Costimulatory Effect of Fas in Mouse T Lymphocytes |
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Authors: | Doo Hyun Chung Kyeong Cheon Jung Weon Seo Park Im-Soon Lee Weon Jin Choi Chong-Jae Kim Seong Hoe Park Youngmee Bae |
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Affiliation: | (1) Department of Pathology, Seoul National University School of Medicine, Seoul, 110-799, Korea;(2) Department of Pathology, Hallym University College of Medicine, Seoul, 110-799, Korea;(3) Department of Pathology, Kangwon National University College of Medicine, Chunchon, 200-701, Korea;(4) Department of Surgery, Kangwon National University College of Medicine, Chunchon, 200-701, Korea;(5) Research Division of Human Life Science, Seoul National University College of Medicine, Seoul, 110-799, Korea |
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Abstract: | To induce proper immune responses, T lymphocytes require two types of stimuli, antigen-specific and costimulatory signals. Among costimulatory molecules, CD28-engagement promotes the survival and proliferation of both naive and memory T cells. In addition, it is now believed that Fas may play a role in T cell activation in the human system. It is, however, controversial whether Fas can act as a costimulatory signal in the murine system. Thus, we investigated fundamental differences in the capacity to induce proliferation of T cells between Fas and CD28 in mice. Fas-mediated T cell proliferation was observed only with a full mitogenic dose of anti-CD3 antibodies, whereas CD28 engagement was able to enhance T cell proliferation in the presence of a suboptimal level of anti-CD3 antibody. Furthermore, Fas-engaged T cells showed faster response in the upregulation of CD25 and CD69 expression than CD28-engaged ones. Here, we report that Fas might play a role in mature T cell activation in the mouse system through a different mechanism from that in CD28 costimulation. |
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Keywords: | CD28 Costimulation Fas Proliferation |
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