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CCR2趋化因子受体的特性:B细胞中功能性CCR2受体的表达

Characterization of the CCR2 chemokine receptor: functional CCR2 receptor expression in B cells.

作者信息

Frade J M, Mellado M, del Real G, Gutierrez-Ramos J C, Lind P, Martinez-A C

机构信息

Department of Immunology and Oncology, Centro Nacional de Biotecnología, Consejo Superior de Investigaciones Cientificas, Campus Cantoblanco, Universidad Autónoma, Madrid, Spain.

出版信息

J Immunol. 1997 Dec 1;159(11):5576-84.

PMID:9548499
Abstract

We have derived anti-human CCR2-specific mAbs by immunization with synthetic peptides corresponding to CCR2 sequences presumably involved in the interaction with its ligand(s). The characterization of these mAbs includes the ability to recognize the CCR2 receptor specifically, as well as the function based on their ability to promote Ca2+ influx or to block MCP-1-induced Ca2+ influx and chemotaxis. One mAb (MCP-1 R02) that is directed to the NH2 terminal domain of the CCR2 receptor has MCP-1 agonist activity, and two that recognize the third extracellular domain (MCP-1R04 and MCP-1 R05) have MCP-1 antagonist activity. We analyzed the presence of CCR2 in several PBL and tonsil-derived leukocyte populations and found expression of this receptor in monocytes, activated T cells, and, surprisingly, in B cells. CCR2 receptor expression in B cells was further corroborated in Southern blot using CCR2-specific probes. Moreover, both MCP-1 and the agonist mAb trigger specific B cell migration via a PTX-sensitive mechanism, indicating the presence of a functional CCR2 receptor in these cells.

摘要

我们通过用与可能参与与其配体相互作用的CCR2序列相对应的合成肽免疫,获得了抗人CCR2特异性单克隆抗体。这些单克隆抗体的特性包括特异性识别CCR2受体的能力,以及基于它们促进Ca2+内流或阻断MCP-1诱导的Ca2+内流和趋化作用的功能。一种针对CCR2受体NH2末端结构域的单克隆抗体(MCP-1 R02)具有MCP-1激动剂活性,而两种识别第三个细胞外结构域的单克隆抗体(MCP-1R04和MCP-1 R05)具有MCP-1拮抗剂活性。我们分析了几种外周血淋巴细胞(PBL)和扁桃体来源的白细胞群体中CCR2的存在情况,发现该受体在单核细胞、活化的T细胞中表达,令人惊讶的是,在B细胞中也有表达。使用CCR2特异性探针的Southern印迹进一步证实了B细胞中CCR2受体的表达。此外,MCP-1和激动剂单克隆抗体均通过对百日咳毒素(PTX)敏感的机制触发特异性B细胞迁移,表明这些细胞中存在功能性CCR2受体。

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