两种肿瘤坏死因子基因多态性在早发性脓毒症早产儿中的患病率。

Biology of the neonate Pub Date : 2006-01-01 Epub Date: 2006-05-29 DOI:10.1159/000093605
A C Schueller, A Heep, E Kattner, M Kroll, M Wisbauer, J Sander, P Bartmann, F Stuber
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引用次数: 32

摘要

背景:肿瘤坏死因子(TNF)是脓毒症的中心介质。肿瘤坏死因子位点内的NcoI多态性已被描述为成年脓毒症患者死亡率的预后标志物。目的:探讨2种TNF基因多态性在早产儿中的基因型及等位基因分布。方法:采用双盲回顾性队列研究,采用A组(含32 + 0孕周早产儿67例)对储存的Guthrie血液抽血卡进行研究。研究人群的基因型和等位基因分布也与健康成年志愿者的参照组进行了比较(n = 252的tnf - β NcoI和n = 233的tnf - α启动子)。采用聚合酶链反应(PCR)分析tnf - α启动子-308区域和tnf - β基因NcoI位点的多态性,然后进行熔化曲线分析或NcoI消化。各组间比较采用Hardy-Weinberg平衡估计。结果:tnf - α -308的总等位基因频率和基因型分布以及tnf - β基因的NcoI多态性与对照组相当。结论:本研究结果提示,所分析的TNF基因多态性均不能作为脓毒症高危早产儿的预后指标。
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Prevalence of two tumor necrosis factor gene polymorphisms in premature infants with early onset sepsis.

Background: Tumor necrosis factor (TNF) is a central mediator of sepsis. The NcoI polymorphism within the TNF locus has been described as a prognostic marker for mortality in adult patients with sepsis.

Objectives: The aim of our study was to investigate the genotype and allele distribution of 2 TNF gene polymorphisms in preterm infants <32 weeks of gestational age, who developed early-onset sepsis.

Methods: A double-blinded retrospective cohort study was carried out on stored Guthrie blood spot cards with group A including 67 premature infants <32 weeks of gestational age with proven early-onset sepsis and group B including 102 healthy newborn infants (>32 + 0 weeks of gestation). The genotype andallele distribution of the study population were also compared to reference groups of healthy adult volunteers (n = 252 for TNF-beta NcoI and n = 233 for -308 TNF-alpha promoter). Polymorphisms of the TNF-alpha promoter -308 region and the NcoI site of the TNF-beta gene were assessed using PCR followed by melting curve analysis or NcoI digestion. The groups were compared by estimation of Hardy-Weinberg equilibrium.

Results: The overall allele frequency and genotype distribution of the -308 TNF-alpha and NcoI polymorphism of the TNF-beta gene were comparable to the values found in the controls.

Conclusion: The study results suggest that none of the analyzed TNF gene polymorphisms may serve as a prognostic marker for preterm infants at high risk of sepsis.

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