Myocardial perfusion defects in hypertrophic cardiomyopathy mutation carriers

Rebecca K. Hughes; Claudia Camaioni; João B. Augusto; Kristopher Knott; Ellie Quinn; Gabriella Captur; Andreas Seraphim; George Joy; Petros Syrris; Perry M. Elliott; Saidi Mohiddin; Peter Kellman; Hui Xue; Luis Rocha Lopes; James C. Moon

doi:10.1161/JAHA.120.020227

Myocardial perfusion defects in hypertrophic cardiomyopathy mutation carriers

Rebecca K. Hughes, Claudia Camaioni, João B. Augusto, Kristopher Knott, Ellie Quinn, Gabriella Captur, Andreas Seraphim, George Joy, Petros Syrris, Perry M. Elliott, Saidi Mohiddin, Peter Kellman, Hui Xue, Luis Rocha Lopes^*, James C. Moon

^*Autor correspondente para este trabalho

Resultado de pesquisa › revisão de pares

29 Citações (Scopus)

Resumo

BACKGROUND: Impaired myocardial blood flow (MBF) in the absence of epicardial coronary disease is a feature of hypertrophic cardiomyopathy (HCM). Although most evident in hypertrophied or scarred segments, reduced MBF can occur in apparently normal segments. We hypothesized that impaired MBF and myocardial perfusion reserve, quantified using perfusion mapping cardiac magnetic resonance, might occur in the absence of overt left ventricular hypertrophy (LVH) and late gadolinium enhancement, in mutation carriers without LVH criteria for HCM (genotype-positive, left ventricular hypertrophy-negative). METHODS AND RESULTS: A single center, case-control study investigated MBF and myocardial perfusion reserve (the ratio of MBF at stress:rest), along with other pre-phenotypic features of HCM. Individuals with genotype-positive, left ventricular hypertrophy-negative (n=50) with likely pathogenic/pathogenic variants and no evidence of LVH, and matched controls (n=28) underwent cardiac magnetic resonance. Cardiac magnetic resonance identified LVH-fulfilling criteria for HCM in 5 patients who were excluded. Individuals with genotype-positive, left ventricular hypertrophy-negative had longer indexed anterior mitral valve leaflet length (12.52±2.1 versus 11.55±1.6 mm/m², P=0.03), lower left ventricular end-systolic volume (21.0±6.9 versus 26.7±6.2 mm/m², P≤0.005) and higher left ventricular ejection fraction (71.9±5.5 versus 65.8±4.4%, P≤0.005). Maximum wall thickness was not significantly different (9.03±1.95 versus 8.37±1.2 mm, P=0.075), and no subject had significant late gadolinium enhancement (minor right ventricle‒insertion point late gadolinium enhancement only). Perfusion mapping demonstrated visual perfusion defects in 9 (20%) carriers versus 0 controls (P=0.011). These were almost all septal or near right ventricle insertion points. Globally, myocardial perfusion reserve was lower in carriers (2.77±0.83 versus 3.24±0.63, P=0.009), with a subendocardial:subepicardial myocardial perfusion reserve gradient (2.55±0.75 versus 3.2±0.65, P=<0.005; 3.01±0.96 versus 3.47±0.75, P=0.026) but equivalent MBF (2.75±0.82 versus 2.65±0.69 mL/g per min, P=0.826). CONCLUSIONS: Regional and global impaired myocardial perfusion can occur in HCM mutation carriers, in the absence of significant hypertrophy or scarring.

Idioma original	English
Número do artigo	e020227
Revista	Journal of the American Heart Association
Volume	10
Número de emissão	15
DOIs	https://doi.org/10.1161/JAHA.120.020227
Estado da publicação	Publicado - 2021
Publicado externamente	Sim

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Hughes, R. K., Camaioni, C., Augusto, J. B., Knott, K., Quinn, E., Captur, G., Seraphim, A., Joy, G., Syrris, P., Elliott, P. M., Mohiddin, S., Kellman, P., Xue, H., Lopes, L. R., & Moon, J. C. (2021). Myocardial perfusion defects in hypertrophic cardiomyopathy mutation carriers. Journal of the American Heart Association, 10(15), Artigo e020227. https://doi.org/10.1161/JAHA.120.020227

@article{90f0da9322e04fc6a94db31049457ef0,

title = "Myocardial perfusion defects in hypertrophic cardiomyopathy mutation carriers",

