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鉴定人单核细胞上的整合膜蛋白RM3/1为富含半胱氨酸的清道夫受体家族(CD163)中糖皮质激素诱导型成员。

Identification of the integral membrane protein RM3/1 on human monocytes as a glucocorticoid-inducible member of the scavenger receptor cysteine-rich family (CD163).

作者信息

Högger P, Dreier J, Droste A, Buck F, Sorg C

机构信息

Institute of Experimental Dermatology, Westfälische Wilhelms-University Münster, Germany.

出版信息

J Immunol. 1998 Aug 15;161(4):1883-90.

PMID:9712057
Abstract

The RM3/1 Ag is a membrane glycoprotein restricted to human monocytes and macrophages that evolve in the late phase of inflammation. Peptide sequence analysis of the RM3/1 protein revealed similarity to CD163, a member of the scavenger receptor cysteine-rich family. Using specific Abs (RM3/1, Ki-M8), we demonstrate an identical cellular regulation for the RM3/1 and the CD163 protein. Most notably, we show for the first time that CD163 is significantly up-regulated by glucocorticoids. In contrast, the protein is down-regulated by the immunosuppressant cyclosporin A and by phorbol esters, while the inflammatory mediator LPS has no significant influence on the expression. We describe the first isolation of a full-length cDNA of CD163 and expression of the corresponding protein. Several splice variants of CD163 exist, and we elucidated the kinetics of induction of three major mRNA splice variants by fluticasone propionate; another splice variant was proved to be unresponsive to this glucocorticoid. Taken together with a previous result showing an involvement of RM3/1 in adhesion of monocytes to the activated endothelium, we discuss that CD163 might play an important role in inflammatory processes.

摘要

RM3/1抗原是一种膜糖蛋白,仅存在于人类单核细胞和巨噬细胞中,在炎症后期出现。RM3/1蛋白的肽序列分析显示其与清道夫受体富含半胱氨酸家族成员CD163相似。使用特异性抗体(RM3/1、Ki-M8),我们证明了RM3/1和CD163蛋白具有相同的细胞调控。最值得注意的是,我们首次表明糖皮质激素可显著上调CD163。相反,该蛋白被免疫抑制剂环孢素A和佛波酯下调,而炎症介质脂多糖对其表达没有显著影响。我们描述了首次分离出CD163的全长cDNA并表达了相应蛋白。CD163存在几种剪接变体,我们阐明了丙酸氟替卡松诱导三种主要mRNA剪接变体的动力学;另一种剪接变体被证明对这种糖皮质激素无反应。结合之前显示RM3/1参与单核细胞与活化内皮细胞黏附的结果,我们讨论CD163可能在炎症过程中起重要作用。

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