巴基斯坦普什图族人群2型糖尿病风险变异(等位基因)的评估

IF 0.6 Q4 ENDOCRINOLOGY & METABOLISM
Asif Jan, Muhammad Saeed, Zakiullah, Rani Akbar, Hamayun Khan
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引用次数: 3

摘要

目的:利用新兴全外显子组测序(WES)评估开伯尔-普赫图赫瓦普什图族人群中2型糖尿病(T2D)风险变异,以更好地了解这一复杂多基因疾病的发病机制。方法:共纳入100例确诊的普什图族T2D患者,从全血样本中提取DNA,使用Illumina Nextera XT DNA文库试剂盒严格按照制造商的说明制备成对端文库。利用Illumina HiSeq 2000对制备的文库进行测序,并进行生物信息学数据分析。结果:CAP10、PAX4、IRS-2、NEUROD1、CDKL1和WFS1共报告了n=11个致病/可能致病变异。在报告的变体CAP10/rs55878652 (C .1990- 7t >C;p.Leu446Pro)和CAP10/rs2975766 (c.1996A>G;发现的p.e ile666val)是新颖的,并且尚未在数据库中报告任何疾病。CAP10/rs7607759 (C . 1510a >G, p.Thr504Ala), PAX4/rs712701 (C . 962a >C;p.His321Pro), PAX4/rs772936097 (c.748-3delT;p.Arg325Trp), IRS-2/rs1805097 (c.3170G>A;p.Gly1057Asp), NEUROD1/rs1801262 (c.133A>G;p.Thr45Ala), CDKL1/rs77152992 (c.1226C>T;p.Pro409Leu), WFS1/rs1801212 (c.997G>A;p.Val333Ile), WFS1/rs1801208 (c.1367G>A;p.Arg456His)和WFS1/rs734312 (c.1832G>A;p.Arg611His)先前在其他种族人群中被发现。我们的研究再次证实了这些变异与巴基斯坦普什图人群中T2D的关联。结论:外显子组测序数据的计算机分析表明,在普什图族人群中,所有(n=11)个已确定的变异与T2D存在统计学上的显著关联。该研究可能为开展旨在揭示T2D相关基因的未来分子研究奠定基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Evaluation of Type 2 Diabetes Risk Variants (Alleles) in the Pashtun Ethnic Population of Pakistan.

Evaluation of Type 2 Diabetes Risk Variants (Alleles) in the Pashtun Ethnic Population of Pakistan.

Evaluation of Type 2 Diabetes Risk Variants (Alleles) in the Pashtun Ethnic Population of Pakistan.

Objective: To evaluate the Type 2 Diabetes (T2D) risk variants in the Pashtun ethnic population of Khyber Pakhtunkhwa using nascent whole-exome sequencing (WES) to better understand the pathogenesis of this complex polygenic disorder.

Methodology: A total of 100 confirmed patients with T2D of Pashtun ethnicity were included in the study, DNA was extracted from whole blood samples, and paired-end libraries were prepared using the Illumina Nextera XT DNA library kit carefully following the manufacturer's instructions. Illumina HiSeq 2000 was used to obtain sequences of the prepared libraries followed by bioinformatics data analysis.

Results: A total of n=11 pathogenic/likely pathogenic variants were reported in the CAP10, PAX4, IRS-2, NEUROD1, CDKL1 and WFS1. Among the reported variants CAP10/rs55878652 (c.1990-7T>C; p.Leu446Pro) and CAP10/rs2975766 (c.1996A>G; p.Ile666Val) identified were novel, and have not yet been reported for any disease in the database.The variants CAP10/rs7607759 (c.1510A>G, p.Thr504Ala), PAX4/rs712701 (c.962A>C; p.His321Pro), PAX4/rs772936097 (c.748-3delT; p.Arg325Trp), IRS-2/rs1805097 (c.3170G>A; p.Gly1057Asp), NEUROD1/rs1801262 (c.133A>G; p.Thr45Ala), CDKL1/rs77152992 (c.1226C>T; p.Pro409Leu), WFS1/rs1801212 (c.997G>A; p.Val333Ile), WFS1/rs1801208 (c.1367G>A; p.Arg456His), and WFS1/rs734312 (c.1832G>A; p.Arg611His) are previously identified in other ethnic populations. Our study reconfirms the associations of these variants with T2D in the Pakistani Pashtun population.

Conclusion: In-silico analysis of exome sequencing data suggests a statistically substantial association of all (n=11) identified variants with T2D in the Pashtun ethnic population. This study may serve as a foundation for performing future molecular studies aimed at unraveling T2D associated genes.

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来源期刊
CiteScore
1.20
自引率
0.00%
发文量
22
审稿时长
8 weeks
期刊介绍: The Journal of the ASEAN Federation of Endocrine Societies (JAFES) is an OPEN ACCESS, internationally peer-reviewed, English language, medical and health science journal that is published in print two times a year by the ASEAN Federation of Endocrine Societies. It shall serve as the endocrine window between the ASEAN region and the world, featuring original papers and publishing key findings from specialists and experts of endocrinology.
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