XIAP Induces NF-ba;B Activation via the BIR1/TAB1 Interaction and BIR1 Dimerization

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• 作者：Miao Lu ; Su-Chang Lin ; Yihua Huang ; Young Jun Kang ; Rebecca Rich ; Yu-Chih Lo ; David Myszka ; Jiahuai Han ; Hao Wu
• 关键词：SIGNALING ; CELLCYCLE
• 刊名：Molecular Cell
• 出版年：2007
• 期刊代码：111_10972765
• 类别：bio
• 出版时间：8 June 2007
• 卷：26
• 期：5
• 页码：689-702
• 文件大小：2284 K

摘要

Summary

In addition to caspase inhibition, X-linked inhibitor of apoptosis (XIAP) induces NF-ba;B and MAP kinase activation during TGF-b and BMP receptor signaling and upon overexpression. Here we show that the BIR1 domain of XIAP, which has no previously ascribed function, directly interacts with TAB1 to induce NF-ba;B activation. TAB1 is an upstream adaptor for the activation of the kinase TAK1, which in turn couples to the NF-ba;B pathway. We report the crystal structures of BIR1, TAB1, and the BIR1/TAB1 complex. The BIR1/TAB1 structure reveals a striking butterfly-shaped dimer and the detailed interaction between BIR1 and TAB1. Structure-based mutagenesis and knockdown of TAB1 show unambiguously that the BIR1/TAB1 interaction is crucial for XIAP-induced TAK1 and NF-ba;B activation. We show that although not interacting with BIR1, Smac, the antagonist for caspase inhibition by XIAP, also inhibits the XIAP/TAB1 interaction. Disruption of BIR1 dimerization abolishes XIAP-mediated NF-ba;B activation, implicating a proximity-induced mechanism for TAK1 activation.