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人类 Toll 样受体的组织表达以及 Toll 样受体 mRNA 在白细胞中对微生物、其产物及细胞因子应答时的差异调节。

Tissue expression of human Toll-like receptors and differential regulation of Toll-like receptor mRNAs in leukocytes in response to microbes, their products, and cytokines.

作者信息

Zarember Kol A, Godowski Paul J

机构信息

Department of Molecular Biology, Genentech Inc., South San Francisco, CA 94080, USA.

出版信息

J Immunol. 2002 Jan 15;168(2):554-61. doi: 10.4049/jimmunol.168.2.554.

DOI:10.4049/jimmunol.168.2.554
PMID:11777946
Abstract

Members of the Toll-like receptor (TLR) family mediate dorsoventral patterning and cellular adhesion in insects as well as immune responses to microbial products in both insects and mammals. TLRs are characterized by extracellular leucine-rich repeat domains and an intracellular signaling domain that shares homology with cytoplasmic sequences of the mammalian IL-1 receptor and plant disease resistance genes. Ten human TLRs have been cloned as well as RP105, a protein similar to TLR4 but lacking the intracellular signaling domain. However, only five TLRs have described functions as receptors for bacterial products (e.g., LPS, lipoproteins). To identify potential sites of action, we used quantitative real-time RT-PCR to examine systematically the expression of mRNAs encoding all known human TLRs, RP105, and several other proteins important in TLR functions (e.g., MD-1, MD-2, CD14, MyD88). Most tissues tested expressed at least one TLR, and several expressed all (spleen, peripheral blood leukocytes). Analysis of TLR expression in fractionated primary human leukocytes (CD4(+), CD8(+), CD19(+), monocytes, and granulocytes) indicates that professional phagocytes express the greatest variety of TLR mRNAs although several TLRs appear more restricted to B cells, suggesting additional roles for TLRs in adaptive immunity. Monocyte-like THP-1 cells regulate TLR mRNA levels in response to a variety of stimuli including phorbol esters, LPS, bacterial lipoproteins, live bacteria, and cytokines. Furthermore, addition of Escherichia coli to human blood ex vivo caused distinct changes in TLR expression, suggesting that important roles exist for these receptors in the establishment and resolution of infections and inflammation.

摘要

Toll样受体(TLR)家族成员在昆虫中介导背腹模式形成和细胞黏附,在昆虫和哺乳动物中均介导对微生物产物的免疫反应。TLR的特征是具有富含亮氨酸的胞外重复结构域和一个胞内信号结构域,该结构域与哺乳动物IL-1受体的胞质序列以及植物抗病基因具有同源性。已克隆出10种人类TLR以及RP105,RP105是一种与TLR4相似但缺乏胞内信号结构域的蛋白质。然而,只有5种TLR被描述为细菌产物(如脂多糖、脂蛋白)的受体。为了确定潜在的作用位点,我们使用定量实时逆转录聚合酶链反应(RT-PCR)系统地检测了编码所有已知人类TLR、RP105以及其他几种对TLR功能重要的蛋白质(如MD-1、MD-2、CD14、髓样分化因子88(MyD88))的mRNA的表达。大多数测试组织至少表达一种TLR,有几种组织表达所有TLR(脾脏、外周血白细胞)。对分离的原代人类白细胞(CD4(+)、CD8(+)、CD19(+)、单核细胞和粒细胞)中TLR表达的分析表明,专职吞噬细胞表达的TLR mRNA种类最多,尽管有几种TLR似乎更局限于B细胞表达,这表明TLR在适应性免疫中还有其他作用。单核细胞样THP-1细胞在受到包括佛波酯、脂多糖、细菌脂蛋白、活细菌和细胞因子在内的多种刺激时会调节TLR mRNA水平。此外,将大肠杆菌加入离体人血中会导致TLR表达发生明显变化,这表明这些受体在感染和炎症的发生与消退过程中发挥重要作用。

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