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树突状细胞和巨噬细胞是αβTCR转基因小鼠CD4+T细胞Th1发育所必需的:用IL-12替代巨噬细胞以刺激IFN-γ产生是IFN-γ依赖性的。

Dendritic cells and macrophages are required for Th1 development of CD4+ T cells from alpha beta TCR transgenic mice: IL-12 substitution for macrophages to stimulate IFN-gamma production is IFN-gamma-dependent.

作者信息

Macatonia S E, Hsieh C S, Murphy K M, O'Garra A

机构信息

Department of Immunology, DNAX Research Institute of Molecular and Cellular Biology, Palo Alto, CA 94304.

出版信息

Int Immunol. 1993 Sep;5(9):1119-28. doi: 10.1093/intimm/5.9.1119.

DOI:10.1093/intimm/5.9.1119
PMID:7902129
Abstract

We have examined the antigen presenting cell (APC) requirements for primary T cell activation and T helper (Th) cell phenotype differentiation using naive CD4+ T cells from alpha beta TCR transgenic mice. Purified dendritic cells were the principal cell required for induction of primary ovalbumin peptide specific T cell activation and clonal expansion. However, dendritic cells did not induce differentiation of T cells toward Th1 or Th2 phenotype. Addition of IL-4 during primary dendritic cell stimulations of T cells resulted in the development of a Th2 phenotype which produced high levels of IL-4 during secondary and tertiary stimulation. In contrast, development of Th1 cells producing high levels of IFN-gamma could not be induced with dendritic cells alone but required the addition of appropriately activated macrophages. Addition of splenic or peritoneal B cells did not induce Th1 development. Activated splenic macrophages induced Th1 development via a non-MHC restricted mechanism. Thus, requirements for induction of proliferation of naive CD4+ T cells are distinct from those directing Th1 phenotype development. IL-12 could replace the requirement for macrophages to induce Th1 development when T cells were activated with dendritic cells. Furthermore, this IL-12 mediated development of Th1 cells producing high levels of IFN-gamma was dependent on IFN-gamma.

摘要

我们使用来自αβTCR转基因小鼠的初始CD4 + T细胞,研究了初始T细胞活化和T辅助(Th)细胞表型分化对抗抗原呈递细胞(APC)的需求。纯化的树突状细胞是诱导初始卵清蛋白肽特异性T细胞活化和克隆扩增所需的主要细胞。然而,树突状细胞并未诱导T细胞向Th1或Th2表型分化。在树突状细胞对T细胞的初始刺激过程中添加IL-4会导致Th2表型的发展,该表型在二次和三次刺激期间产生高水平的IL-4。相反,仅用树突状细胞无法诱导产生高水平IFN-γ的Th1细胞的发育,而是需要添加适当活化的巨噬细胞。添加脾细胞或腹膜B细胞不会诱导Th1的发育。活化的脾巨噬细胞通过非MHC限制机制诱导Th1的发育。因此,诱导初始CD4 + T细胞增殖的需求与指导Th1表型发育的需求不同。当T细胞用树突状细胞激活时,IL-12可以替代巨噬细胞来诱导Th1的发育。此外,这种由IL-12介导的产生高水平IFN-γ的Th1细胞的发育依赖于IFN-γ。

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