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LFA-1 亲和力调节在 T 细胞黏附、渗出和淋巴结间质迁移中的不同作用。

Distinct roles for LFA-1 affinity regulation during T-cell adhesion, diapedesis, and interstitial migration in lymph nodes.

机构信息

Immune Disease Institute, Boston, MA, USA.

出版信息

Blood. 2010 Feb 25;115(8):1572-81. doi: 10.1182/blood-2009-08-237917. Epub 2009 Dec 18.

Abstract

During the course of homing to lymph nodes (LNs), T cells undergo a multistep adhesion cascade that culminates in a lymphocyte function-associated antigen 1 (LFA-1)-dependent firm adhesion to the luminal surface of high endothelial venules (HEVs). The importance of LFA-1 affinity regulation in supporting T-cell arrest on HEVs has been well established, however, its importance in the postadhesion phase, which involves intraluminal crawling and diapedesis to the extravascular space, remains elusive. Here we have shown that LFA-1 affinity needs to be appropriately regulated to support these essential steps in the homing cascade. Genetically engineered T cells that were unable to properly down-regulate LFA-1 affinity underwent enhanced, chemokine-independent arrest in HEVs but showed perturbed intravascular crawling to transmigration sites and compromised diapedesis across HEVs. By contrast, the extravascular migration of T cells was insensitive to the affinity-enhancing LFA-1 mutation. These results highlight the requirement for balanced LFA-1 affinity regulation in intravascular and transvascular, but not extravascular, T-cell migration in LNs.

摘要

在归巢到淋巴结 (LNs) 的过程中,T 细胞经历一个多步骤的黏附级联反应,最终导致淋巴细胞功能相关抗原 1 (LFA-1) 依赖性牢固黏附在内皮细胞高通透性血管 (HEVs) 的管腔表面。已经充分证实,LFA-1 亲和力的调节对于支持 T 细胞在 HEVs 上的阻滞非常重要,然而,其在后续黏附阶段的重要性,包括管腔内爬行和穿越血管内皮细胞到血管外空间,仍然难以捉摸。在这里,我们已经表明,LFA-1 亲和力需要适当调节,以支持归巢级联反应中的这些重要步骤。不能正确下调 LFA-1 亲和力的基因工程 T 细胞在 HEVs 中经历了增强的、趋化因子非依赖性的阻滞,但显示出血管内爬行到迁移部位的紊乱和穿越 HEVs 的缺陷。相比之下,T 细胞的血管外迁移对增强 LFA-1 亲和力的突变不敏感。这些结果突出了在 LN 中,平衡的 LFA-1 亲和力调节对于血管内和跨血管但不是血管外 T 细胞迁移的必要性。

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