细胞因子组合对初始和记忆静止T细胞的抗原非依赖性激活。
Antigen-independent activation of naive and memory resting T cells by a cytokine combination.
作者信息
Unutmaz D, Pileri P, Abrignani S
机构信息
Immunobiology Research Institute Siena, Italy.
出版信息
J Exp Med. 1994 Sep 1;180(3):1159-64. doi: 10.1084/jem.180.3.1159.
Abstract
We investigated whether human resting T cells could be activated to proliferate and display effector function in the absence of T cell receptor occupancy. We report that combination of interleukin 2 (IL-2), tumor necrosis factor alpha, and IL-6 activated highly purified naive (CD45RA+) and memory (CD45RO+) resting CD4+ T cells to proliferate. Under this condition, memory resting T cells could also display effector function as measured by lymphokine synthesis and help for immunoglobulin production by B cells. This novel Ag-independent pathway of T cell activation may play an important role in vivo in recruiting effector T cells at the site of immune response and in maintaining the clonal size of memory T cells in the absence of antigenic stimulation. Moreover, cytokines can induce proliferation of naive T cells without switch to memory phenotype and this may help the maintenance of the peripheral pool of naive T cells.
摘要
我们研究了在不存在T细胞受体占据的情况下,人类静息T细胞是否能够被激活以进行增殖并发挥效应功能。我们报告称,白细胞介素2(IL-2)、肿瘤坏死因子α和IL-6的组合可激活高度纯化的初始(CD45RA +)和记忆(CD45RO +)静息CD4 + T细胞进行增殖。在此条件下,记忆静息T细胞也可发挥效应功能,这可通过淋巴因子合成以及对B细胞产生免疫球蛋白的辅助作用来衡量。这种新的T细胞激活的非抗原依赖性途径可能在体内免疫反应部位募集效应T细胞以及在缺乏抗原刺激时维持记忆T细胞的克隆大小方面发挥重要作用。此外,细胞因子可诱导初始T细胞增殖而不转变为记忆表型,这可能有助于维持初始T细胞的外周库。
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