TLR4基因变异影响创伤后器官衰竭和休克的风险:一项队列研究

S. Shalhub, C. Junker, S. Imahara, M. Mindrinos, S. Dissanaike, G. O’Keefe
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引用次数: 50

摘要

遗传变异与败血症的风险和结果有关。我们试图确定炎症相关基因的变异是否与创伤患者脓毒症的严重程度有关。方法对一组严重损伤的高加索患者进行研究,并对候选单核苷酸多态性(snp)进行基因分型。包括toll样受体4 (TLR4) A896G、肿瘤坏死因子- α G-308A、白细胞介素-6 G-174C、白细胞介素-1 β C-31T和分化标记簇14C-159T。采用chi2和logistic回归分析脓毒症及合并脓毒症患者的SNP基因型。随后检测了TLR4基因中6个单倍型标记snp,分析其对TLR4 A896G snp与脓毒症严重程度关系的影响。结果共入组598例患者。147例(25%)并发脓毒症。调整独立危险因素后,携带变异TLR4 896 G等位基因与并发症脓毒症的风险降低相关(优势比为0.3,95%可信区间为0.1-0.7,p = 0.008)。此外,两种单倍型似乎比变异的TLR4 896G等位基因更好地表征了这种风险。变体TLR4 896G等位基因与一种常见的单倍型相关联,这似乎大大降低了复杂败血症的风险。(aOR = 0.2 95%置信区间,0.05 ~ 0.7,p = 0.01)。结论TLR4基因变异与创伤后脓毒症的严重程度有关。这种风险可能不仅仅与TLR4 A896G SNP有关。TLR4基因的其他未表征的变异可能导致败血症的严重程度。需要对TLR4基因的变异性进行全面评估,以确定败血症的风险。
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Variation in the TLR4 gene influences the risk of organ failure and shock posttrauma: a cohort study.
BACKGROUND Genetic variation contributes to risk and outcomes of sepsis. We sought to determine whether variation in inflammation related genes is associated with severity of sepsis in trauma patients. METHODS A cohort of severely injured Caucasian patients was studied and genotyped for candidate single nucleotide polymorphisms (SNPs). These were toll-like receptor 4 (TLR4) A896G, tumor necrosis factor-alpha G-308A, interleukin-6 G-174C, interleukin-1beta C-31T, and cluster of differentiation marker 14C-159T. SNP genotypes among patients with sepsis and complicated sepsis were analyzed by chi2 and logistic regression. Six haplotype-tagging SNPs in the TLR4 gene were subsequently examined to analyze their influence on TLR4 A896G SNPs relationship to sepsis severity. RESULTS We enrolled 598 patients. Complicated sepsis developed in 147 (25%). Adjusting for independent risk factors, carriage of the variant TLR4 896 G allele was associated with decreased risk of complicated sepsis (odds ratio = 0.3, 95% confidence interval, 0.1-0.7, p = 0.008). Furthermore, two haplotypes seemed to better characterize this risk than the variant TLR4 896G allele. The variant TLR4 896G allele is linked to one common haplotype, which seems to confer a considerably reduced risk of complicated sepsis. (aOR = 0.2 95% confidence interval, 0.05-0.7, p = 0.01). CONCLUSIONS Variation within TLR4 gene is associated with severity of posttraumatic sepsis. This risk may not be solely related to TLR4 A896G SNP. It is likely that other, uncharacterized variations in the TLR4 gene contribute to sepsis severity. A thorough evaluation of variability within the TLR4 gene is needed to characterize sepsis risk.
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