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一类在结构上与果蝇Toll受体相关的人类受体。

A family of human receptors structurally related to Drosophila Toll.

作者信息

Rock F L, Hardiman G, Timans J C, Kastelein R A, Bazan J F

机构信息

Department of Molecular Biology, DNAX Research Institute, Palo Alto, CA 94304-1104, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Jan 20;95(2):588-93. doi: 10.1073/pnas.95.2.588.

Abstract

The discovery of sequence homology between the cytoplasmic domains of Drosophila Toll and human interleukin 1 receptors has sown the conviction that both molecules trigger related signaling pathways tied to the nuclear translocation of Rel-type transcription factors. This conserved signaling scheme governs an evolutionarily ancient immune response in both insects and vertebrates. We report the molecular cloning of a class of putative human receptors with a protein architecture that is similar to Drosophila Toll in both intra- and extracellular segments. Five human Toll-like receptors--named TLRs 1-5--are probably the direct homologs of the fly molecule and, as such, could constitute an important and unrecognized component of innate immunity in humans. Intriguingly, the evolutionary retention of TLRs in vertebrates may indicate another role--akin to Toll in the dorsoventralization of the Drosophila embryo--as regulators of early morphogenetic patterning. Multiple tissue mRNA blots indicate markedly different patterns of expression for the human TLRs. By using fluorescence in situ hybridization and sequence-tagged site database analyses, we also show that the cognate Tlr genes reside on chromosomes 4 (TLRs 1, 2, and 3), 9 (TLR4), and 1 (TLR5). Structure prediction of the aligned Toll-homology domains from varied insect and human TLRs, vertebrate interleukin 1 receptors and MyD88 factors, and plant disease-resistance proteins recognizes a parallel beta/alpha fold with an acidic active site; a similar structure notably recurs in a class of response regulators broadly involved in transducing sensory information in bacteria.

摘要

果蝇Toll蛋白胞质结构域与人类白细胞介素1受体之间序列同源性的发现,使人们坚信这两种分子触发了与Rel型转录因子核转位相关的信号通路。这种保守的信号传导机制在昆虫和脊椎动物中都控制着一种进化上古老的免疫反应。我们报道了一类推定的人类受体的分子克隆,其蛋白质结构在细胞内和细胞外片段上都与果蝇Toll相似。五种人类Toll样受体(命名为TLRs 1 - 5)可能是果蝇分子的直接同源物,因此可能构成人类先天免疫中一个重要但未被认识的组成部分。有趣的是,TLRs在脊椎动物中的进化保留可能表明其具有另一种作用——类似于Toll在果蝇胚胎背腹分化中的作用——作为早期形态发生模式的调节因子。多种组织mRNA印迹显示人类TLRs的表达模式明显不同。通过荧光原位杂交和序列标签位点数据库分析,我们还表明相关的Tlr基因位于4号染色体(TLRs 1、2和3)、9号染色体(TLR4)和1号染色体(TLR5)上。对来自不同昆虫和人类TLRs、脊椎动物白细胞介素1受体和MyD88因子以及植物抗病蛋白的对齐Toll同源结构域进行结构预测,识别出具有酸性活性位点的平行β/α折叠;类似的结构在一类广泛参与细菌感觉信息转导的反应调节因子中显著重复出现。

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