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The impact of interleukin-10 (IL-10) gene 4 polymorphisms on peripheral blood IL-10 variation and prostate cancer risk based on published studies

机译:基于已发表研究的白细胞介素10(IL-10)基因4多态性对外周血IL-10变异和前列腺癌风险的影响

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摘要

This study purported to investigate the impact of interleukin-10 (IL-10) gene 4 polymorphisms (−1082G>A, -819T>C, -592A>C and 210T>C) on peripheral blood IL-10 variation and prostate cancer (PCa) risk, with a special consideration given to various origins of between-study heterogeneity. 2 researchers independently fulfilled literature retrieval, quality assessment and information collection. Sub-grouped analyses per ethnicity, continent, design type, control source, genotyping procedure, genotype validation, age-matched status, study sample size, quality score and controls’ mean age were conducted, respectively. Total 17 unduplicated studies (patients/controls: 7561/8101) were assessable for PCa risk, and 4 unduplicated studies (1189 subjects) for peripheral blood IL-10 variation. Pooling all assessable studies identified a marginally significant association between the -1082A allele and increased PCa risk (odds ratio (OR)=1.10, 95% confidence interval [CI]: 1.00 to 1.21) (Heterogeneity I2=64.3%), and no significance was detected in sub-grouped analyses of this polymorphism. Contrastingly, the -592C allele was significantly associated with reduced PCa risk in both prospective (OR=0.85, 95% CI: 0.77 to 0.95) and population-based (OR=0.92, 95% CI: 0.84 to 1.00) studies (Heterogeneity I2=0.0% and 18.1%). Moreover, carriers of combined -592CA/CC genotypes had a significant higher level of peripheral blood IL-10 than the -592AA genotype carriers (weighted mean difference=0.45 and 0.54 mg/dL, 95% CI: 0.23 to 0.67 and 0.30 to 0.39). The above comparisons possessed a low probability of publication bias. In sum, our findings suggested that IL-10 gene -592A>C polymorphism may represent a promising candidate locus for the occurrence of PCa, and further signified a contributing role of this polymorphism in prostate carcinogenesis.
机译:这项研究旨在调查白介素10(IL-10)基因4多态性(−1082G> A,-819T> C,-592A> C和210T> C)对外周血IL-10变异和前列腺癌的影响( PCa)风险,并特别考虑研究之间异质性的各种来源。 2名研究人员独立完成文献检索,质量评估和信息收集。分别按种族,大陆,设计类型,对照来源,基因分型程序,基因型验证,年龄匹配状态,研究样本量,质量得分和对照的平均年龄进行了分组分析。共有17项不重复的研究(患者/对照:7561/8101)可评估PCa风险,4项不重复的研究(1189名受试者)评估外周血IL-10的变化。汇总所有可评估的研究,发现-1082A等位基因与PCa风险增加之间存在边际显着关联(几率(OR)= 1.10,95%置信区间[CI]:1.00至1.21)(异构性I 2 = 64.3%),并且在该多态性的分组分析中未检测到显着性。相反,在前瞻性研究(OR = 0.85,95%CI:0.77至0.95)和基于人群的研究(OR = 0.92,95%CI:0.84至1.00)中,-592C等位基因与PCa风险降低显着相关(异质性I 2 = 0.0%和18.1%)。此外,组合的-592CA / CC基因型携带者比-592AA基因型携带者具有更高的外周血IL-10水平(加权平均差异= 0.45和0.54 mg / dL,95%CI:0.23至0.67和0.30至0.39 )。上述比较具有较低的发表偏见可能性。总之,我们的发现提示IL-10基因-59​​2A> C多态性可能代表PCa发生的有希望的候选基因座,并进一步表明该多态性在前列腺癌发生中的作用。

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