abstract = "BACKGROUND: Impaired myocardial blood flow (MBF) in the absence of epicardial coronary disease is a feature of hypertrophic cardiomyopathy (HCM). Although most evident in hypertrophied or scarred segments, reduced MBF can occur in apparently normal segments. We hypothesized that impaired MBF and myocardial perfusion reserve, quantified using perfusion mapping cardiac magnetic resonance, might occur in the absence of overt left ventricular hypertrophy (LVH) and late gadolinium enhancement, in mutation carriers without LVH criteria for HCM (genotype-positive, left ventricular hypertrophy-negative). METHODS AND RESULTS: A single center, case-control study investigated MBF and myocardial perfusion reserve (the ratio of MBF at stress:rest), along with other pre-phenotypic features of HCM. Individuals with genotype-positive, left ventricular hypertrophy-negative (n=50) with likely pathogenic/pathogenic variants and no evidence of LVH, and matched controls (n=28) underwent cardiac magnetic resonance. Cardiac magnetic resonance identified LVH-fulfilling criteria for HCM in 5 patients who were excluded. Individuals with genotype-positive, left ventricular hypertrophy-negative had longer indexed anterior mitral valve leaflet length (12.52±2.1 versus 11.55±1.6 mm/m2, P=0.03), lower left ventricular end-systolic volume (21.0±6.9 versus 26.7±6.2 mm/m2, P≤0.005) and higher left ventricular ejection fraction (71.9±5.5 versus 65.8±4.4%, P≤0.005). Maximum wall thickness was not significantly different (9.03±1.95 versus 8.37±1.2 mm, P=0.075), and no subject had significant late gadolinium enhancement (minor right ventricle‒insertion point late gadolinium enhancement only). Perfusion mapping demonstrated visual perfusion defects in 9 (20%) carriers versus 0 controls (P=0.011). These were almost all septal or near right ventricle insertion points. Globally, myocardial perfusion reserve was lower in carriers (2.77±0.83 versus 3.24±0.63, P=0.009), with a subendocardial:subepicardial myocardial perfusion reserve gradient (2.55±0.75 versus 3.2±0.65, P=<0.005; 3.01±0.96 versus 3.47±0.75, P=0.026) but equivalent MBF (2.75±0.82 versus 2.65±0.69 mL/g per min, P=0.826). CONCLUSIONS: Regional and global impaired myocardial perfusion can occur in HCM mutation carriers, in the absence of significant hypertrophy or scarring.",

keywords = "Genetics, Hypertrophic cardiomyopathy, Quantitative perfusion mapping, Sarcomere mutations carriers without hypertrophy",

author = "Hughes, {Rebecca K.} and Claudia Camaioni and Augusto, {Jo{\~a}o B.} and Kristopher Knott and Ellie Quinn and Gabriella Captur and Andreas Seraphim and George Joy and Petros Syrris and Elliott, {Perry M.} and Saidi Mohiddin and Peter Kellman and Hui Xue and Lopes, {Luis Rocha} and Moon, {James C.}",

note = "Funding Information: R.K.H. is supported by the British Heart Foundation (grant number FS/17/82/33222). G.C. is supported by the National Institute for Health Research Rare Diseases Translational Research Collaboration (NIHR RD‐TRC, #171603) and by NIHR University College London Hospitals Biomedical Research Centre. J.C.M., P.S., L.R.L., and P.M.E. are directly and indirectly supported by the University College London Hospitals NIHR Biomedical Research Centre and Biomedical Research Unit at Barts Hospital, respectively. Part of this work was supported by a Barts Charity Grant to L.R.L. L.R.L. is funded by a Medical Research Council Clinical Academic Research Partnership (CARP) award. Publisher Copyright: {\textcopyright} 2021 The Authors. Published on behalf of the American Heart Association, Inc., by Wiley.",

year = "2021",

doi = "10.1161/JAHA.120.020227",

language = "English",

volume = "10",

journal = "Journal of the American Heart Association",

issn = "2047-9980",

publisher = "Wiley-Blackwell Publishing Ltd",

number = "15",

}

TY - JOUR

T1 - Myocardial perfusion defects in hypertrophic cardiomyopathy mutation carriers

AU - Hughes, Rebecca K.

AU - Camaioni, Claudia

AU - Augusto, João B.

AU - Knott, Kristopher

AU - Quinn, Ellie

AU - Captur, Gabriella

AU - Seraphim, Andreas

AU - Joy, George

AU - Syrris, Petros

AU - Elliott, Perry M.

AU - Mohiddin, Saidi

AU - Kellman, Peter

AU - Xue, Hui

AU - Lopes, Luis Rocha

AU - Moon, James C.

N1 - Funding Information: R.K.H. is supported by the British Heart Foundation (grant number FS/17/82/33222). G.C. is supported by the National Institute for Health Research Rare Diseases Translational Research Collaboration (NIHR RD‐TRC, #171603) and by NIHR University College London Hospitals Biomedical Research Centre. J.C.M., P.S., L.R.L., and P.M.E. are directly and indirectly supported by the University College London Hospitals NIHR Biomedical Research Centre and Biomedical Research Unit at Barts Hospital, respectively. Part of this work was supported by a Barts Charity Grant to L.R.L. L.R.L. is funded by a Medical Research Council Clinical Academic Research Partnership (CARP) award. Publisher Copyright: © 2021 The Authors. Published on behalf of the American Heart Association, Inc., by Wiley.

