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肿瘤坏死因子(TNF)与小鼠和人类体内TNF受体家族成员的相互作用。

Interactions of tumor necrosis factor (TNF) and TNF receptor family members in the mouse and human.

作者信息

Bossen Claudia, Ingold Karine, Tardivel Aubry, Bodmer Jean-Luc, Gaide Olivier, Hertig Sylvie, Ambrose Christine, Tschopp Jürg, Schneider Pascal

机构信息

Biochemistry Department, University of Lausanne, CH-1066 Epalinges, Switzerland.

出版信息

J Biol Chem. 2006 May 19;281(20):13964-71. doi: 10.1074/jbc.M601553200. Epub 2006 Mar 17.

Abstract

Ligands of the tumor necrosis factor superfamily (TNFSF) (4-1BBL, APRIL, BAFF, CD27L, CD30L, CD40L, EDA1, EDA2, FasL, GITRL, LIGHT, lymphotoxin alpha, lymphotoxin alphabeta, OX40L, RANKL, TL1A, TNF, TWEAK, and TRAIL) bind members of the TNF receptor superfamily (TNFRSF). A comprehensive survey of ligand-receptor interactions was performed using a flow cytometry-based assay. All ligands engaged between one and five receptors, whereas most receptors only bound one to three ligands. The receptors DR6, RELT, TROY, NGFR, and mouse TNFRH3 did not interact with any of the known TNFSF ligands, suggesting that they either bind other types of ligands, function in a ligand-independent manner, or bind ligands that remain to be identified. The study revealed that ligand-receptor pairs are either cross-reactive between human and mouse (e.g. Tweak/Fn14, RANK/RANKL), strictly species-specific (GITR/GITRL), or partially species-specific (e.g. OX40/OX40L, CD40/CD40L). Interestingly, the receptor binding patterns of lymphotoxin alpha and alphabeta are redundant in the human but not in the mouse system. Ligand oligomerization allowed detection of weak interactions, such as that of human TNF with mouse TNFR2. In addition, mouse APRIL exists as two different splice variants differing by a single amino acid. Although human APRIL does not interact with BAFF-R, the shorter variant of mouse APRIL exhibits weak but detectable binding to mouse BAFF-R.

摘要

肿瘤坏死因子超家族(TNFSF)的配体(4-1BBL、APRIL、BAFF、CD27L、CD30L、CD40L、EDA1、EDA2、FasL、GITRL、LIGHT、淋巴毒素α、淋巴毒素αβ、OX40L、RANKL、TL1A、TNF、TWEAK和TRAIL)与肿瘤坏死因子受体超家族(TNFRSF)的成员结合。使用基于流式细胞术的检测方法对配体-受体相互作用进行了全面调查。所有配体与一至五种受体结合,而大多数受体仅结合一至三种配体。受体DR6、RELT、TROY、NGFR和小鼠TNFRH3不与任何已知的TNFSF配体相互作用,这表明它们要么结合其他类型的配体,以不依赖配体的方式发挥作用,要么结合有待鉴定的配体。该研究表明,配体-受体对在人和小鼠之间要么具有交叉反应性(例如Tweak/Fn14、RANK/RANKL),要么严格具有物种特异性(GITR/GITRL),要么部分具有物种特异性(例如OX40/OX40L、CD40/CD40L)。有趣的是,淋巴毒素α和αβ的受体结合模式在人类系统中是冗余的,但在小鼠系统中并非如此。配体寡聚化能够检测到弱相互作用,例如人TNF与小鼠TNFR2之间的相互作用。此外,小鼠APRIL以两种不同的剪接变体形式存在,它们仅相差一个氨基酸。虽然人APRIL不与BAFF-R相互作用,但小鼠APRIL的较短变体与小鼠BAFF-R表现出弱但可检测到的结合。

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