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小鼠淋巴结归巢受体cDNA克隆编码一种揭示串联相互作用结构域的糖蛋白。

Mouse lymph node homing receptor cDNA clone encodes a glycoprotein revealing tandem interaction domains.

作者信息

Siegelman M H, van de Rijn M, Weissman I L

机构信息

Department of Pathology, Stanford University School of Medicine, CA 94305.

出版信息

Science. 1989 Mar 3;243(4895):1165-72. doi: 10.1126/science.2646713.

Abstract

Isolation of a clone encoding the mouse lymph node homing receptor reveals a deduced protein with an unusual protein mosaic architecture, containing a separate carbohydrate-binding (lectin) domain, an epidermal growth factor-like (EGF) domain, and an extracellular precisely duplicated repeat unit, which preserves the motif seen in the homologous repeat structure of complement regulatory proteins and other proteins. The receptor molecule is potentially highly glycosylated, and contains an apparent transmembrane region. Analysis of messenger RNA transcripts reveals a predominantly lymphoid distribution in direct relation to the cell surface expression of the MEL-14 determinant, and the cDNA clone is shown to confer the MEL-14 epitope in heterologous cells. The many novel features, including ubiquitination, embodied in this single receptor molecule form the basis for numerous approaches to the study of cell-cell interactions.

摘要

编码小鼠淋巴结归巢受体的克隆的分离,揭示了一种推导的蛋白质,其具有不寻常的蛋白质镶嵌结构,包含一个单独的碳水化合物结合(凝集素)结构域、一个表皮生长因子样(EGF)结构域和一个细胞外精确重复的重复单元,该重复单元保留了在补体调节蛋白和其他蛋白质的同源重复结构中所见的基序。该受体分子可能高度糖基化,并含有一个明显的跨膜区域。信使核糖核酸转录本的分析揭示了与MEL-14决定簇的细胞表面表达直接相关的主要淋巴样分布,并且该cDNA克隆在异源细胞中显示出赋予MEL-14表位。这个单一受体分子中体现的许多新特征,包括泛素化,构成了研究细胞间相互作用的众多方法的基础。

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