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Genetic influence on peripheral blood T lymphocyte levels

机译:遗传对外周血T淋巴细胞水平的影响

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摘要

T lymphocytes are a major component of the adaptive immune system. CD4 positive T cell subpopulations regulate a cell and macrophage effector function while CD8 positive T cells are largely responsible for anti-viral cytotoxic activity. The degree of natural variation in the levels and ratios of the various T cell subpopulations is a possible risk factor for the development of autommune disease, infectious disease and cancer. There is some evidence from studies of inbred strains of mice and humans which suggests that variation in T cell subpopulations is genetically influenced. However, family studies alone cannot distinguish between common environmental and shared genetic influences and provide less robust estimates of the heritability than twin studies. To comprehensively examine genetic influences on a selection of important T cell phenotypes, we investigated variation in levels of total lymphocytes, CD3(+), CD4(+), CD8(+), CD3(+)CD4(+), CD3(+)CD8(+) lymphocytes and in CD4:CD8 ratio as a proportion of lymphocytes and of T cells using the classical twin model approach. Healthy female twin pairs were sampled from the St. Thomas' UK Adult Twin Registry. A maximum of 103 monozygotic (MZ) and 186 dizygotic (DZ) twins aged 18-80 years participated in the study. Whole blood samples were analysed for T cell subsets by flow cytometry. The relative genetic contribution to these phenotypes was estimated using a variance components model-fitting approach. Heritability estimates were calculated of 65% for CD4:CD8 T cell and lymphocyte ratios, around 50% for absolute lymphocyte, CD8 and CD4(+) counts, and 56% for CD8(+) numbers. Unique (rather than shared) familial environment explains the remainder of the variance. Genetic factors have a major influence on the variation in peripheral T cell subset numbers. Polymorphism dictating such Variation should be taken into account when assessing risk factors for T cell immune-mediated disease with a genetic background.
机译:T淋巴细胞是适应性免疫系统的主要组成部分。 CD4阳性T细胞亚群调节细胞和巨噬细胞效应子的功能,而CD8阳性T细胞在很大程度上负责抗病毒的细胞毒活性。各种T细胞亚群的水平和比率的自然变化程度是发生自体疾病,传染病和癌症的可能危险因素。从小鼠和人类的近交系的研究中有一些证据表明,T细胞亚群的变异受遗传影响。但是,单靠家庭研究无法区分常见的环境影响和共享的遗传影响,并且无法提供比双基因研究可靠的遗传力估计。为了全面检查遗传因素对选择重要T细胞表型的影响,我们调查了总淋巴细胞,CD3(+),CD4(+),CD8(+),CD3(+)CD4(+),CD3(+)的水平变化CD8(+)淋巴细胞,并使用经典孪生模型方法以CD4:CD8的比例表示淋巴细胞和T细胞的比例。健康的雌性双胞胎对是从圣托马斯英国成人双胞胎登记处取样的。年龄在18-80岁之间的最多103个单卵(MZ)和186双卵(DZ)双胞胎参与了这项研究。通过流式细胞术分析全血样品中的T细胞亚群。使用方差成分模型拟合方法估算了这些表型的相对遗传贡献。对于CD4:CD8 T细胞和淋巴细胞比率,遗传估计估计为65%,绝对淋巴细胞,CD8和CD4(+)计数约为50%,而CD8(+)数目约为56%。独特的(而不是共享的)家庭环境可以解释其余的差异。遗传因素对外周T细胞亚群数量的变化有重大影响。当评估具有遗传背景的T细胞免疫介导疾病的危险因素时,应考虑到指示这种变异的多态性。

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