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白细胞介素-2调节T淋巴细胞中CC趋化因子受体的表达和趋化反应性。

Interleukin-2 regulates CC chemokine receptor expression and chemotactic responsiveness in T lymphocytes.

作者信息

Loetscher P, Seitz M, Baggiolini M, Moser B

机构信息

Theodor-Kocher Institute, University of Bern, Switzerland.

出版信息

J Exp Med. 1996 Aug 1;184(2):569-77. doi: 10.1084/jem.184.2.569.

DOI:10.1084/jem.184.2.569
PMID:8760810
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2192704/
Abstract

Several studies have shown that CC chemokines attract T lymphocytes, and that CD45RO+, memory phenotype cells are considered to be the main responders. The results, however, have often been contradictory and the role of lymphocyte activation and proliferation has remained unclear. Using CD45RO+ blood lymphocytes cultured under different stimulatory conditions, we have now studied chemotaxis as well as chemokine receptor expression. Expression of the RANTES/MIP-1 alpha receptor (CC-CKR1) and the MCP-1 receptor (CC-CKR2) was highly correlated with migration toward RANTES, MCP-1, and other CC chemokines, and was strictly dependent on the presence of IL-2 in the culture medium. Migration and receptor expression were rapidly downregulated when IL-2 was withdrawn, but were fully restored when IL-2 was added again. The effect of IL-2 could be partially mimicked by IL-4, IL-10, or IL-12, but not by IL-13, IFN gamma, IL-1 beta, TNF-alpha, or by exposure to anti-CD3, anti-CD28 or phytohemagglutinin. Activation of fully responsive lymphocytes through the TCR/CD3 complex and CD28 antigen actually had the opposite effect. It rapidly downregulated receptor expression and consequent migration even in the presence of IL-2. In contrast to the effects on CC chemokine receptors, stimulation of CD45RO+ T lymphocytes with IL-2 neither induced the expression of the CXC chemokine receptors, IL8-R1 and IL8-R2, nor chemotaxis to IL-8. The prominent role of IL-2 in CC chemokine responsiveness of lymphocytes suggests that IL-2-mediated expansion is a prerequisite for the recruitment of antigen-activated T cells into sites of immune and inflammatory reactions.

摘要

多项研究表明,CC趋化因子可吸引T淋巴细胞,且CD45RO+记忆表型细胞被认为是主要应答细胞。然而,研究结果往往相互矛盾,淋巴细胞活化和增殖的作用仍不明确。我们利用在不同刺激条件下培养的CD45RO+血液淋巴细胞,研究了趋化性以及趋化因子受体的表达。RANTES/MIP-1α受体(CC-CKR1)和MCP-1受体(CC-CKR2)的表达与向RANTES、MCP-1及其他CC趋化因子的迁移高度相关,且严格依赖于培养基中IL-2的存在。当撤除IL-2时,迁移和受体表达迅速下调,但再次添加IL-2时则完全恢复。IL-4、IL-10或IL-十二可部分模拟IL-2的作用,但IL-13、IFNγ、IL-1β、TNF-α或抗CD3、抗CD28或植物血凝素则不能。通过TCR/CD3复合物和CD28抗原激活完全应答的淋巴细胞实际上产生了相反的效果。即使在有IL-2存在的情况下,它也会迅速下调受体表达及随之而来的迁移。与对CC趋化因子受体的影响相反,用IL-2刺激CD45RO+T淋巴细胞既不诱导CXC趋化因子受体IL8-R1和IL8-R2的表达,也不诱导对IL-8的趋化性。IL-2在淋巴细胞CC趋化因子反应性中的突出作用表明,IL-2介导的扩增是将抗原激活的T细胞募集到免疫和炎症反应部位的先决条件。

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