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Persistent skewing of the T-cell profile in adolescents adopted internationally from institutional care

机译:从机构关怀采用的青少年中T细胞剖面的持续偏移

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The developing immune system is an adaptive system, primed by antigens, responsive to infectious pathogens, and can be affected by other aspects of the early rearing environment, including deviations from the normal provision of parental care. We investigated whether early rearing in an institutional setting, even when followed by years living in supportive and well-resourced families, would be associated with a persistent shift in T cell profiles. Immunophenotyping was used to enumerate CD4 + CD57 + and CD8 + CD57 + subsets, with gating strategies employed to differentiate naive, central-memory, effector-memory, and terminally differentiated EM cells expressing CD45RA (TEMRA). Blood samples were collected from 96 adolescents, and PBMC isolated via Ficol gradient, followed by an optimized immunophenotypic characterization. CMV antibody titers were determined via ELISA. Adopted adolescents had lower CD4/CD8 ratios than did the control adolescents. Early rearing had a significant effect on the T cells, especially the CD8 + CD57 + CM, EM, and TEMRA cells and the CD4 + CD57 + EM cells. Adolescents who had spent their infancy in institutions before adoption were more likely to be seropositive for CMV, with higher antibody titers. CMV antibody titers were significantly correlated with the percentages of all CD8 + CD57 + cell subsets. In the statistical modeling, CMV antibody titer also completely mediated the relationship between institutional exposure and the ratio of CD4-to-CD8 cells, as well as the percentages of CD4 + CD57 + and CD8 + CD57 + subsets. These findings demonstrate that persistent immune differences are still evident even years after adoption by supportive American families. The shift in the T cells was associated with being a latent carrier of CMV and may reflect the role of specific T cell subsets in Herpes virus containment. In older adults, sustained CMV antigen persistence and immunoregulatory containment ultimately contributes to an accumulation of differentiated T cells with a decreased proliferative capacity and to immune senescence.
机译:开发免疫系统是由抗原引发的适应性系统,响应于传染病,并且可能受早期饲养环境的其他方面的影响,包括与正常提供父母护理的偏差。我们调查了是否在机构环境中提前饲养,即使在居住在支持性和资源良好的家庭中的几年时,也会与T细胞谱的持续转变有关。免疫蛋白酶用于枚举CD4 + CD57 +和CD8 + CD57 +亚群,采用用于区分幼稚,中央记忆,效应记忆和表达CD45RA(TEMRA)的末端分化的EM细胞的门控策略。从96个青少年收集血液样品,并通过Ficol梯度分离PBMC,然后优化免疫蛋白酶特征。通过ELISA测定CMV抗体滴度。采用的青少年的CD4 / CD8比率低于对照青少年。早期饲养对T细胞具有显着影响,尤其是CD8 + CD57 + CM,EM和迎膜细胞和CD4 + CD57 + EM细胞。在采用之前花在机构中的青少年更有可能对CMV进行血清阳性,具有更高的抗体滴度。 CMV抗体滴度与所有CD8 + CD57 +细胞亚群的百分比显着相关。在统计学建模中,CMV抗体滴度也完全介导体制暴露与CD4-至CD8细胞的比率之间的关系,以及CD4 + CD57 +和CD8 + CD57 +子集的百分比。这些研究结果表明,持续的免疫差异甚至在通过支持者家庭通过后甚至很明显。 T细胞的偏移与CMV的潜伏载体相关,并且可以反映特定T细胞亚群在病毒遏制中的作用。在老年人中,持续的CMV抗原持久性和免疫调节抑制最终导致分化的T细胞的积累,其增殖能力降低和免疫衰老。

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