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人多形核白细胞白三烯B4受体膜蛋白结合成分的亲和标记

Affinity labeling of the membrane protein-binding component of human polymorphonuclear leukocyte receptors for leukotriene B4.

作者信息

Goldman D W, Gifford L A, Young R N, Marotti T, Cheung M K, Goetzl E J

机构信息

Department of Medicine, University of California Medical Center, San Francisco 94143-0724.

出版信息

J Immunol. 1991 Apr 15;146(8):2671-7.

PMID:1849936
Abstract

A radiolabeled N-(3-aminopropyl)-leukotriene B4 amide ([3H]LTB4-APA) analog of the potent leukocyte chemotactic factor leukotriene B4 (LTB4) binds to receptors for LTB4 in plasma membrane-enriched preparations from human blood polymorphonuclear leukocytes (PMNL) and intact PMNL with respective mean dissociation constants of 2.3 nM and 69 nM at 4 degrees C. The [3H]LTB4-APA bound to plasma membrane-enriched preparations from PMNL was covalently cross-linked to membrane proteins with disuccinimidyl suberate. Solubilization and resolution by SDS-PAGE of proteins from [3H]LTB4-APA-labeled PMNL membranes revealed predominant labeling of a 60-kDa protein. Labeling of the PMNL membrane protein was inhibited by LTB4 and its analogs at concentrations similar to those inhibiting the binding of [3H]LTB4 to its receptor, with an identical rank order of potency of LTB4 greater than 20-hydroxy-LTB4 greater than LTB4-APA = 5(S),12(R)-dihydroxy-eicosa-14-cis-6,8,10-trans-tetraenoic acid much greater than LTD4 = LTC4. GTP suppressed the labeling of the 60-kDa PMNL membrane protein to an extent consistent with the decrease in receptor affinity for LTB4 induced by GTP. The stereospecificity of the affinity cross-linking reaction and the regulation by GTP support the identification of an approximately 60-kDa protein as the binding component of the PMNL receptor for LTB4.

摘要

强效白细胞趋化因子白三烯B4(LTB4)的放射性标记N-(3-氨丙基)-白三烯B4酰胺([3H]LTB4-APA)类似物,在4℃下与人血多形核白细胞(PMNL)的富含质膜的制剂及完整PMNL中的LTB4受体结合,其平均解离常数分别为2.3 nM和69 nM。与PMNL富含质膜的制剂结合的[3H]LTB4-APA,用辛二酸二琥珀酰亚胺酯与膜蛋白共价交联。对来自[3H]LTB4-APA标记的PMNL膜的蛋白质进行SDS-PAGE溶解和分离,显示主要标记了一种60 kDa的蛋白质。LTB4及其类似物在与抑制[3H]LTB4与其受体结合的浓度相似时,抑制了PMNL膜蛋白的标记,LTB4的效价顺序相同,即LTB4>20-羟基-LTB4>LTB4-APA = 5(S),12(R)-二羟基-二十碳-14-顺-6,8,10-反-四烯酸>LTD4 = LTC4。GTP抑制了60 kDa PMNL膜蛋白的标记,其程度与GTP诱导的受体对LTB4亲和力降低一致。亲和交联反应的立体特异性和GTP的调节作用支持将一种约60 kDa的蛋白质鉴定为PMNL中LTB4受体的结合成分。

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