Ligand recognition and G protein coupling of the human itch receptor MRGPRX1

Author:

Guo Lulu,Zhang Yumu,Fang Guoxing,Tie Lu,Zhuang Yuming,Xue ChenyangORCID,Liu Qi,Zhang Minghui,Zhu Kongkai,You Chongzhao,Xu PeiyuORCID,Yuan Qingning,Zhang Chao,Liu Lei,Rong Naikang,Peng Shengxuan,Liu Yuan,Wang Chuanzheng,Luo Xin,Lv Zongyao,Kang DongweiORCID,Yu XiaoORCID,Zhang Cheng,Jiang Yi,Dong Xinzhong,Zhou Jiuyao,Liu ZhongminORCID,Yang FanORCID,Eric Xu H.ORCID,Sun Jin-PengORCID

Abstract

AbstractMRGPRX1, a Mas-related GPCR (MRGPR), is a key receptor for itch perception and targeting MRGPRX1 may have potential to treat both chronic itch and pain. Here we report cryo-EM structures of the MRGPRX1-Gi1 and MRGPRX1-Gq trimers in complex with two peptide ligands, BAM8-22 and CNF-Tx2. These structures reveal a shallow orthosteric pocket and its conformational plasticity for sensing multiple different peptidic itch allergens. Distinct from MRGPRX2, MRGPRX1 contains a unique pocket feature at the extracellular ends of TM3 and TM4 to accommodate the peptide C-terminal “RF/RY” motif, which could serve as key mechanisms for peptidic allergen recognition. Below the ligand binding pocket, the G6.48XP6.50F6.51G6.52X(2)F/W6.55 motif is essential for the inward tilting of the upper end of TM6 to induce receptor activation. Moreover, structural features inside the ligand pocket and on the cytoplasmic side of MRGPRX1 are identified as key elements for both Gi and Gq signaling. Collectively, our studies provide structural insights into understanding itch sensation, MRGPRX1 activation, and downstream G protein signaling.

Funder

China National Funds for Distinguished Young Scientists

National Natural Science Foundation of China

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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