Structure of the MST4 in Complex with MO25 Provides Insights into Its Activation Mechanism

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• 作者：Zhubing Shi¹ ; ² ; Shi Jiao¹ ; ² ; Zhen Zhang¹ ; ² ; Miao Ma¹ ; Zhao Zhang¹ ; Cuicui Chen¹ ; Ke Wang¹ ; Huizhen Wang¹ ; Wenjia Wang¹ ; Lei Zhang¹ ; Yun Zhao¹ ; ^{yunzhao@sibcb.ac.cn} ; Zhaocai Zhou¹ ; ^{zczhou@sibcb.ac.cn}
• 刊名：Structure
• 出版年：2013
• 出版时间：5 March, 2013
• 年：2013
• 卷：21
• 期：3
• 页码：449-461
• 全文大小：2650 K

文摘

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Summary

Mammalian STE20-like kinase MST4 regulates multiple cellular aspects such as cell polarity and proliferation. MST4 acts downstream of LKB1/MO25/STRAD complex to induce brush border formation. MO25 directly interacts with MST4 to promote its kinase activity. Here, we report the crystal structure of MST4 in complex with MO25. Association of MO25 rotates the ¦ÁC helix of MST4 toward its catalytic core, stabilizing the ¦ÁC helix in an active position. The kinase domain of MST4 forms a specific homodimer that is required for trans-autophosphorylation. MO25-stimulated activation of MST4 promotes apoptosis in HEK293T cells. Atomic resolution permitted the study of interface mutations capable of disrupting the MST4-MO25 interaction or?the kinase-domain-mediated homodimerization. These mutations impaired MST4 kinase activation and function within the cell. Collectively, our study identifies the activation mechanism of MST4 and provides a structural basis for further functional study.