Article Synopsis

  • Our sense of smell relies on around 400 odorant receptors in the human genome, which work together to detect various odor molecules.
  • Using cryo-electron microscopy, researchers revealed how the odorant propionate binds to the receptor OR51E2, highlighting the specific interactions necessary for receptor activation.
  • Mutations in the receptor's binding site showed that the selectivity for different fatty acid lengths depends on how tightly the odorant fits, and simulations indicated that the binding of propionate leads to crucial changes that activate the receptor.

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Article Abstract

Our sense of smell enables us to navigate a vast space of chemically diverse odour molecules. This task is accomplished by the combinatorial activation of approximately 400 odorant G protein-coupled receptors encoded in the human genome. How odorants are recognized by odorant receptors remains unclear. Here we provide mechanistic insight into how an odorant binds to a human odorant receptor. Using cryo-electron microscopy, we determined the structure of the active human odorant receptor OR51E2 bound to the fatty acid propionate. Propionate is bound within an occluded pocket in OR51E2 and makes specific contacts critical to receptor activation. Mutation of the odorant-binding pocket in OR51E2 alters the recognition spectrum for fatty acids of varying chain length, suggesting that odorant selectivity is controlled by tight packing interactions between an odorant and an odorant receptor. Molecular dynamics simulations demonstrate that propionate-induced conformational changes in extracellular loop 3 activate OR51E2. Together, our studies provide a high-resolution view of chemical recognition of an odorant by a vertebrate odorant receptor, providing insight into how this large family of G protein-coupled receptors enables our olfactory sense.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10580732PMC
http://dx.doi.org/10.1038/s41586-023-05798-yDOI Listing

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