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TRPV6variants confer susceptibility to chronic pancreatitis in the Chinese population

机译:TRPV6 Variants赋予中国人口慢性胰腺炎的敏感性

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Chronic pancreatitis (CP) is a progressive fibroinflammatory syndrome of the pancreatic tissue caused by genetic and environmental factors. Previously reported susceptibility genes in CP explain less than half of the apparent heritability. To uncover novel pathogenic mechanisms, we initially performed low-coverage whole-genome sequencing on 464 Chinese CP patients and 504 controls. The transient receptor potential cation channel, Subfamily V, Member 6 (TRPV6) gene was found to be significantly associated with CP after a burden test of aggregated rare nonsynonymous variants with a combined annotation dependent depletion score > 20 (p = .020). In the replication stage, we analyzed the entire coding sequence and exon/intron boundaries of theTPRV6gene by Sanger sequencing in another 205 patients with CP and 105 controls. Integration of the findings from the two stages resulted in the identification of 25TRPV6variants: 1 rare nonsense variant, 20 rare missense variants, and 4 common missense variants. Loss-of-function variants, as determined by intracellular Ca(2+)concentration in transfected HEK293T cells, were significantly overrepresented in patients as compared to controls (9/669 [1.35%] vs. 1/609 [0.16%]; odds ratio = 8.29;p = .022). This study provides evidence suggesting thatTRPV6is a novel susceptibility gene for CP.
机译:慢性胰腺炎(CP)是由遗传和环境因素引起的胰腺组织的渐进纤维炎综合征。先前报告的CP中的易感性基因解释了不到一半的表观遗传性。为了发现新的致病机制,我们最初在464例中国CP患者和504例对照中进行了低覆盖的全基因组测序。瞬时受体潜在阳离子通道,亚家族V,成员6(TRPV6)基因被发现与CP之后CP与CP的聚集稀有的非纯变种的负担依赖性耗尽分数> 20(P = .020)进行了显着相关。在复制阶段,通过另外205例CP和105次对照,通过Sanger测序分析了ThetPrv6庚烯的整个编码序列和外显子/内外界。从两个阶段的整合结果导致鉴定25TRPV6变异:1稀有的非阵容,20个罕见的畸形变种,以及4个常见的畸形变种。通过转染的HEK293T细胞中的细胞内Ca(2+)浓度确定的函数变体,与对照组(9/669 [1.35%]与1/609 [0.16%];赔率比率= 8.29; p = .022)。本研究提供了证据表明TheTrpv6是CP的新型易感基因。

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