PY - 2021

Y1 - 2021

N2 - BACKGROUND: Impaired myocardial blood flow (MBF) in the absence of epicardial coronary disease is a feature of hypertrophic cardiomyopathy (HCM). Although most evident in hypertrophied or scarred segments, reduced MBF can occur in apparently normal segments. We hypothesized that impaired MBF and myocardial perfusion reserve, quantified using perfusion mapping cardiac magnetic resonance, might occur in the absence of overt left ventricular hypertrophy (LVH) and late gadolinium enhancement, in mutation carriers without LVH criteria for HCM (genotype-positive, left ventricular hypertrophy-negative). METHODS AND RESULTS: A single center, case-control study investigated MBF and myocardial perfusion reserve (the ratio of MBF at stress:rest), along with other pre-phenotypic features of HCM. Individuals with genotype-positive, left ventricular hypertrophy-negative (n=50) with likely pathogenic/pathogenic variants and no evidence of LVH, and matched controls (n=28) underwent cardiac magnetic resonance. Cardiac magnetic resonance identified LVH-fulfilling criteria for HCM in 5 patients who were excluded. Individuals with genotype-positive, left ventricular hypertrophy-negative had longer indexed anterior mitral valve leaflet length (12.52±2.1 versus 11.55±1.6 mm/m2, P=0.03), lower left ventricular end-systolic volume (21.0±6.9 versus 26.7±6.2 mm/m2, P≤0.005) and higher left ventricular ejection fraction (71.9±5.5 versus 65.8±4.4%, P≤0.005). Maximum wall thickness was not significantly different (9.03±1.95 versus 8.37±1.2 mm, P=0.075), and no subject had significant late gadolinium enhancement (minor right ventricle‒insertion point late gadolinium enhancement only). Perfusion mapping demonstrated visual perfusion defects in 9 (20%) carriers versus 0 controls (P=0.011). These were almost all septal or near right ventricle insertion points. Globally, myocardial perfusion reserve was lower in carriers (2.77±0.83 versus 3.24±0.63, P=0.009), with a subendocardial:subepicardial myocardial perfusion reserve gradient (2.55±0.75 versus 3.2±0.65, P=<0.005; 3.01±0.96 versus 3.47±0.75, P=0.026) but equivalent MBF (2.75±0.82 versus 2.65±0.69 mL/g per min, P=0.826). CONCLUSIONS: Regional and global impaired myocardial perfusion can occur in HCM mutation carriers, in the absence of significant hypertrophy or scarring.

AB - BACKGROUND: Impaired myocardial blood flow (MBF) in the absence of epicardial coronary disease is a feature of hypertrophic cardiomyopathy (HCM). Although most evident in hypertrophied or scarred segments, reduced MBF can occur in apparently normal segments. We hypothesized that impaired MBF and myocardial perfusion reserve, quantified using perfusion mapping cardiac magnetic resonance, might occur in the absence of overt left ventricular hypertrophy (LVH) and late gadolinium enhancement, in mutation carriers without LVH criteria for HCM (genotype-positive, left ventricular hypertrophy-negative). METHODS AND RESULTS: A single center, case-control study investigated MBF and myocardial perfusion reserve (the ratio of MBF at stress:rest), along with other pre-phenotypic features of HCM. Individuals with genotype-positive, left ventricular hypertrophy-negative (n=50) with likely pathogenic/pathogenic variants and no evidence of LVH, and matched controls (n=28) underwent cardiac magnetic resonance. Cardiac magnetic resonance identified LVH-fulfilling criteria for HCM in 5 patients who were excluded. Individuals with genotype-positive, left ventricular hypertrophy-negative had longer indexed anterior mitral valve leaflet length (12.52±2.1 versus 11.55±1.6 mm/m2, P=0.03), lower left ventricular end-systolic volume (21.0±6.9 versus 26.7±6.2 mm/m2, P≤0.005) and higher left ventricular ejection fraction (71.9±5.5 versus 65.8±4.4%, P≤0.005). Maximum wall thickness was not significantly different (9.03±1.95 versus 8.37±1.2 mm, P=0.075), and no subject had significant late gadolinium enhancement (minor right ventricle‒insertion point late gadolinium enhancement only). Perfusion mapping demonstrated visual perfusion defects in 9 (20%) carriers versus 0 controls (P=0.011). These were almost all septal or near right ventricle insertion points. Globally, myocardial perfusion reserve was lower in carriers (2.77±0.83 versus 3.24±0.63, P=0.009), with a subendocardial:subepicardial myocardial perfusion reserve gradient (2.55±0.75 versus 3.2±0.65, P=<0.005; 3.01±0.96 versus 3.47±0.75, P=0.026) but equivalent MBF (2.75±0.82 versus 2.65±0.69 mL/g per min, P=0.826). CONCLUSIONS: Regional and global impaired myocardial perfusion can occur in HCM mutation carriers, in the absence of significant hypertrophy or scarring.

KW - Genetics

KW - Hypertrophic cardiomyopathy

KW - Quantitative perfusion mapping

KW - Sarcomere mutations carriers without hypertrophy

UR - http://www.scopus.com/inward/record.url?scp=85111077655&partnerID=8YFLogxK

U2 - 10.1161/JAHA.120.020227

DO - 10.1161/JAHA.120.020227

M3 - Article

C2 - 34310159

AN - SCOPUS:85111077655

SN - 2047-9980

VL - 10

JO - Journal of the American Heart Association

JF - Journal of the American Heart Association

IS - 15

M1 - e020227

ER -

Myocardial perfusion defects in hypertrophic cardiomyopathy mutation carriers

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