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タイトル
和文: 
英文:Spatiotemporal Regulation of T Cell Costimulation by TCR-CD28 Microclusters and Protein Kinase C θ Translocation 
著者
和文: Tadashi Yokosuka, Wakana Kobayashi, 十川久美子, Masako Takamatsu, Akiko Hashimoto-Tane, Michael L. Dustin, 徳永 万喜洋, Takashi Saito.  
英文: Tadashi Yokosuka, Wakana Kobayashi, Kumiko Sakata-Sogawa, Masako Takamatsu, Akiko Hashimoto-Tane, Michael L. Dustin, Makio Tokunaga, Takashi Saito.  
言語 English 
掲載誌/書名
和文: 
英文:Immunity 
巻, 号, ページ Volume 29    Number 4    pp. 589-601
出版年月 2008年10月 
出版者
和文: 
英文:Cellpress 
会議名称
和文: 
英文: 
開催地
和文: 
英文: 
DOI https://doi.org/10.1016/j.immuni.2008.08.011
アブストラクト T cell activation is mediated by microclusters (MCs) containing T cell receptors (TCRs), kinases, and adaptors. Although TCR MCs translocate to form a central supramolecular activation cluster (cSMAC) of the immunological synapse at the interface of a T cell and an antigen-presenting cell, the role of MC translocation in T cell signaling remains unclear. Here, we found that the accumulation of MCs at cSMAC was important for T cell costimulation. Costimulatory receptor CD28 was initially recruited coordinately with TCR to MCs, and its signals were mediated through the assembly with the kinase PKCθ. The accumulation of MCs at the cSMAC was accompanied by the segregation of CD28 from the TCR, which resulted in the translocation of both CD28 and PKCθ to a spatially unique subregion of cSMAC. Thus, costimulation is mediated by the generation of a unique costimulatory compartment in the cSMAC via the dynamic regulation of MC translocation.

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