centers.Methods: Data on 4591 HCM patients (2763 genotyped), followed for a mean of 5.4±6.9 years (24,791 patient-years; median [interquartile range] 2.9 [0.3-7.9] years) were analyzed regarding cardiac ar

Published

2018

7. T1 measurements identify extracellular volume expansion in hypertrophic cardiomyopathy sarcomere mutation carriers with and without left ventricular hypertrophy

Author

Ho, C.Y. (Carolyn Y.), Abbasi, S.A. (S.A.), Neilan, T.G. (T.G.), Shah, R.V.(R.V.), Chen, Y.(Y.), Heydari, B. (B.), Cirino, A.L. (Alison L.), Lakdawala, N.K. (Neal K.), Orav, E.J. (E. J.), González-Miqueo, A. (Aránzazu), Lopez-Salazar, M.B. (María Begoña), Diez-Martinez, J. (Javier), Jerosch-Herold, M. (M.), and Kwong, R.Y. (Raymond Y.)

Subjects

Magnetic resonance imaging, Genetic, cardiovascular system, Hypertrophic cardiomyopath, cardiovascular diseases, Fibrosis

Abstract

Background—Myocardial fibrosis is a hallmark of hypertrophic cardiomyopathy (HCM) and a potential substrate for arrhythmias and heart failure. Sarcomere mutations seem to induce profibrotic changes before left ventricular hypertrophy (LVH) develops. To further evaluate these processes, we used cardiac magnetic resonance with T1 measurements on a genotyped HCM population to quantify myocardial extracellular volume (ECV). Methods and Results—Sarcomere mutation carriers with LVH (G+/LVH+, n=37) and without LVH (G+/LVH−, n=29), patients with HCM without mutations (sarcomere-negative HCM, n=11), and healthy controls (n=11) underwent contrast cardiac magnetic resonance, measuring T1 times pre- and postgadolinium infusion. Concurrent echocardiography and serum biomarkers of collagen synthesis, hemodynamic stress, and myocardial injury were also available in a subset. Compared with controls, ECV was increased in patients with overt HCM, as well as G+/LVH− mutation carriers (ECV=0.36±0.01, 0.33±0.01, 0.27±0.01 in G+/LVH+, G+/LVH−, controls, respectively; P≤0.001 for all comparisons). ECV correlated with N-terminal probrain natriuretic peptide levels (r=0.58; P60% of overt patients with HCM but absent from G+/LVH− subjects. Both ECV and late gadolinium enhancement were more extensive in sarcomeric HCM than sarcomere-negative HCM. Conclusions—Myocardial ECV is increased in HCM sarcomere mutation carriers even in the absence of LVH. These data provide additional support that fibrotic remodeling is triggered early in disease pathogenesis. Quantifying ECV may help characterize the development of myocardial fibrosis in HCM and ultimately assist in developing novel disease-modifying therapy, targeting interstitial fibrosis.

Published

2013

8. Myocardial fibrosis as an early manifestation of hypertrophic cardiomyopathy

Author

Ho, C.Y. (Carolyn Y.)

Subjects

Cardiomyopathy, Hypertrophic/complications, Myocardium/pathology, Procollagen/blood

Abstract

BACKGROUND: Myocardial fibrosis is a hallmark of hypertrophic cardiomyopathy and a proposed substrate for arrhythmias and heart failure. In animal models, profibrotic genetic pathways are activated early, before hypertrophic remodeling. Data showing early profibrotic responses to sarcomere-gene mutations in patients with hypertrophic cardiomyopathy are lacking. METHODS: We used echocardiography, cardiac magnetic resonance imaging (MRI), and serum biomarkers of collagen metabolism, hemodynamic stress, and myocardial injury to evaluate subjects with hypertrophic cardiomyopathy and a confirmed genotype. RESULTS: The study involved 38 subjects with pathogenic sarcomere mutations and overt hypertrophic cardiomyopathy, 39 subjects with mutations but no left ventricular hypertrophy, and 30 controls who did not have mutations. Levels of serum C-terminal propeptide of type I procollagen (PICP) were significantly higher in mutation carriers without left ventricular hypertrophy and in subjects with overt hypertrophic cardiomyopathy than in controls (31% and 69% higher, respectively; P

Published

2010