7sf7 Citations

The tethered peptide activation mechanism of adhesion GPCRs.

Barros-Álvarez X, Nwokonko RM, Vizurraga A, Matzov D, He F, Papasergi-Scott MM, Robertson MJ, Panova O, Yardeni EH, Seven AB, Kwarcinski FE, Su H, Peroto MC, Meyerowitz JG, Shalev-Benami M, Tall GG, Skiniotis G
Nature 604 757-762 (2022)
Cited: 41 times
EuropePMC logo PMID: 35418682

Abstract

Adhesion G-protein-coupled receptors (aGPCRs) are characterized by the presence of auto-proteolysing extracellular regions that are involved in cell-cell and cell-extracellular matrix interactions1. Self cleavage within the aGPCR auto-proteolysis-inducing (GAIN) domain produces two protomers-N-terminal and C-terminal fragments-that remain non-covalently attached after receptors reach the cell surface1. Upon dissociation of the N-terminal fragment, the C-terminus of the GAIN domain acts as a tethered agonist (TA) peptide to activate the seven-transmembrane domain with a mechanism that has been poorly understood2-5. Here we provide cryo-electron microscopy snapshots of two distinct members of the aGPCR family, GPR56 (also known as ADGRG1) and latrophilin 3 (LPHN3 (also known as ADGRL3)). Low-resolution maps of the receptors in their N-terminal fragment-bound state indicate that the GAIN domain projects flexibly towards the extracellular space, keeping the encrypted TA peptide away from the seven-transmembrane domain. High-resolution structures of GPR56 and LPHN3 in their active, G-protein-coupled states, reveal that after dissociation of the extracellular region, the decrypted TA peptides engage the seven-transmembrane domain core with a notable conservation of interactions that also involve extracellular loop 2. TA binding stabilizes breaks in the middle of transmembrane helices 6 and 7 that facilitate aGPCR coupling and activation of heterotrimeric G proteins. Collectively, these results enable us to propose a general model for aGPCR activation.

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  1. The GPCR properties of polycystin-1- A new paradigm. Maser RL, Calvet JP, Parnell SC. Front Mol Biosci 9 1035507 (2022)
  2. Structure, function and drug discovery of GPCR signaling. Cheng L, Xia F, Li Z, Shen C, Yang Z, Hou H, Sun S, Feng Y, Yong X, Tian X, Qin H, Yan W, Shao Z. Mol Biomed 4 46 (2023)
  3. Adhesion G protein-coupled receptor gluing action guides tissue development and disease. Sreepada A, Tiwari M, Pal K. J Mol Med (Berl) 100 1355-1372 (2022)
  4. Role of Adhesion G Protein-Coupled Receptors in Immune Dysfunction and Disorder. Tseng WY, Stacey M, Lin HH. Int J Mol Sci 24 5499 (2023)
  5. Structural clarity is brought to adhesion G protein-coupled receptor tethered agonism. Gupta C, Bernadyn TF, Tall GG. Basic Clin Pharmacol Toxicol 133 295-300 (2023)
  6. The clinical relevance of the adhesion G protein-coupled receptor F5 for human diseases and cancers. Jacenik D, Hikisz P, Beswick EJ, Fichna J. Biochim Biophys Acta Mol Basis Dis 1869 166683 (2023)
  7. Mechanosensitive GPCRs and ion channels in shear stress sensing. Xiao R, Liu J, Xu XZS. Curr Opin Cell Biol 84 102216 (2023)
  8. AI-Driven Deep Learning Techniques in Protein Structure Prediction. Chen L, Li Q, Nasif KFA, Xie Y, Deng B, Niu S, Pouriyeh S, Dai Z, Chen J, Xie CY. Int J Mol Sci 25 8426 (2024)

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