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功能性血小板活化因子受体由单核细胞和粒细胞表达,但正常个体或哮喘患者的静息或活化T和B淋巴细胞不表达。

Functional platelet-activating factor receptors are expressed by monocytes and granulocytes but not by resting or activated T and B lymphocytes from normal individuals or patients with asthma.

作者信息

Simon H U, Tsao P W, Siminovitch K A, Mills G B, Blaser K

机构信息

Swiss Institute of Allergy and Asthma Research, Davos.

出版信息

J Immunol. 1994 Jul 1;153(1):364-77.

PMID:8207248
Abstract

Platelet-activating factor (PAF) may play a role in the regulation of immune responsiveness and is a potent mediator in asthmatic inflammation. However, as yet, the mechanisms whereby PAF mediates its pleiomorphic effects on immune cells have not been elucidated. Because PAF is a potent chemotactic factor for eosinophils, the presence of receptors for PAF (PAFR) on lymphocytes may provide a mechanism for the concurrent recruitment of both eosinophils and T lymphocytes into the airways of asthmatic patients. To address this issue, we have examined freshly isolated PBMC and granulocytic cells as well as various T and B lymphocyte lines with regards to PAFR expression and PAF-induced changes in intracellular calcium concentration. Using two-color immunofluorescence techniques and highly purified cell populations, it was not possible to detect surface PAFR protein or functional PAFR on resting and in vivo or in vitro activated T and B cells derived from nonallergic individuals or patients with allergic asthma. In addition, we were unable to detect PAFR mRNA, protein, or functional response to PAF in human or murine T cell lines. In contrast, we found functional PAFR in most B lymphoblastoid cell lines. Within the PBMC population, CD14+ cells respond to PAF. These results suggest that PAF does not interact directly with lymphocytes and thus that previous observations suggestive of such an interaction likely reflect the effects of PAF on monocytes. PAF-induced increases in intracellular calcium concentration were also detected in neutrophils and eosinophils, but were lower in granulocytes relative to the levels detected in monocytes.

摘要

血小板活化因子(PAF)可能在免疫反应调节中发挥作用,并且是哮喘炎症中的一种强效介质。然而,迄今为止,PAF介导其对免疫细胞多形性作用的机制尚未阐明。由于PAF是嗜酸性粒细胞的强效趋化因子,淋巴细胞上PAF受体(PAFR)的存在可能为嗜酸性粒细胞和T淋巴细胞同时募集到哮喘患者气道中提供一种机制。为解决这一问题,我们已就PAFR表达以及PAF诱导的细胞内钙浓度变化,对新鲜分离的外周血单核细胞(PBMC)和粒细胞以及各种T和B淋巴细胞系进行了检测。使用双色免疫荧光技术和高度纯化的细胞群体,无法在来自非过敏个体或过敏性哮喘患者的静息以及体内或体外活化的T和B细胞上检测到表面PAFR蛋白或功能性PAFR。此外,我们无法在人或鼠T细胞系中检测到PAFR mRNA、蛋白或对PAF的功能性反应。相比之下,我们在大多数B淋巴母细胞系中发现了功能性PAFR。在PBMC群体中,CD14+细胞对PAF有反应。这些结果表明,PAF不直接与淋巴细胞相互作用,因此先前提示这种相互作用的观察结果可能反映了PAF对单核细胞的作用。在中性粒细胞和嗜酸性粒细胞中也检测到PAF诱导的细胞内钙浓度升高,但相对于在单核细胞中检测到的水平,粒细胞中的升高较低。

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