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肿瘤坏死因子-[FC12]α、白细胞介素-1β、白细胞介素-4受体[FC12]α链、白细胞介素-6和白细胞介素-10基因的遗传变异不是低体重儿败血症的危险因素。

Genetic variants of TNF-[FC12]a, IL-1beta, IL-4 receptor [FC12]a-chain, IL-6 and IL-10 genes are not risk factors for sepsis in low-birth-weight infants.

作者信息

Treszl András, Kocsis István, Szathmári Miklós, Schuler Agnes, Héninger Erika, Tulassay Tivadar, Vásárhelyi Barna

机构信息

Research Laboratory of Pediatrics and Nephrology, Semmelweis University, Budapest, Hungary.

出版信息

Biol Neonate. 2003;83(4):241-5. doi: 10.1159/000069484.

Abstract

The amount of inflammatory cytokines is a major determinant for the development of sepsis in very-low-birth-weight (VLBW) neonates. We investigated whether variants of tumor necrosis factor-alpha, interleukin (IL)-1 beta, IL-4 receptor alpha-chain, IL-6 and IL-10 genes, associated with altered cytokine production, might influence the risk and complications of sepsis in VLBW infants. We determined the presence of these genetic variants in dried blood samples of 33 septic, 35 infected and 35 healthy VLBW neonates by PCR and RFLP methods and analyzed their association with the risk and complications of sepsis. The frequencies of genetic variants did not differ in uninfected and in infected infants with or without sepsis. Moreover, none of the studied complications was associated with carrier state of any of genetic variants. Four of the 5 septic neonates with disseminated intravascular coagulation, however, carried simultaneously the variants of IL-1 beta and IL-10 genes. We concluded that these genetic polymorphisms do not influence the risk and course of sepsis in VLBW neonates.

摘要

炎症细胞因子的量是极低出生体重(VLBW)新生儿发生败血症的主要决定因素。我们研究了与细胞因子产生改变相关的肿瘤坏死因子-α、白细胞介素(IL)-1β、IL-4受体α链、IL-6和IL-10基因的变异是否会影响VLBW婴儿败血症的风险和并发症。我们通过PCR和RFLP方法确定了33例败血症、35例感染和35例健康VLBW新生儿干血样本中这些基因变异的存在情况,并分析了它们与败血症风险和并发症的相关性。未感染以及感染但有或无败血症的婴儿中基因变异的频率没有差异。此外,所研究的并发症均与任何基因变异的携带状态无关。然而,5例发生弥散性血管内凝血的败血症新生儿中有4例同时携带IL-1β和IL-10基因的变异。我们得出结论,这些基因多态性不会影响VLBW新生儿败血症的风险和病程。

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