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马来酰化白蛋白的受体识别可诱导人单核细胞趋化。

Receptor recognition of maleyl-albumin induces chemotaxis in human monocytes.

作者信息

Haberland M E, Rasmussen R R, Fogelman A M

出版信息

J Clin Invest. 1986 Sep;78(3):827-31. doi: 10.1172/JCI112647.

Abstract

We demonstrate here that the exceptionally active maleyl-albumin receptor of human monocytes functions in vitro as a chemoattractant receptor. Chemotaxis of human monocytes occurs at an effective median dose of 3-4 microM maleyl-albumin, a concentration representing 1% of the total albumin in the adult human. Computerized analyses by LIGAND of the saturable binding of maleyl-albumin to human monocytes reveal two classes of binding sites, described by dissociation constants of 37 nM and 5.3 microM with maximal binding of 1.6 and 23 pmol maleyl-albumin/mg cellular protein, respectively. Chemotaxis of human monocytes thus occurs at concentrations of maleyl-albumin promoting binding to the lower-affinity sites. We propose that conformational isomers of albumin that are chemotactic may form in vivo and that albumin, in addition to receptor-independent plasma transport functions, may also play an important role in the receptor-mediated recruitment and accumulation of phagocytic cells at sites of inflammation and injury.

摘要

我们在此证明,人类单核细胞中异常活跃的顺丁烯二酰化白蛋白受体在体外作为趋化因子受体发挥作用。人类单核细胞的趋化作用在3-4微摩尔顺丁烯二酰化白蛋白的有效中位剂量下发生,该浓度占成年人体内总白蛋白的1%。通过LIGAND对顺丁烯二酰化白蛋白与人单核细胞的饱和结合进行计算机分析,发现两类结合位点,其解离常数分别为37纳摩尔和5.3微摩尔,最大结合量分别为1.6和23皮摩尔顺丁烯二酰化白蛋白/毫克细胞蛋白。因此,人类单核细胞的趋化作用发生在促进与低亲和力位点结合的顺丁烯二酰化白蛋白浓度下。我们提出,具有趋化作用的白蛋白构象异构体可能在体内形成,并且白蛋白除了具有不依赖受体的血浆运输功能外,还可能在炎症和损伤部位受体介导的吞噬细胞募集和聚集过程中发挥重要作用。

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