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Infantile hypertrophic pyloric stenosis: evaluation of three positional candidate genes, TRPC1, TRPC5 and TRPC6, by association analysis and re-sequencing

机译:婴儿肥厚性幽门狭窄:通过关联分析和重新测序评估三个位置候选基因TRPC1,TRPC5和TRPC6

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摘要

Infantile hypertrophic pyloric stenosis (IHPS) is the most common inherited form of gastrointestinal obstruction in infancy with a striking male preponderance. Infants present with vomiting due to gastric outlet obstruction caused by hypertrophy of the smooth muscle of the pylorus. Two loci specific to extended pedigrees displaying autosomal dominant inheritance have been identified. A genome scan identified loci on chromosomes 11q14–q22 and Xq23–q24 which are predicted to be responsible for a subset of smaller families with IHPS demonstrating non-Mendelian inheritance. The two linked chromosomal regions both harbour functional candidate genes which are members of the canonical transient receptor potential (TRPC) family of ion channels. Both TRPC5 (Xq23–q24) and TRPC6 (11q14–q22) have a potential role in smooth muscle control and hypertrophy. Here, we report suggestive evidence for a third locus on chromosome 3q12–q25 (Z max = 2.7, p < 0.004), a region which harbours a third TRPC gene, TRPC1. Fine mapping of all three genes using a tagSNP approach and re-sequencing identified a SNP in the promoter region of TRPC6 and a missense variant in exon 4 of TRPC6 which may be putative causal variants.
机译:婴儿肥厚性幽门狭窄(IHPS)是婴儿期胃肠道阻塞的最常见遗传形式,男性占优势。婴儿因幽门幽门平滑肌肥大引起胃出口阻塞而出现呕吐。已确定了两个特定于扩展谱系的位点,它们显示了常染色体显性遗传。基因组扫描确定了染色体11q14–q22和Xq23–q24上的基因座,这些基因座预计与较小的IHPS家族的子集有关,表现出非孟德尔遗传。两个连接的染色体区域均包含功能候选基因,这些功能候选基因是离子通道的标准瞬时受体电位(TRPC)家族的成员。 TRPC5(Xq23–q24)和TRPC6(11q14–q22)在平滑肌控制和肥大中均具有潜在作用。在这里,我们报告了第3个染色体3q12–q25上第三个基因座的暗示证据(Z max = 2.7,p <0.004),该区域带有第三个TRPC基因TRPC1。使用tagSNP方法对所有三个基因进行精细定位并进行重新测序,确定了TRPC6启动子区域中的SNP和TRPC6外显子4中的错义变体,这可能是推定的因果变体。

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