del Pozo M A, Sánchez-Mateos P, Nieto M, Sánchez-Madrid F
Servicio de Inmunología, Hospital de la Princesa, Universidad Autónoma de Madrid, Spain.
J Cell Biol. 1995 Oct;131(2):495-508. doi: 10.1083/jcb.131.2.495.
Leukocyte recruitment is a key step in the inflammatory reaction. Several changes in the cell morphology take place during lymphocyte activation and migration: spheric-shaped resting T cells become polarized during activation, developing a well defined cytoplasmic projection designated as cellular uropod. We found that the chemotactic and proinflammatory chemokines RANTES, MCP-1, and, to a lower extent, MIP-1 alpha, MIP-1 beta, and IL-8, were able to induce uropod formation and ICAM-3 redistribution in T lymphoblasts adhered to ICAM-1 or VCAM-1. A similar chemokine-mediated effect was observed during T cells binding to the fibronectin fragments of 38- and 80-kD, that contain the binding sites for the integrins VLA-4 and VLA-5, respectively. The uropod structure concentrated the ICAM-3 adhesion molecule (a ligand for LFA-1), and emerged to the outer milieu from the area of contact between lymphocyte and protein ligands. In addition, we found that other adhesion molecules such as ICAM-1, CD43, and CD44, also redistributed to the lymphocyte uropod upon RANTES stimulation, whereas a wide number of other cell surface receptors did not redistribute. Chemokines displayed a selective effect among different T cell subsets; MIP-1 beta had more potent action on CD8+ T cells and tumor infiltrating lymphocytes (TIL), whereas RANTES and MIP-1 alpha targeted selectively CD4+ T cells. We have also examined the involvement of cAMP signaling pathway in uropod formation. Interestingly, several cAMP agonists were able to induce uropod formation and ICAM-3 redistribution, whereas H-89, a specific inhibitor of the cAMP-dependent protein kinase, abrogated the chemokine-mediated uropod formation, thus pointing out a role for cAMP-dependent signaling in the development of this cytoplasmic projection. Since the lymphocyte uropod induced by chemokines was completely abrogated by Bordetella pertussis toxin, the formation of this membrane projection appears to be dependent on G proteins signaling pathways. In addition, the involvement of myosin-based cytoskeleton in uropod formation and ICAM-3 redistribution in response to chemokines was suggested by the prevention of this phenomenon with the myosin-disrupting agent butanedione monoxime. Interestingly, this agent also inhibited the ICAM-3-mediated cell aggregation, but not the cell adhesion to substrata. Altogether, these results demonstrate that uropod formation and adhesion receptor redistribution is a novel function mediated by chemokines; this phenomenon may represent a mechanism that significantly contributes to the recruitment of circulating leukocytes to inflammatory foci.
白细胞募集是炎症反应中的关键步骤。在淋巴细胞激活和迁移过程中,细胞形态会发生多种变化:球形的静息T细胞在激活过程中会极化,形成一个定义明确的细胞质突起,称为细胞尾足。我们发现趋化性和促炎性趋化因子RANTES、MCP-1,以及程度较低的MIP-1α、MIP-1β和IL-8,能够在黏附于ICAM-1或VCAM-1的T淋巴母细胞中诱导尾足形成和ICAM-3重新分布。在T细胞与分别含有整合素VLA-4和VLA-5结合位点的38-kD和80-kD纤连蛋白片段结合过程中,也观察到了类似的趋化因子介导的效应。尾足结构使ICAM-3黏附分子(LFA-1的配体)聚集,并从淋巴细胞与蛋白质配体的接触区域伸向外部环境。此外,我们发现其他黏附分子,如ICAM-1、CD43和CD44,在RANTES刺激下也会重新分布到淋巴细胞尾足上,而许多其他细胞表面受体则不会重新分布。趋化因子在不同T细胞亚群中表现出选择性作用;MIP-1β对CD8+T细胞和肿瘤浸润淋巴细胞(TIL)的作用更强,而RANTES和MIP-1α则选择性地作用于CD4+T细胞。我们还研究了cAMP信号通路在尾足形成中的作用。有趣的是,几种cAMP激动剂能够诱导尾足形成和ICAM-3重新分布,而cAMP依赖性蛋白激酶的特异性抑制剂H-89则消除了趋化因子介导的尾足形成,从而指出cAMP依赖性信号在这种细胞质突起形成中的作用。由于趋化因子诱导的淋巴细胞尾足被百日咳博德特氏菌毒素完全消除,这种膜突起的形成似乎依赖于G蛋白信号通路。此外,肌球蛋白破坏剂丁二酮肟可预防这种现象,这表明基于肌球蛋白的细胞骨架参与了趋化因子诱导的尾足形成和ICAM-3重新分布。有趣的是,这种试剂也抑制了ICAM-3介导的细胞聚集,但不影响细胞与基质的黏附。总之,这些结果表明尾足形成和黏附受体重新分布是趋化因子介导的一种新功能;这种现象可能代表了一种机制,对循环白细胞募集到炎症部位有显著贡献。
