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一氧化氮可诱导致脑炎性T细胞中肌动蛋白极化,并以不依赖p70S6激酶的方式抑制其体外跨内皮迁移。

Nitric oxide induces polarization of actin in encephalitogenic T cells and inhibits their in vitro trans-endothelial migration in a p70S6 kinase-independent manner.

作者信息

Staykova Maria A, Berven Leise A, Cowden William B, Willenborg David O, Crouch Michael F

机构信息

Neurosciences Research Unit, The Canberra Hospital, Australia.

出版信息

FASEB J. 2003 Jul;17(10):1337-9. doi: 10.1096/fj.02-0577fje. Epub 2003 May 20.

DOI:10.1096/fj.02-0577fje
PMID:12759332
Abstract

Nitric oxide (NO) inhibits both actively induced and transferred autoimmune encephalomyelitis. To explore potential mechanisms, we examined the ability of NO to inhibit migration of T lymphoblasts through both collagen matrices and monolayers of rat brain endothelial cells. The NO donor 1-hydroxy-2-oxo-3, 3-bis (2-aminoethyl)-1-triazene (HOBAT) inhibited migration in a concentration-dependent manner. NO pretreatment of T cells inhibited migration through untreated endothelial cells, but NO pretreatment of endothelial cells had no inhibitory effect on untreated T cells. Therefore NO's migration inhibitory action was mediated through its effect on T cells and not endothelial cells. HOBAT did not inhibit migration by inducing T-cell death but rather by polarizing the T cells, resulting in a morphology suggestive of migrating cells. P70S6 kinase, shown to have a role in NO-induced migration inhibition in fibroblasts, had no role in the inhibitory effect of NO on T-cell migration. Thus, HOBAT did not alter p70S6K activity nor did rapamycin, a specific inhibitor of p70S6K, inhibit HOBAT-induced T-cell morphological changes or T-cell migration. We suggest that NO-induced morphological changes result in T cells with predefined migratory directionality, thus limiting the ability of these cells to respond to other migratory signals.

摘要

一氧化氮(NO)可抑制主动诱导型和转移型自身免疫性脑脊髓炎。为探究潜在机制,我们检测了NO抑制T淋巴母细胞通过胶原蛋白基质和大鼠脑内皮细胞单层迁移的能力。NO供体1-羟基-2-氧代-3,3-双(2-氨基乙基)-1-三氮烯(HOBAT)以浓度依赖性方式抑制迁移。对T细胞进行NO预处理可抑制其通过未处理的内皮细胞的迁移,但对内皮细胞进行NO预处理对未处理的T细胞没有抑制作用。因此,NO的迁移抑制作用是通过其对T细胞的作用介导的,而非内皮细胞。HOBAT并非通过诱导T细胞死亡来抑制迁移,而是通过使T细胞极化,导致细胞形态呈现出迁移细胞的特征。P70S6激酶在成纤维细胞中显示在NO诱导的迁移抑制中起作用,但在NO对T细胞迁移的抑制作用中没有作用。因此,HOBAT不会改变p70S6K的活性,p70S6K的特异性抑制剂雷帕霉素也不会抑制HOBAT诱导的T细胞形态变化或T细胞迁移。我们认为,NO诱导的形态变化导致T细胞具有预定义的迁移方向性,从而限制了这些细胞对其他迁移信号作出反应的能力。

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