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Higher-Order Clustering of the Transmembrane Anchor of DR5 Drives Signaling.

Cell. 2019-03; 
PanLiqiang,FuTian-Min,ZhaoWenbin,ZhaoLinlin,ChenWen,QiuChixiao,LiuWenhui,LiuZhijun,PiaiAlessandro,FuQingshan,ChenShuqing,WuHao,ChouJam
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Gene Synthesis The human DR5 (isoform 1) fragment, residues 208 – 242, corresponding to the TMH was synthesized by GenScript (Piscataway, NJ) (Figure S1A). Get A Quote

摘要

Receptor clustering on the cell membrane is critical in the signaling of many immunoreceptors, and this mechanism has previously been attributed to the extracellular and/or the intracellular interactions. Here, we report an unexpected finding that for death receptor 5 (DR5), a receptor in the tumor necrosis factor receptor superfamily, the transmembrane helix (TMH) alone in the receptor directly assembles a higher-order structure to drive signaling and that this structure is inhibited by the unliganded ectodomain. Nuclear magnetic resonance structure of the TMH in bicelles shows distinct trimerization and dimerization faces, allowing formation of dimer-trimer interaction networks. Single-TMH mutations... More

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