Ishii T, Ohnuma K, Murakami A, Takasawa N, Kobayashi S, Dang N H, Schlossman S F, Morimoto C
Department of Clinical Immunology, Advanced Clinical Research Center, Institute of Medical Science, University of Tokyo, 4-6-1, Shirokanedai, Minato-ku, Tokyo 108-8639, Japan.
Proc Natl Acad Sci U S A. 2001 Oct 9;98(21):12138-43. doi: 10.1073/pnas.211439098. Epub 2001 Oct 2.
CD26 is a T cell activation antigen that contains dipeptidyl peptidase IV activity and is known to bind adenosine deaminase. The mechanism by which CD26 costimulation potentiates T cell receptor-mediated T cell activation, leading to subsequent exertion of T cell effector function, is still not clearly defined. In this article, we demonstrate that CD26 localizes into lipid rafts, and targeting of CD26 to rafts is necessary for signaling events through CD26. Importantly, aggregation of CD26 by anti-CD26 mAb crosslinking also causes coaggregation of CD45 into rafts. Moreover, we show that CD26 directly binds to the cytoplasmic domain of CD45. Our results therefore indicate a mechanism whereby CD26 engagement promotes aggregation of lipid rafts and facilitates colocalization of CD45 to T cell receptor signaling molecules p56(Lck), ZAP-70, and TCRzeta, thereby enhancing protein tyrosine phosphorylation of various signaling molecules and subsequent interleukin-2 production.
CD26是一种T细胞活化抗原,具有二肽基肽酶IV活性,已知可结合腺苷脱氨酶。CD26共刺激增强T细胞受体介导的T细胞活化并导致随后T细胞效应功能发挥的机制仍未明确界定。在本文中,我们证明CD26定位于脂筏,并且将CD26靶向脂筏对于通过CD26的信号事件是必需的。重要的是,抗CD26单克隆抗体交联导致的CD26聚集也会使CD45共聚集到脂筏中。此外,我们表明CD26直接结合CD45的胞质结构域。因此,我们的结果表明了一种机制,即CD26的结合促进脂筏聚集并促进CD45与T细胞受体信号分子p56(Lck)、ZAP-70和TCRzeta共定位,从而增强各种信号分子的蛋白酪氨酸磷酸化以及随后的白细胞介素-2产生。
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