Katagiri Koko, Katakai Tomoya, Ebisuno Yukihiko, Ueda Yoshihiro, Okada Takaharu, Kinashi Tatsuo
Department of Molecular Genetics, Kansai Medical University, Fumizono-cho, Moriguchi-City, Osaka, Japan.
EMBO J. 2009 May 6;28(9):1319-31. doi: 10.1038/emboj.2009.82. Epub 2009 Apr 2.
The regulation of lymphocyte adhesion and migration plays crucial roles in lymphocyte trafficking during immunosurveillance. However, our understanding of the intracellular signalling that regulates these processes is still limited. Here, we show that the Ste20-like kinase Mst1 plays crucial roles in lymphocyte trafficking in vivo. Mst1(-/-) lymphocytes exhibited an impairment of firm adhesion to high endothelial venules, resulting in an inefficient homing capacity. In vitro lymphocyte adhesion cascade assays under physiological shear flow revealed that the stopping time of Mst1(-/-) lymphocytes on endothelium was markedly reduced, whereas their L-selectin-dependent rolling/tethering and transition to LFA-1-mediated arrest were not affected. Mst1(-/-) lymphocytes were also defective in the stabilization of adhesion through alpha4 integrins. Consequently, Mst1(-/-) mice had hypotrophic peripheral lymphoid tissues and reduced marginal zone B cells and dendritic cells in the spleen, and defective emigration of single positive thymocytes. Furthermore, Mst1(-/-) lymphocytes had impaired motility over lymph node-derived stromal cells and within lymph nodes. Thus, our data indicate that Mst1 is a key enzyme involved in lymphocyte entry and interstitial migration.
淋巴细胞黏附和迁移的调节在免疫监视期间的淋巴细胞运输中起着关键作用。然而,我们对调节这些过程的细胞内信号传导的理解仍然有限。在此,我们表明,类Ste20激酶Mst1在体内淋巴细胞运输中起着关键作用。Mst1(-/-)淋巴细胞对高内皮微静脉的牢固黏附受损,导致归巢能力低下。在生理剪切流下进行的体外淋巴细胞黏附级联分析显示,Mst1(-/-)淋巴细胞在内皮上的停留时间显著缩短,而其L-选择素依赖性滚动/系留以及向LFA-1介导的黏附停滞的转变不受影响。Mst1(-/-)淋巴细胞通过α4整合素稳定黏附的能力也存在缺陷。因此,Mst1(-/-)小鼠的外周淋巴组织发育不全,脾脏边缘区B细胞和树突状细胞减少,单阳性胸腺细胞的迁出存在缺陷。此外,Mst1(-/-)淋巴细胞在淋巴结来源的基质细胞上以及淋巴结内的运动能力受损。因此,我们的数据表明,Mst1是参与淋巴细胞进入和间质迁移的关键酶。
