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- W4292430006 abstract "G protein-coupled receptors (GPCRs) constitute the largest class of membrane proteins that transduce signals across the plasma membrane and orchestrate a multitude of physiological processes within cells. The serotonin1A receptor is a crucial neurotransmitter receptor in the GPCR family involved in a multitude of neurological, behavioral and cognitive functions. We have previously shown, using a combination of experimental and simulation approaches, that membrane cholesterol acts as a key regulator of organization, dynamics, signaling and endocytosis of the serotonin1A receptor. In addition, we showed that membrane cholesterol stabilizes the serotonin1A receptor against thermal deactivation. In the present work, we explored the molecular basis of cholesterol-induced thermal stability of the serotonin1A receptor. For this, we explored the possible role of the K101 residue in a cholesterol recognition/interaction amino acid consensus (CRAC) motif in transmembrane helix 2 in conferring the thermal stability of the serotonin1A receptor. Our results show that a mutation in the K101 residue leads to loss in thermal stability of the serotonin1A receptor imparted by cholesterol, independent of membrane cholesterol content. We envision that our results could have potential implications in structural biological advancements of GPCRs and design of thermally stabilized receptors for drug development." @default.
- W4292430006 created "2022-08-20" @default.
- W4292430006 creator A5063835467 @default.
- W4292430006 creator A5083046186 @default.
- W4292430006 creator A5083143380 @default.
- W4292430006 date "2022-08-20" @default.
- W4292430006 modified "2023-09-25" @default.
- W4292430006 title "Lysine 101 in the CRAC Motif in Transmembrane Helix 2 Confers Cholesterol-Induced Thermal Stability to the Serotonin1A Receptor" @default.
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- W4292430006 doi "https://doi.org/10.1007/s00232-022-00262-w" @default.
- W4292430006 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/35986776" @default.
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