MIP-1 gamma: molecular cloning, expression, and biological activities of a novel CC chemokine that is constitutively secreted in vivo.

Journal of inflammation Pub Date : 1995-01-01

A N Poltorak, F Bazzoni, I I Smirnova, E Alejos, P Thompson, G Luheshi, N Rothwell, B Beutler

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Abstract

We have identified a novel CC chemokine family member, herein termed MIP-1 gamma in view of its similarity to existing members of the MIP-1 group. The murine protein has a predicted length of 100 amino acids. Like MIP-1 alpha, recombinant MIP-1 gamma acts as a pyrogen when administered intracerebroventricularly. MIP-1 gamma and MIP-1 alpha engage the same high-affinity receptor on neutrophils, activating calcium release within seconds following cell contact. Pretreatment with either chemokine abolishes responses to the other, and to itself, suggesting utilization of a common signaling pathway. However, unlike MIP-1 alpha or any of the other CC chemokines, MIP-1 gamma is expressed constitutively by a wide variety of tissues, and circulates in the blood of healthy mice at concentrations of approximately 1 microgram/ml (90 nM). It would therefore be predicted that MIP-1 gamma occupies most of the CC chemokine receptors that exist in the intravascular compartment. As such it might, under normal circumstances, markedly influence responses to the inducible CC chemokines.

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MIP-1 γ:一种新型CC趋化因子的分子克隆、表达和生物活性，该趋化因子在体内组成性分泌。

我们已经确定了一个新的CC趋化因子家族成员，鉴于其与MIP-1组现有成员的相似性，本文将其命名为MIP-1 γ。该小鼠蛋白预计长度为100个氨基酸。与MIP-1 α一样，重组MIP-1 γ在脑室内给予时作为热原。MIP-1 γ和MIP-1 α与中性粒细胞上相同的高亲和力受体结合，在细胞接触后几秒钟内激活钙释放。用任何一种趋化因子预处理都可以消除对另一种趋化因子的反应，也可以消除对自身的反应，这表明利用了一个共同的信号通路。然而，与MIP-1 α或任何其他CC趋化因子不同，MIP-1 γ通过多种组织组成性表达，并以约1微克/毫升(90 nM)的浓度在健康小鼠的血液中循环。因此，可以预测MIP-1 γ占据了血管内腔室中存在的大部分CC趋化因子受体。因此，在正常情况下，它可能显著影响对诱导CC趋化因子的反应。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Journal of inflammation

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