接受者的基因R702W NOD2变体与原位肝移植后细菌感染风险增加相关。
Recipient's genetic R702W NOD2 variant is associated with an increased risk of bacterial infections after orthotopic liver transplantation.
作者信息
Janse Marcel, de Rooij Bert-Jan F, van Hoek Bart, van den Berg Arie P, Porte Robert J, Blokzijl Hans, Coenraad Minneke J, Hepkema Bouke G, Schaapherder Alexander F, Ringers Jan, Weersma Rinse K, Verspaget Hein W
机构信息
Department of Gastroenterology and Hepatology, University of Groningen and University Medical Center Groningen, Groningen, The Netherlands.
出版信息
PLoS One. 2013 Aug 19;8(8):e72617. doi: 10.1371/journal.pone.0072617. eCollection 2013.
INTRODUCTION
Orthotopic liver transplantation (OLT) is accompanied by a significant postoperative infection risk. Immunosuppression to prevent rejection increases the susceptibility to infections, mainly by impairing the adaptive immune system. Genetic polymorphisms in the lectin complement pathway of the donor have recently been identified as important risk determinants of clinically significant bacterial infection (CSI) after OLT. Another genetic factor involved in innate immunity is NOD2, which was reported to be associated with increased risk of spontaneous bacterial peritonitis in cirrhotic patients.
METHODS
We assessed association of three genetic NOD2 variants (R702W, G908R and 3020insC) with increased risk of CSI after OLT. 288 OLT recipient-donor pairs from two tertiary referral centers were genotyped for the three NOD2 variants. The probability of CSI in relation to NOD2 gene variants was determined with cumulative incidence curves and log-rank analysis.
RESULTS
The R702W NOD2 variant in the recipient was associated with CSI after OLT. Eight out of 15 (53.3%) individuals with a mutated genotype compared to 80/273 (29.3%) with wild type genotype developed CSI (p=0.027, univariate cox regression), illustrated by a higher frequency of CSI after OLT over time (p=0.0003, log rank analysis). Multivariate analysis (including the donor lectin complement pathway profile) showed independence of this R702W NOD2 association from other risk factors (HR 2.0; p=0.04). The other NOD2 variants, G908R and 3020insC, in the recipient were not associated with CSI. There was no association with CSI after OLT for any of the NOD2 variants in the donor.
CONCLUSION
The mutated NOD2 R702W genotype in the recipient is independently associated with an increased risk of bacterial infections after liver transplantation, indicating a predisposing role for this genetic factor impairing the recipient's innate immune system.
引言
原位肝移植(OLT)术后存在显著的感染风险。用于预防排斥反应的免疫抑制主要通过损害适应性免疫系统来增加感染易感性。最近已确定供体凝集素补体途径中的基因多态性是OLT术后临床上显著细菌感染(CSI)的重要风险决定因素。另一个参与固有免疫的遗传因素是NOD2,据报道它与肝硬化患者自发性细菌性腹膜炎风险增加有关。
方法
我们评估了三种NOD2基因变体(R702W、G908R和3020insC)与OLT术后CSI风险增加之间的关联。对来自两个三级转诊中心的288对OLT受者 - 供者进行了这三种NOD2变体的基因分型。通过累积发病率曲线和对数秩分析确定与NOD2基因变体相关的CSI概率。
结果
受者中的R702W NOD2变体与OLT术后的CSI相关。15名基因型突变个体中有8名(53.3%)发生了CSI,而野生型基因型个体中为80/273(29.3%)(p = 0.027,单变量cox回归),OLT术后随着时间推移CSI频率更高(p = 0.0003,对数秩分析)说明了这一点。多变量分析(包括供体凝集素补体途径概况)显示这种R702W NOD2关联独立于其他风险因素(HR 2.0;p = 0.04)。受者中的其他NOD2变体G908R和3020insC与CSI无关。供体中的任何NOD2变体与OLT术后的CSI均无关联。
结论
受者中突变的NOD2 R702W基因型与肝移植后细菌感染风险增加独立相关,表明该遗传因素对受者固有免疫系统有易患作用。
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