Determination of the chromosomal location and genomic structure of the Hedgehog-Interacting Protein gene, and analysis of its role in Holoprosencephaly

Gene Function & Disease Pub Date : 2001-08-17 DOI:10.1002/1438-826X(200010)1:3/4<119::AID-GNFD119>3.0.CO;2-K

Liang Huo, Erich Roessler, Amalia Dutra, Pao-Tien Chuang, A. P. McMahon, Maximilian Muenke

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引用次数: 2

Abstract

Hedgehog-Interacting Protein (HIP) is a novel component of the Sonic Hedgehog (SHH) signaling pathway. Recently, defects in this pathway have been shown to cause holoprosencephaly (HPE), which is the most common birth defect of the brain and face in humans. In animal models knockout mice with homozygous null mutations for Shh displayed abnormalities consistent with HPE. Hip has been shown to function as a co-receptor and attenuate Hedgehog signaling by cell-surface binding of the Hedgehog protein and is hypothesized to act as part of a negative regulatory feedback loop. Although Hip is an important factor in the Shh signaling pathway, its potential role in HPE had not been examined in humans. Here, we report the complete gene structure of the human HIP gene and present its mutational analysis in HPE patients. No mutations were found either in the entire coding region or 1 kb upstream of the transcriptional start site (representing the putative promotor) suggesting this gene may not be involved in HPE pathogenesis.

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刺猬相互作用蛋白基因的染色体定位和基因组结构的确定及其在前脑畸形中的作用分析

刺猬相互作用蛋白(HIP)是Sonic Hedgehog (SHH)信号通路的一个新组成部分。最近，这一通路的缺陷已被证明会导致无前脑畸形(HPE)，这是人类大脑和面部最常见的出生缺陷。在动物模型中，Shh纯合子零突变的敲除小鼠表现出与HPE一致的异常。Hip已被证明是一种共受体，通过与Hedgehog蛋白的细胞表面结合来减弱Hedgehog信号，并被假设为负调节反馈回路的一部分。虽然Hip是Shh信号通路中的一个重要因子，但其在人类HPE中的潜在作用尚未得到研究。在这里，我们报道了人类HIP基因的完整基因结构，并介绍了其在HPE患者中的突变分析。在整个编码区或转录起始位点上游1kb处(代表假定的启动子)均未发现突变，这表明该基因可能与HPE发病机制无关。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Gene Function & Disease

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