4.7 Article

Conserved C-terminal motifs in odorant receptors instruct their cell surface expression and cAMP signaling

期刊

FASEB JOURNAL
卷 35, 期 2, 页码 -

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WILEY
DOI: 10.1096/fj.202000182RR

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GPCR; helix 8; intracellular transport; luciferase assay; phylogenetic trees

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The study reveals the presence of highly conserved C-terminal amino acid motifs in odorant receptors, which differentiate between class-I and class-II receptors and increase in number during evolution. Experimentation shows that these motifs have differential impacts on the cell surface expression and cAMP signaling of odorant receptors, with some individual amino acids and combinations playing a key role.
The highly individual plasma membrane expression and cAMP signaling of odorant receptors have hampered their ligand assignment and functional characterization in test cell systems. Chaperones have been identified to support the cell surface expression of only a portion of odorant receptors, with mechanisms remaining unclear. The presence of amino acid motifs that might be responsible for odorant receptors' individual intracellular retention or cell surface expression, and thus, for cAMP signaling, is under debate: so far, no such protein motifs have been suggested. Here, we demonstrate the existence of highly conserved C-terminal amino acid motifs, which discriminate at least between class-I and class-II odorant receptors, with their numbers of motifs increasing during evolution, by comparing C-terminal protein sequences from 4808 receptors across eight species. Truncation experiments and mutation analysis of C-terminal motifs, largely overlapping with helix 8, revealed single amino acids and their combinations to have differential impact on the cell surface expression and on stimulus-dependent cAMP signaling of odorant receptors in NxG 108CC15 cells. Our results demonstrate class-specific and individual C-terminal motif equipment of odorant receptors, which instruct their functional expression in a test cell system, and in situ may regulate their individual cell surface expression and intracellular cAMP signaling.

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