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巨噬细胞分泌一种具有炎症和中性粒细胞趋化特性的新型肝素结合蛋白。

Macrophages secrete a novel heparin-binding protein with inflammatory and neutrophil chemokinetic properties.

作者信息

Wolpe S D, Davatelis G, Sherry B, Beutler B, Hesse D G, Nguyen H T, Moldawer L L, Nathan C F, Lowry S F, Cerami A

机构信息

Laboratory of Medical Biochemistry, Rockefeller University, New York.

出版信息

J Exp Med. 1988 Feb 1;167(2):570-81. doi: 10.1084/jem.167.2.570.

Abstract

We report the identification and purification of a new inflammatory monokine synthesized by the macrophage tumor cell line RAW 264.7 in response to endotoxin. This monokine, which we term "macrophage inflammatory protein" (MIP), is a doublet with an apparent molecular mass of approximately 8,000 daltons on SDS-PAGE but forms aggregates of greater than 2 x 10(6) daltons as assessed by gel filtration. Partial NH2-terminal amino acid sequence data reveal no significant homology with any previously described protein. Although the monokine is anionic under physiological conditions, it is one of two major macrophage-secreted proteins that bind to heparin at high salt concentrations. At 100 ng/ml or greater, MIP is chemokinetic for human polymorphonuclear cells and triggers hydrogen peroxide production. Subcutaneous injection of 10 ng or greater of MIP into footpads of C3H/HeJ mice elicits an inflammatory response, characterized by neutrophil infiltration. These findings suggest that MIP is an endogenous mediator that may play a role in the host responses that occur during endotoxemia and other inflammatory events.

摘要

我们报告了一种新的炎症单核因子的鉴定和纯化,该因子由巨噬细胞肿瘤细胞系RAW 264.7对内毒素作出反应而合成。这种单核因子,我们称之为“巨噬细胞炎症蛋白”(MIP),在SDS-PAGE上是一个双峰,表观分子量约为8000道尔顿,但通过凝胶过滤评估,它形成大于2×10⁶道尔顿的聚集体。部分氨基末端氨基酸序列数据显示与任何先前描述的蛋白质无明显同源性。尽管该单核因子在生理条件下呈阴离子性,但它是在高盐浓度下与肝素结合的两种主要巨噬细胞分泌蛋白之一。在100 ng/ml或更高浓度时,MIP对人多形核细胞具有趋化作用并触发过氧化氢的产生。将10 ng或更多的MIP皮下注射到C3H/HeJ小鼠的足垫中会引发炎症反应,其特征为中性粒细胞浸润。这些发现表明MIP是一种内源性介质,可能在内毒素血症和其他炎症事件期间发生的宿主反应中起作用。

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