Identification of Variants and Mutational Analyses of Cardiac Myosin-binding Protein C (MYBPC3) Gene of Adult Bangladeshi Patients with Hypertrophic Cardiomyopathy.

Mymensingh medical journal : MMJ Pub Date : 2023-04-01
L A Banu, M M Masum, S Rahman, S Mahbuba, M Hossain, M J Hosen, S K Banerjee, D K Adhikary, S A Habib, G N Sultana, M N Islam
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Abstract

Hypertrophic cardiomyopathy (HCM) is the most prevalent genetic hereditary cardiomyopathy characterized by sudden cardiac death. Mutations in the MYBPC3 gene are often the most prevalent genetic abnormality in HCM with a prevalence ranging from 20.0 to 42.0%. The mutation spectrum is available for different countries, but such studies are lacking in the Asian population including Bangladeshi patients. A cross-sectional descriptive study was conducted for mutation analysis of the whole MYBPC3 gene on a cohort of 75 HCM Bengali Bangladeshi probands through Next Generation Sequencing at the Genetic Research Lab of Bangabandhu Sheikh Mujib Medical University from 2016 to 2019. The structural and functional impact of the mutations was further analyzed by in silico process. We analyzed the data and found 103 variants in 102 locations in the MYBPC3 gene. Variants were identified in both the coding region and the non-coding region. We found one possibly novel variant in the MYBPC3 gene. The findings of this research will help to develop a genetic database of HCM which will help in the early diagnosis and proper management of HCM patients in Bangladesh. One pathogenic splice donor variant (47356592 C >T) was found in the intronic region. Among the variants in the coding region, one missense mutation was pathogenic (NP₋000247.2: p.Asp770Asn) which was found in seven patients and another one is of conflicting interpretations of pathogenicity (NP₋000247.2: p.Ser217Gly) which was found in two patients. We have identified one in-frame deletion (NP₋000247.2: p.Ala433del) that is possible a novel variant responsible for the development of HCM.

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孟加拉国成年肥厚性心肌病患者心肌肌球蛋白结合蛋白C (MYBPC3)基因的变异鉴定和突变分析
肥厚性心肌病(HCM)是最常见的遗传性心肌病,其特征是心源性猝死。MYBPC3基因突变通常是HCM中最常见的遗传异常,患病率为20.0%至42.0%。突变谱在不同的国家都有,但在包括孟加拉国患者在内的亚洲人群中缺乏这样的研究。2016 - 2019年,在孟加拉谢赫穆吉布医科大学遗传研究实验室,通过下一代测序对75名HCM孟加拉裔先证者进行了全MYBPC3基因突变的横断面描述性研究。通过硅化工艺进一步分析突变对结构和功能的影响。我们分析了数据,在MYBPC3基因的102个位置发现了103个变体。在编码区和非编码区都发现了变异。我们在MYBPC3基因中发现了一个可能的新变体。这项研究的结果将有助于建立一个HCM遗传数据库,这将有助于孟加拉国HCM患者的早期诊断和适当管理。在内含子区发现1个致病性剪接供体变异(47356592 C >T)。在编码区变异中,1个错义突变为致病性突变(NP 247.2: p.Asp770Asn),在7例患者中发现;另1个错义突变(NP 247.2: p.Ser217Gly)在2例患者中发现,对致病性解释矛盾。我们已经确定了一个帧内缺失(NP 247.2: p.Ala433del),这可能是一个负责HCM发展的新变体。
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