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Evaluation of CD86 gene polymorphism at +1057 position in liver transplant recipients.

机译:肝移植受者中+1057位CD86基因多态性的评估。

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BACKGROUND: Efficient T cell-APC interaction requires the participation of primary and co-stimulatory signals. The main co-stimulatory pathway involves the interaction of CD80 and CD86, expressed on the APCs, with their T cell counter-receptor, CD28 and CTLA-4. Recently, a G to A transition has been described at position +1057 of the CD86 gene, located in their cytoplasmic tail. METHODS: CD86 polymorphism was analyzed by sequence based typing in DNA samples obtained from 205 liver transplant recipients. Acute rejection and chronic rejection were diagnosed based upon conventional clinical, biochemical and histological criteria. RESULTS: The study of CD86 +1057 (G/A) polymorphism revealed that recipients bearing the A allele or the AA genotype have a reduced risk of acute rejection. In fact, the AA genotype was absent in the group of patients showing acute rejection episodes, whereas its frequency in those patients without acute rejection episodes was 8.8% (P=0.009, OR=0.07). This polymorphism did not reveal any association with the incidence of chronic rejection, but patients bearing the AA genotype showed a higher graft survival rate (83.3%) than those bearing the GA genotype (49.3%) or GG genotype (56.5%). CONCLUSIONS: The results of the present report suggest that the CD86 AA genotype at +1057 position could be involved in liver transplant acceptance, given that its presence is related to a decrease of acute rejection frequency and to a graft survival increase.
机译:背景:有效的T细胞-APC相互作用需要初级和共刺激信号的参与。主要的共刺激途径涉及在APC上表达的CD80和CD86与它们的T细胞反受体CD28和CTLA-4的相互作用。最近,在其细胞质尾部的CD86基因的+1057位置已描述了从G到A的转变。方法:通过对来自205位肝移植受者的DNA样本进行基于序列的分型,分析CD86多态性。根据常规的临床,生化和组织学标准诊断为急性排斥反应和慢性排斥反应。结果:对CD86 +1057(G / A)多态性的研究表明,带有A等位基因或AA基因型的接受者的急性排斥反应风险降低。实际上,在显示急性排斥反应发作的患者组中不存在AA基因型,而在没有急性排斥反应发作的患者中,AA基因型的频率为8.8%(P = 0.009,OR = 0.07)。这种多态性并未显示出与慢性排斥反应的发生有任何关联,但是具有AA基因型的患者的移植物存活率(83.3%)高于具有GA基因型(49.3%)或GG基因型(56.5%)的患者。结论:本报告的结果表明,在+1057位置的CD86 AA基因型可能参与肝移植的接受,因为它的存在与急性排斥反应频率的降低和移植物存活的增加有关。

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