AI Article Synopsis

  • The class B secretin GPCR (SecR) has important roles in various physiological functions and potential therapeutic applications for metabolic and cardiovascular diseases.
  • A study utilized cryo-electron microscopy, molecular dynamics, and biochemical methods to determine the 2.3 Å structure of secretin bound to the SecR:Gs complex, highlighting unique interactions compared to similar proteins.
  • Findings suggest that secretin engages with SecR in a dynamic manner, with key initial interactions occurring between the peptide's N-terminus and the receptor's extracellular loops following the binding of its C-terminus.

Article Abstract

The class B secretin GPCR (SecR) has broad physiological effects, with target potential for treatment of metabolic and cardiovascular disease. Molecular understanding of SecR binding and activation is important for its therapeutic exploitation. We combined cryo-electron microscopy, molecular dynamics, and biochemical cross-linking to determine a 2.3 Å structure, and interrogate dynamics, of secretin bound to the SecR:Gs complex. SecR exhibited a unique organization of its extracellular domain (ECD) relative to its 7-transmembrane (TM) core, forming more extended interactions than other family members. Numerous polar interactions formed between secretin and the receptor extracellular loops (ECLs) and TM helices. Cysteine-cross-linking, cryo-electron microscopy multivariate analysis and molecular dynamics simulations revealed that interactions between peptide and receptor were dynamic, and suggested a model for initial peptide engagement where early interactions between the far N-terminus of the peptide and SecR ECL2 likely occur following initial binding of the peptide C-terminus to the ECD.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7435274PMC
http://dx.doi.org/10.1038/s41467-020-17791-4DOI Listing

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