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韩国和日本患者下颌前突的全基因组连锁分析。

Genome-wide linkage analysis of mandibular prognathism in Korean and Japanese patients.

作者信息

Yamaguchi T, Park S B, Narita A, Maki K, Inoue I

机构信息

Department of Orthodontics, School of Dentistry, Showa University, 2-1-1 Kitasenzoku, Outa-ku, Tokyo 145-8515, Japan.

出版信息

J Dent Res. 2005 Mar;84(3):255-9. doi: 10.1177/154405910508400309.

Abstract

The existence of familial aggregation of mandibular prognathism (MP) suggests that genetic components play an important role in its etiology. In this study, a genome-wide linkage analysis to identify loci susceptible to MP was conducted with 90 affected sibling-pairs in 42 families, comprised of 40 Korean sibling-pairs and 50 Japanese sibling-pairs. Two non-parametric linkage analyses, GENEHUNTER-PLUS and SIBPAL, were applied and detected nominal statistical significance of linkage to MP at chromosomes 1p36, 6q25, and 19p13.2. The best evidence of linkage was detected near D1S234 (maximum Z(lr) = 2.51, P = 0.0012). In addition, evidence of linkage was observed near D6S305 (maximum Z(lr) = 2.23, P = 0.025) and D19S884 (maximum Z(lr) = 1.93, P = 0.0089). Identification of the susceptible genes in the linkage regions will pave the way for insights into the molecular pathways that cause MP, especially overgrowth of the mandible, and may lead to the development of novel therapeutic tools.

摘要

下颌前突(MP)的家族聚集性表明遗传因素在其病因中起着重要作用。在本研究中,对42个家庭中的90对患病同胞进行了全基因组连锁分析,以确定易患MP的基因座,其中包括40对韩国同胞和50对日本同胞。应用了两种非参数连锁分析方法GENEHUNTER-PLUS和SIBPAL,在1p36、6q25和19p13.2染色体上检测到与MP连锁的名义统计学显著性。在D1S234附近检测到最强的连锁证据(最大Z(lr)=2.51,P=0.0012)。此外,在D6S305附近(最大Z(lr)=2.23,P=0.025)和D19S884附近(最大Z(lr)=1.93,P=0.0089)也观察到连锁证据。确定连锁区域中的易感基因将为深入了解导致MP的分子途径,尤其是下颌骨过度生长,铺平道路,并可能导致新型治疗工具的开发。

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