T细胞受体连接的程度可决定初始CD4+ T细胞的功能分化。
Extent of T cell receptor ligation can determine the functional differentiation of naive CD4+ T cells.
作者信息
Constant S, Pfeiffer C, Woodard A, Pasqualini T, Bottomly K
机构信息
Section of Immunobiology, Yale University School of Medicine, New Haven, Connecticut, USA.
出版信息
J Exp Med. 1995 Nov 1;182(5):1591-6. doi: 10.1084/jem.182.5.1591.
Abstract
Naive CD4+ T cells can differentiate into cells predominantly involved in humoral immunity, known as T helper type 2 cells (Th2), or cells involved in cell-mediated immunity, known as Th1 cells. In this report, we show that priming of CD4+ T cells bearing a transgene-encoded T cell receptor can lead to differentiation into Th1-like cells producing abundant interferon gamma when the cells are exposed to high antigen doses, while low doses of the same peptide induce cells with the same T cell receptor to differentiate into Th2-like cells producing abundant interleukin 4. Thus antigen dose is one factor that can control the differentiation fate of a naive CD4+ T cell.
摘要
初始CD4+ T细胞可分化为主要参与体液免疫的细胞,即2型辅助性T细胞(Th2),或参与细胞介导免疫的细胞,即Th1细胞。在本报告中,我们表明,当携带转基因编码的T细胞受体的CD4+ T细胞暴露于高抗原剂量时,其启动可导致分化为产生大量干扰素γ的Th1样细胞,而低剂量的相同肽则诱导具有相同T细胞受体的细胞分化为产生大量白细胞介素4的Th2样细胞。因此,抗原剂量是可以控制初始CD4+ T细胞分化命运的一个因素。
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