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GSTO2(N142D)基因多态性对急性肾排斥反应的影响。

Influence of GSTO2 (N142D) genetic polymorphism on acute renal rejection.

机构信息

Department of Biology, College of Sciences, Shiraz University, 71454, Shiraz, Iran.

出版信息

Mol Biol Rep. 2013 Aug;40(8):4857-60. doi: 10.1007/s11033-013-2584-5. Epub 2013 May 7.

Abstract

Acute renal allograft rejection remains an important problem following kidney transplantation. Several immunological and non-immunological factors intervene in renal graft rejection. Glutathione S-transferase super family is one of the important enzymes for biotransformation of both exogenous and endogenous xenobiotic compounds such as immunosuppressive drugs. The new class of this family is omega that includes two subunits GSTO1 and GSTO2. In this study 282 samples were collected from renal recipients of Namazi hospital in Shiraz-Iran during 2007-2010 years. Also 300 healthy samples as control group were collected from Shiraz population, included in our study. The primary outcome of this study was defined as biopsy-proven acute rejection during 1 year of renal transplantation. We applied polymerase chain reaction-restriction fragment length polymorphism method for determination of GSTO2 N142D polymorphism. Our result showed no significant association between GSTO2 polymorphism and acute rejection. Also this genetic variant has no significant effect with the risk of end stage renal disease. Cadaveric donor type for acute rejection significantly differed between acute rejection and non acute rejection patients (P=0.004). The combination effect of donor type and GSTO2 polymorphism indicates DD genotype with cadaver donor type increase risk of acute rejection (OR=3.82, 95% CI 1.80-12.37, P=0.02).

摘要

肾移植后急性肾移植排斥仍是一个重要问题。 几种免疫和非免疫因素介入肾移植物排斥。 谷胱甘肽 S-转移酶超级家族是生物转化外源性和内源性异源化合物(如免疫抑制剂)的重要酶之一。 该家族的新类别是ω,包括两个亚基 GSTO1 和 GSTO2。 在这项研究中,2007-2010 年间从伊朗 Shiraz 的 Namazi 医院的肾受者收集了 282 个样本。 还从 Shiraz 人群中收集了 300 个健康样本作为对照组,包括在我们的研究中。 本研究的主要结果定义为肾移植后 1 年内活检证实的急性排斥反应。 我们应用聚合酶链反应 - 限制性片段长度多态性方法确定 GSTO2 N142D 多态性。 我们的结果表明 GSTO2 多态性与急性排斥反应之间没有显著关联。 此外,这种遗传变异与终末期肾病的风险没有显著影响。 急性排斥反应和非急性排斥反应患者之间的供体类型存在显著差异(P=0.004)。 供体类型和 GSTO2 多态性的组合效应表明 DD 基因型与尸体供体类型增加急性排斥反应的风险(OR=3.82,95%CI 1.80-12.37,P=0.02)。

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