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分析II类主要组织相容性复合体呈递在通过靶向进入外源性抗原-I类主要组织相容性复合体呈递途径的抗原刺激细胞毒性T淋巴细胞中的作用。

Analysis of the role of MHC class II presentation in the stimulation of cytotoxic T lymphocytes by antigens targeted into the exogenous antigen-MHC class I presentation pathway.

作者信息

Rock K L, Clark K

机构信息

Division of Lymphocyte Biology, Dana Farber Cancer Institute, Boston, MA 02115, USA.

出版信息

J Immunol. 1996 May 15;156(10):3721-6.

PMID:8621907
Abstract

By conjugation of proteins to beads, Ags can be selectively targeted into the MHC class I pathway of phagocytes in vivo and can stimulate CTL responses. Because phagocytes also present particulate Ag on MHC class II molecules, we examined whether these Ags stimulated concomitant CD4 T cell immunity. Although the priming of CD4 T cells with soluble OVA required adjuvants, particulate Ag was stimulatory when injected in saline. We next examined whether CD4 T cell responses played a role in the generation of CTL to particulate Ag. At low concentrations of Ag, OVA primed CTLs in wild-type mice but not in MHC class II-deficient animals, indicating that MHC class II presentation of Ag was essential for CTL generation. These data both support a model where CD4 T cells collaborate with CTLs as part of a three-cell interaction and identify a phagocyte as the third cell in this reaction. Interestingly, injection of higher concentrations of the same Ag primed equivalent CTL responses in both wild-type and MHC class II-deficient mice. These results indicate that a key variable in determining whether CTL generation is helper cell dependent or independent is the dose of immunogen. This may explain in part why CTL responses to abundant Ags, such as viruses, tend to be helper independent, while responses to less abundant Ags, such as minor histocompatibility Ags, require T helper cells. In addition, these results also point to the potential of using particulate Ags to prime or boost responses in settings with CD4 immunodeficiency.

摘要

通过将蛋白质与珠子偶联,抗原(Ag)可在体内被选择性地靶向至吞噬细胞的MHC I类途径,并能刺激细胞毒性T淋巴细胞(CTL)反应。由于吞噬细胞也会在MHC II类分子上呈递颗粒性抗原,我们研究了这些抗原是否能刺激伴随的CD4 T细胞免疫反应。尽管用可溶性卵清蛋白(OVA)启动CD4 T细胞需要佐剂,但颗粒性抗原在注射到盐水中时具有刺激性。接下来,我们研究了CD4 T细胞反应在针对颗粒性抗原产生CTL的过程中是否发挥作用。在低浓度抗原的情况下,OVA在野生型小鼠中启动了CTL,但在MHC II类缺陷动物中则没有,这表明抗原的MHC II类呈递对于CTL的产生至关重要。这些数据既支持了一种模型,即CD4 T细胞作为三细胞相互作用的一部分与CTL协作,并确定吞噬细胞是该反应中的第三个细胞。有趣的是,注射更高浓度的相同抗原在野生型和MHC II类缺陷小鼠中均启动了等效的CTL反应。这些结果表明,决定CTL产生是依赖辅助细胞还是独立于辅助细胞的一个关键变量是免疫原的剂量。这可能部分解释了为什么针对丰富抗原(如病毒)的CTL反应往往独立于辅助细胞,而针对较少丰富抗原(如次要组织相容性抗原)的反应则需要T辅助细胞。此外,这些结果还指出了在存在CD4免疫缺陷的情况下使用颗粒性抗原启动或增强反应的潜力。

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