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Review
. 2010 Apr;40(4):360-9.
doi: 10.1111/j.1365-2362.2010.02268.x.

Hypertrophic cardiomyopathy: from genetics to treatment

Ali J Marian  1
Affiliations
Review

Hypertrophic cardiomyopathy: from genetics to treatment

Ali J Marian. Eur J Clin Invest. 2010 Apr.

Abstract

Background: Hypertrophic cardiomyopathy (HCM) is the prototypic form of pathological cardiac hypertrophy. HCM is an important cause of sudden cardiac death in the young and a major cause of morbidity in the elderly.

Design: We discuss the clinical implications of recent advances in the molecular genetics of HCM.

Results: The current diagnosis of HCM is neither adequately sensitive nor specific. Partial elucidation of the molecular genetic basis of HCM has raised interest in genetic-based diagnosis and management. Over a dozen causal genes have been identified. MYH7 and MYBPC3 mutations account for about 50% of cases. The remaining known causal genes are uncommon and some are rare. Advances in DNA sequencing techniques have made genetic screening practical. The difficulty, particularly in the sporadic cases and in small families, is to discern the causal from the non-causal variants. Overall, the causal mutations alone have limited implications in risk stratification and prognostication, as the clinical phenotype arises from complex and often non-linear interactions between various determinants.

Conclusions: The clinical phenotype of 'HCM' results from mutations in sarcomeric proteins and subsequent activation of multiple cellular constituents including signal transducers. We advocate that HCM, despite its current recognition and management as a single disease entity, involves multiple partially independent mechanisms, despite similarity in the ensuing phenotype. To treat HCM effectively, it is necessary to delineate the underlying fundamental mechanisms that govern the pathogenesis of the phenotype and apply these principles to the treatment of each subset of clinically recognized HCM.

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Figures

Figure 1
Figure 1
Contrasting effects of mutations on calcium sensitivity of myofibrillar ATPase activity. Calcium sensitivity of myofibrillar ATPase activity is reduced in the β-myosin heavy chain-Q403 (MyHCQ403) transgenic rabbits as compared to non-transgenic rabbits. In contrast, it was increased in the cardiac troponin T-Q92 (cTnT-Q92) transgenic mice.
Figure 2
Figure 2
Pathogenesis of HCM. Mutations in sarcomeric proteins impair the protein structure and function and provide the initial impetus for expression and activation of the intermediary molecular phenotype. The intermediary molecular phenotype including activation of the hypertrophic signalling molecules induce cardiac hypertrophy and other histological and morphological phenotypes in HCM.
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