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生存素基因启动子多态性-31G/C作为牙源性角化囊性瘤发生的危险因素。

Survivin gene promoter polymorphism -31G/C as a risk factor for keratocystic odontogenic tumor development.

作者信息

Andric Miroslav, Nikolic Nađa, Boskovic Marija, Milicic Biljana, Skodric Sanja, Basta Jovanovic Gordana, Milasin Jelena

机构信息

University of Belgrade, School of Dentistry, Clinic of Oral Surgery, Belgrade, Serbia.

出版信息

Eur J Oral Sci. 2012 Feb;120(1):9-13. doi: 10.1111/j.1600-0722.2011.00919.x.

Abstract

Several single nucleotide polymorphisms in survivin gene promoters, notably -31G/C, have been shown to modulate the expression and activity of the survivin protein. Consequently, the -31G/C polymorphism has been identified as a risk factor for the development of several types of tumors. The aim of this study was to investigate a possible association between the -31G/C polymorphism and the risk for keratocystic odontogenic tumor (KCOT) development. DNA from 52 biopsy specimens of KCOTs and from 82 buccal swabs of healthy individuals was subjected to PCR restriction fragment length polymorphism analysis to identify individual genotypes. The distribution of genotypes in KCOT and control groups, respectively, was: GG: 30 (57.7%) vs. 26 (31.7%); CG: 17 (32.7%) vs. 45 (54.9%); and CC: 5 (9.6%) vs. 11 (13.4%), respectively. These differences were statistically significant. The G allele was more common in the KCOT group than in the control group: 76 (74%) vs. 96 (59%), respectively. Logistic regression analysis showed that GC heterozygotes had a considerably decreased susceptibility for KCOTs compared with GG homozygotes. The same was true for GC+CC vs. GG. The GG genotype of the -31G/C polymorphism might be a risk factor for KCOT development.

摘要

生存素基因启动子中的几个单核苷酸多态性,尤其是-31G/C,已被证明可调节生存素蛋白的表达和活性。因此,-31G/C多态性已被确定为几种类型肿瘤发生的危险因素。本研究的目的是调查-31G/C多态性与牙源性角化囊性瘤(KCOT)发生风险之间的可能关联。对52例KCOT活检标本和82例健康个体的颊拭子DNA进行聚合酶链反应-限制性片段长度多态性分析,以确定个体基因型。KCOT组和对照组的基因型分布分别为:GG:分别为30例(57.7%)和26例(31.7%);CG:分别为17例(32.7%)和45例(54.9%);CC:分别为5例(9.6%)和11例(13.4%)。这些差异具有统计学意义。G等位基因在KCOT组中比在对照组中更常见:分别为76例(74%)和96例(59%)。逻辑回归分析表明,与GG纯合子相比,GC杂合子患KCOT的易感性显著降低。GC+CC与GG相比也是如此。-31G/C多态性的GG基因型可能是KCOT发生的危险因素。

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