| Literature DB >> 34047934 |
Yanghui Chen1,2, Yang Sun1,2, Zongzhe Li1,2, Chenze Li1,2, Lei Xiao1,2, Jiaqi Dai1,2, Shiyang Li1,2,3, Hao Liu1,2, Dong Hu1,2, Dongyang Wu1,2, Senlin Hu1,2, Bo Yu1,2, Peng Chen1,2, Ping Xu4, Wei Kong5, Dao Wen Wang6,7.
Abstract
Thoracic aortic dissection (TAD) without familial clustering or syndromic features is known as sporadic TAD (STAD). So far, the genetic basis of STAD remains unknown. Whole exome sequencing was performed in 223 STAD patients and 414 healthy controls from the Chinese Han population (N = 637). After population structure and genetic relationship and ancestry analyses, we used the optimal sequence kernel association test to identify the candidate genes or variants of STAD. We found that COL3A1 was significantly relevant to STAD (P = 7.35 × 10-6) after 10 000 times permutation test (P = 2.49 × 10-3). Moreover, another independent cohort, including 423 cases and 734 non-STAD subjects (N = 1157), replicated our results (P = 0.021). Further bioinformatics analysis showed that COL3A1 was highly expressed in dissected aortic tissues, and its expression was related to the extracellular matrix (ECM) pathway. Our study identified a profile of known heritable TAD genes in the Chinese STAD population and found that COL3A1 could increase the risk of STAD through the ECM pathway. We wanted to expand the knowledge of the genetic basis and pathology of STAD, which may further help in providing better genetic counseling to the patients.Entities:
Keywords: case-control study; exome sequencing; extracellular matrix; gene COL3A1; sporadic thoracic aortic dissection
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Year: 2021 PMID: 34047934 DOI: 10.1007/s11684-020-0826-1
Source DB: PubMed Journal: Front Med ISSN: 2095-0217 Impact factor: 4.592