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和文: 
英文:CLIP-170 is essential for MTOC repositioning during T cell activation by regulating dynein localisation on the cell surface 
著者
和文: Lim Wei Ming, 伊藤 由馬, 十川 久美子, 徳永 万喜洋.  
英文: Lim Wei Ming, Ito Y, Sakata-Sogawa K, Tokunaga M.  
言語 English 
掲載誌/書名
和文: 
英文:Scientific Reports 
巻, 号, ページ Vol. 8    No. 1    p. 17447
出版年月 2018年11月28日 
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DOI https://doi.org/10.1038/s41598-018-35593-z.
アブストラクト The microtubule-organizing centre (MTOC) is repositioned to the centre of the contacted cell surface, the immunological synapse, during T cell activation. However, our understanding of its molecular mechanism remains limited. Here, we found that the microtubule plus-end tracking cytoplasmic linker protein 170 (CLIP-170) plays a novel role in MTOC repositioning using fluorescence imaging. Inhibition of CLIP-170 phosphorylation impaired both MTOC repositioning and interleukin-2 (IL-2) expression. T cell stimulation induced some fraction of dynein to colocalise with CLIP-170 and undergo plus-end tracking. Concurrently, it increased dynein in minus-end-directed movement. It also increased dynein relocation to the centre of the contact surface. Dynein not colocalised with CLIP-170 showed both an immobile state and minus-end-directed movement at a velocity in good agreement with the velocity of MTOC repositioning, which suggests that dynein at the immunological synapse may pull the microtubules and the MTOC. Although CLIP-170 is phosphorylated by AMP-activated protein kinase (AMPK) irrespective of stimulation, phosphorylated CLIP-170 is essential for dynein recruitment to plus-end tracking and for dynein relocation. This indicates that dynein relocation results from coexistence of plus-end- and minus-end-directed translocation. In conclusion, CLIP-170 plays an indispensable role in MTOC repositioning and full activation of T cells by regulating dynein localisation.

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