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MHC II类分子对于新产生的CD4+ T细胞的存活并非必需,但会影响它们的长期寿命。

MHC class II molecules are not required for survival of newly generated CD4+ T cells, but affect their long-term life span.

作者信息

Takeda S, Rodewald H R, Arakawa H, Bluethmann H, Shimizu T

机构信息

Basel Institute for Immunology, Switzerland.

出版信息

Immunity. 1996 Sep;5(3):217-28. doi: 10.1016/s1074-7613(00)80317-9.

Abstract

We grafted fetal thymi from wild-type mice into immunodeficient RAG-2-/- or class II-/-RAG-2-/- (class II MHC-) recipients and followed the fate of naive CD4+ T cells derived from the grafts. In both types of recipients, newly generated CD4+ T cells proliferated to the same extent in the periphery and rapidly filled the empty T cell compartment. However, CD4+ T cells in class II- recipients gradually decreased in number over 6 months. These results show that interactions between the TCR and class II molecules are not required for newly generated CD4+ T cells to survive and proliferate, but are necessary to maintain the size of the peripheral T cell pool for extended periods.

摘要

我们将野生型小鼠的胎胸腺移植到免疫缺陷的RAG-2-/-或II类-/-RAG-2-/-(II类MHC-)受体中,并追踪源自移植胸腺的初始CD4+T细胞的命运。在这两种类型的受体中,新产生的CD4+T细胞在外周血中以相同程度增殖,并迅速填充空的T细胞区室。然而,II类-受体中的CD4+T细胞数量在6个月内逐渐减少。这些结果表明,新产生的CD4+T细胞存活和增殖不需要TCR与II类分子之间的相互作用,但对于长期维持外周T细胞库的大小是必要的。

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