Structural basis for recognition of N-formyl peptides as pathogen-associated molecular patterns

Author:

Chen Geng,Wang XiankunORCID,Liao QiwenORCID,Ge YunjunORCID,Jiao Haizhan,Chen Qiang,Liu YezhouORCID,Lyu Wenping,Zhu LizheORCID,van Zundert Gydo C. P.,Robertson Michael J.ORCID,Skiniotis GeorgiosORCID,Du YangORCID,Hu HongliORCID,Ye Richard D.ORCID

Abstract

AbstractThe formyl peptide receptor 1 (FPR1) is primarily responsible for detection of short peptides bearing N-formylated methionine (fMet) that are characteristic of protein synthesis in bacteria and mitochondria. As a result, FPR1 is critical to phagocyte migration and activation in bacterial infection, tissue injury and inflammation. How FPR1 distinguishes between formyl peptides and non-formyl peptides remains elusive. Here we report cryo-EM structures of human FPR1-Gi protein complex bound toS. aureus-derived peptide fMet-Ile-Phe-Leu (fMIFL) andE. coli-derived peptide fMet-Leu-Phe (fMLF). Both structures of FPR1 adopt an active conformation and exhibit a binding pocket containing the R2015.38XXXR2055.42(RGIIR) motif for formyl group interaction and receptor activation. This motif works together with D1063.33for hydrogen bond formation with the N-formyl group and with fMet, a model supported by MD simulation and functional assays of mutant receptors with key residues for recognition substituted by alanine. The cryo-EM model of agonist-bound FPR1 provides a structural basis for recognition of bacteria-derived chemotactic peptides with potential applications in developing FPR1-targeting agents.

Funder

Science, Technology and Innovation Commission of Shenzhen Municipality

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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