Systematic HOIP interactome profiling reveals critical roles of linear ubiquitination in tissue homeostasis

Author:

Fu Yesheng,Li Lei,Zhang XinORCID,Deng Zhikang,Wu Ying,Chen Wenzhe,Liu Yuchen,He Shan,Wang JianORCID,Xie Yuping,Tu Zhiwei,Lyu Yadi,Wei Yange,Wang Shujie,Cui Chun-PingORCID,Liu Cui HuaORCID,Zhang LingqiangORCID

Abstract

AbstractLinear ubiquitination catalyzed by HOIL-1-interacting protein (HOIP), the key component of the linear ubiquitination assembly complex, plays fundamental roles in tissue homeostasis by executing domain-specific regulatory functions. However, a proteome-wide analysis of the domain-specific interactome of HOIP across tissues is lacking. Here, we present a comprehensive mass spectrometry-based interactome profiling of four HOIP domains in nine mouse tissues. The interaction dataset provides a high-quality HOIP interactome resource with an average of approximately 90 interactors for each bait per tissue. HOIP tissue interactome presents a systematic understanding of linear ubiquitination functions in each tissue and also shows associations of tissue functions to genetic diseases. HOIP domain interactome characterizes a set of previously undefined linear ubiquitinated substrates and elucidates the cross-talk among HOIP domains in physiological and pathological processes. Moreover, we show that linear ubiquitination of Integrin-linked protein kinase (ILK) decreases focal adhesion formation and promotes the detachment of Shigella flexneri-infected cells. Meanwhile, Hoip deficiency decreases the linear ubiquitination of Smad ubiquitination regulatory factor 1 (SMURF1) and enhances its E3 activity, finally causing a reduced bone mass phenotype in mice. Overall, our work expands the knowledge of HOIP-interacting proteins and provides a platform for further discovery of linear ubiquitination functions in tissue homeostasis.

Funder

National Natural Science Foundation of China

Publisher

Springer Science and Business Media LLC

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