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白细胞介素-7对新生儿和成人CD4 + T细胞的细胞周期进程及基于HIV-1的载体感染具有不同的调节作用。

IL-7 differentially regulates cell cycle progression and HIV-1-based vector infection in neonatal and adult CD4+ T cells.

作者信息

Dardalhon V, Jaleco S, Kinet S, Herpers B, Steinberg M, Ferrand C, Froger D, Leveau C, Tiberghien P, Charneau P, Noraz N, Taylor N

机构信息

Institut de Génétique Moléculaire de Montpellier, UMR 5535/IFR 22, F34293 Montpellier, France.

出版信息

Proc Natl Acad Sci U S A. 2001 Jul 31;98(16):9277-82. doi: 10.1073/pnas.161272698. Epub 2001 Jul 24.

Abstract

Differences in the immunological reactivity of umbilical cord (UC) and adult peripheral blood (APB) T cells are poorly understood. Here, we show that IL-7, a cytokine involved in lymphoid homeostasis, has distinct regulatory effects on APB and UC lymphocytes. Neither naive nor memory APB CD4(+) cells proliferated in response to IL-7, whereas naive UC CD4(+) lymphocytes underwent multiple divisions. Nevertheless, both naive and memory IL-7-treated APB T cells progressed into the G(1b) phase of the cell cycle, albeit at higher levels in the latter subset. The IL-7-treated memory CD4(+) lymphocyte population was significantly more susceptible to infection with an HIV-1-derived vector than dividing CD4(+) UC lymphocytes. However, activation through the T cell receptor rendered UC lymphocytes fully susceptible to HIV-1-based vector infection. These data unveil differences between UC and APB CD4(+) T cells with regard to IL-7-mediated cell cycle progression and HIV-1-based vector infectivity. This evidence indicates that IL-7 differentially regulates lymphoid homeostasis in adults and neonates.

摘要

人们对脐带血(UC)和成人外周血(APB)T细胞免疫反应性的差异了解甚少。在此,我们发现,参与淋巴细胞内环境稳定的细胞因子白细胞介素-7(IL-7)对APB和UC淋巴细胞具有不同的调节作用。无论是初始型还是记忆型APB CD4(+)细胞都不会因IL-7而增殖,而初始型UC CD4(+)淋巴细胞则会进行多次分裂。然而,经IL-7处理的初始型和记忆型APB T细胞均进入细胞周期的G(1b)期,尽管后者亚群中的水平更高。与正在分裂的CD4(+) UC淋巴细胞相比,经IL-7处理的记忆型CD4(+)淋巴细胞群体对源自HIV-1的载体感染更为敏感。然而,通过T细胞受体激活可使UC淋巴细胞完全易受基于HIV-1的载体感染。这些数据揭示了UC和APB CD4(+) T细胞在IL-7介导的细胞周期进程和基于HIV-1的载体感染性方面的差异。这一证据表明,IL-7对成人和新生儿的淋巴细胞内环境稳定具有不同的调节作用。

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