Novel MYBPC3 Mutations in Indian Population with Cardiomyopathies.

IF 1.8 4区医学 Q3 PHARMACOLOGY & PHARMACY

Pharmacogenomics & Personalized Medicine Pub Date : 2023-09-20 eCollection Date: 2023-01-01 DOI:10.2147/PGPM.S407179

Deepa Selvi Rani, Apoorva Kasala, Perundurai S Dhandapany, Uthiralingam Muthusami, Sreejith Kunnoth, Andiappan Rathinavel, Dharma Rakshak Ayapati, Kumarasamy Thangaraj

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Abstract

Background: Mutations in Myosin Binding Protein C (MYBPC3) are one of the most frequent causes of cardiomyopathies in the world, but not much data are available in India.

Methods: We carried out targeted direct sequencing of MYBPC3 in 115 hypertrophic (HCM) and 127 dilated (DCM) cardiomyopathies against 197 ethnically matched healthy controls from India.

Results: We detected 34 single nucleotide variations in MYBPC3, of which 19 were novel. We found a splice site mutation [(IVS6+2T) T>G] and 16 missense mutations in Indian cardiomyopathies [5 in HCM; E258K, T262S, H287L, R408M, V483A: 4 in DCM; T146N, V321L, A392T, E393K and 7 in both HCM and DCM; L104M, V158M, S236G, R272C, T290A, G522E, A626V], but those were absent in 197 normal healthy controls. Interestingly, we found 7 out of 16 missense mutations (V158M, E258K, R272C, A392T, V483A, G522E, and A626V) in MYBPC3 were altering the evolutionarily conserved native amino acids, accounted for 8.7% and 6.3% in HCM and DCM, respectively. The bioinformatic tools predicted that those 7 missense mutations were pathogenic. Moreover, the co-segregation of those 7 mutations in families further confirmed their pathogenicity. Remarkably, we also identified compound mutations within the MYBPC3 gene of 6 cardiomyopathy patients (5%) with more severe disease phenotype; of which, 3 were HCM (2.6%) [(1. K244K + E258K + (IVS6+2T) T>G); (2. L104M + G522E + A626V); (3. P186P + G522E + A626V]; and 3 were DCM (2.4%) [(1. 5'UTR + A392T; 2. V158M+G522E; and 3.V158M + T262T + A626V].

Conclusion: The present comprehensive study on MYBPC3 has revealed both single and compound mutations in MYBPC3 and their association with disease in Indian Population with Cardiomyopathies. Our findings may perhaps help in initiating diagnostic strategies and eventually recognizing the targets for therapeutic interventions.

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印度心肌病人群中新的MYBPC3突变。

背景：肌球蛋白结合蛋白C（MYBPC3）突变是世界上最常见的心肌病病因之一，方法：我们对115例肥厚型（HCM）和127例扩张型（DCM）心肌病患者的MYBPC3进行了靶向直接测序，对来自印度的197名种族匹配的健康对照进行了测序。结果：我们检测到MYBPC3的34个单核苷酸变异，其中19个是新的。我们在印度心肌病中发现了一个剪接位点突变[（IVS6+2T）T>G]和16个错义突变[5在HCM中；E258K、T262S、H287L、R408M、V483A:4在DCM中；T146N、V321L、A392T、E393K和7在HCM和DCM中；L104M、V158M、S236G、R272C、T290A、G522E、A626V]，但在197个正常健康对照中没有这些突变。有趣的是，我们发现MYBPC3中16个错义突变中有7个（V158M、E258K、R272C、A392T、V483A、G522E和A626V）改变了进化上保守的天然氨基酸，在HCM和DCM中分别占8.7%和6.3%。生物信息学工具预测这7个错义突变具有致病性。此外，这7个突变在家族中的共分离进一步证实了它们的致病性。值得注意的是，我们还在6名具有更严重疾病表型的心肌病患者（5%）的MYBPC3基因中发现了复合突变；其中HCM 3例（2.6%）[（1。K244K+E258K+（IVS6+2T）T>G）；（2.L104M+G522E+A626V）；（3.P186P+G522E+A626V]；3例为DCM（2.4%）[（1。5'UTR+392t；2.V158M+G522E；结论：目前对MYBPC3的综合研究揭示了MYBPC3中的单一和复合突变及其与印度心肌病患者疾病的关系。我们的发现可能有助于启动诊断策略，并最终确定治疗干预的目标。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Pharmacogenomics & Personalized Medicine Biochemistry, Genetics and Molecular Biology-Molecular Medicine

CiteScore

3.30

自引率

5.30%

发文量

110

审稿时长

16 weeks

期刊介绍： Pharmacogenomics and Personalized Medicine is an international, peer-reviewed, open-access journal characterizing the influence of genotype on pharmacology leading to the development of personalized treatment programs and individualized drug selection for improved safety, efficacy and sustainability. In particular, emphasis will be given to: Genomic and proteomic profiling Genetics and drug metabolism Targeted drug identification and discovery Optimizing drug selection & dosage based on patient''s genetic profile Drug related morbidity & mortality intervention Advanced disease screening and targeted therapeutic intervention Genetic based vaccine development Patient satisfaction and preference Health economic evaluations Practical and organizational issues in the development and implementation of personalized medicine programs.