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首页> 外文期刊>European cytokine network >Relation between the tumor necrosis factor-alpha (TNF-alpha) gene and protein expression, and clinical, biochemical, and genetic markers: age, body mass index and uric acid are independent predictors for an elevated TNF-alpha plasma level in a comple
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Relation between the tumor necrosis factor-alpha (TNF-alpha) gene and protein expression, and clinical, biochemical, and genetic markers: age, body mass index and uric acid are independent predictors for an elevated TNF-alpha plasma level in a comple

机译:肿瘤坏死因子-α(TNF-α)基因和蛋白质表达与临床,生化和遗传标记之间的关系:年龄,体重指数和尿酸是完全性TNF-α血浆水平升高的独立预测因子

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摘要

BACKGROUND: Tumor necrosis factor-alpha (TNF-alpha) has been implicated in the pathogenesis of numerous complex diseases. The plasma level of this pro-inflammatory cytokine is associated with a variety of different risk factors, but little is known about the genetic background and the complex interactions. METHODS: in this clinical study, correlations were studied between plasma levels of circulating TNF-alpha protein (ELISA), its mRNA expression in monocytes (RT-PCR) and genetic variants of TNF-alpha gene (SSCP), with several diseases, including obesity, atherosclerosis, diabetes mellitus, hypertension, as well as risk factors such as age, gender, inflammatory markers, the coagulationibrinolysis balance, and lipid metabolism. One hundred and ninety four clinically and biochemically well-characterized patients were enrolled. RESULTS: At the transcriptional level, measured in monocytes, no association with any clinical or biochemical parameter investigated was found, including TNF-alpha protein level.Investigating the influence of genetic variants of the TNF-alpha gene on mRNA and protein levels, only one promoter polymorphism, namely c.-238G > A, was shown to be associated with transcriptional but not with translational expression. However, at the translational level, significant positive, but weak associations were determined for obesity (P -/+ 0.037), age (P -/+ 0.038), uric acid (P < 0.001), body mass index (P -/+ 0.01), plasminogen (P -/+ 0.013), and fibrinogen (P -/+ 0.002) in bivariate regression analyses, whereas HDL-cholesterol (P -/+ 0.005) was shown to be negatively correlated. However, investigating confounding effects in stepwise multivariate regression analysis, body mass index (P -/+ 0.009), uric acid (P -/+ 0.026) and age (P -/+ 0.037) turned out to be significantly associated with plasma levels of circulating TNF-alpha (adjusted R(2) -/+ 0.117; SE: 0.688).
机译:背景:肿瘤坏死因子-α(TNF-alpha)已牵涉到许多复杂疾病的发病机理。这种促炎性细胞因子的血浆水平与多种不同的危险因素有关,但对遗传背景和复杂的相互作用知之甚少。方法:在这项临床研究中,研究了血浆循环TNF-α蛋白(ELISA)水平,其在单核细胞中的mRNA表达(RT-PCR)和TNF-alpha基因的遗传变异(SSCP)之间的相关性,包括以下几种疾病:肥胖,动脉粥样硬化,糖尿病,高血压以及诸如年龄,性别,炎症标记,凝血/纤维蛋白溶解平衡和脂质代谢等危险因素。入选了194例临床和生化良好的患者。结果:在单核细胞中测量的转录水平上,未发现与包括TNF-α蛋白水平在内的任何临床或生化指标相关联。调查TNF-α基因的遗传变异对mRNA和蛋白水平的影响启动子多态性,即c.-238G> A,被证明与转录相关,但与翻译表达无关。然而,在翻译水平上,肥胖(P-/ + 0.037),年龄(P-/ + 0.038),尿酸(P <0.001),体重指数(P-/ +)被确定为显着的阳性但弱关联。在双变量回归分析中,血浆纤溶酶原(P-/ + 0.013)为0.01),纤维蛋白原(P-/ + 0.002),而HDL-胆固醇(P-/ + 0.005)呈负相关。但是,在逐步多元回归分析,体重指数(P-/ + 0.009),尿酸(P-/ + 0.026)和年龄(P-/ + 0.037)方面研究混杂效应与血浆血浆水平显着相关。循环TNF-alpha(调整后的R(2)-/ + 0.117; SE:0.688)。

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