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CCR2和MCP-3在单核细胞从骨髓动员及募集至炎症部位过程中的关键作用。

Critical roles for CCR2 and MCP-3 in monocyte mobilization from bone marrow and recruitment to inflammatory sites.

作者信息

Tsou Chia-Lin, Peters Wendy, Si Yue, Slaymaker Sarah, Aslanian Ara M, Weisberg Stuart P, Mack Matthias, Charo Israel F

机构信息

Gladstone Institute of Cardiovascular Disease, UCSF, San Francisco, California 94158, USA.

出版信息

J Clin Invest. 2007 Apr;117(4):902-9. doi: 10.1172/JCI29919. Epub 2007 Mar 15.

Abstract

Monocyte recruitment to sites of inflammation is regulated by members of the chemokine family of chemotactic cytokines. However, the mechanisms that govern the migration of monocytes from bone marrow to blood and from blood to inflamed tissues are not well understood. Here we report that CC chemokine receptor 2 (CCR2) is highly expressed on a subpopulation of blood monocytes whose numbers are markedly decreased in CCR2(-/-) mice. In bone marrow, however, CCR2(-/-) mice had an increased number of monocytes, suggesting that CCR2 is critical for monocyte egress. Intravenous infusion of ex vivo-labeled WT or CCR2(-/-) bone marrow into WT recipient mice demonstrated that CCR2 is necessary for efficient monocyte recruitment from the blood to inflamed tissue. Analysis of mice lacking monocyte chemoattractant protein-1 (MCP-1), MCP-3, MCP-5, or MCP-2 plus MCP-5 revealed that MCP-3 and MCP-1 are the CCR2 agonists most critical for the maintenance of normal blood monocyte counts. These findings provide evidence that CCR2 and MCP-3/MCP-1 are critical for monocyte mobilization and suggest new roles for monocyte chemoattractants in leukocyte homeostasis.

摘要

单核细胞向炎症部位的募集受趋化细胞因子趋化因子家族成员的调控。然而,单核细胞从骨髓迁移至血液以及从血液迁移至炎症组织的机制尚未完全明确。在此我们报告,CC趋化因子受体2(CCR2)在血液单核细胞亚群上高表达,其数量在CCR2基因敲除(CCR2(-/-))小鼠中显著减少。然而,在骨髓中,CCR2(-/-)小鼠的单核细胞数量增加,这表明CCR2对单核细胞的外流至关重要。将体外标记的野生型(WT)或CCR2(-/-)骨髓静脉输注到WT受体小鼠体内表明,CCR2对于单核细胞从血液有效募集至炎症组织是必需的。对缺乏单核细胞趋化蛋白-1(MCP-1)、MCP-3、MCP-5或MCP-2加MCP-5的小鼠进行分析发现,MCP-3和MCP-1是维持正常血液单核细胞计数最为关键的CCR2激动剂。这些发现证明CCR2和MCP-3/MCP-1对单核细胞动员至关重要,并提示单核细胞趋化因子在白细胞稳态中具有新作用。

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