FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4289755428> ?p ?o ?g. }

• W4289755428 endingPage "102328" @default.
• W4289755428 startingPage "102328" @default.
• W4289755428 abstract "Within the intestine, the human G protein-coupled receptor (GPCR) GPR35 is involved in oncogenic signaling, bacterial infections, and inflammatory bowel disease. GPR35 is known to be expressed as two distinct isoforms that differ only in the length of their extracellular N-termini by 31 amino acids, but detailed insights into their functional differences are lacking. Through gene expression analysis in immune and gastrointestinal cells, we show that these isoforms emerge from distinct promoter usage and alternative splicing. Additionally, we employed optical assays in living cells to thoroughly profile both GPR35 isoforms for constitutive and ligand-induced activation and signaling of 10 different heterotrimeric G proteins, ligand-induced arrestin recruitment, and receptor internalization. Our results reveal that the extended N-terminus of the long isoform limits G protein activation yet elevates receptor-β-arrestin interaction. To better understand the structural basis for this bias, we examined structural models of GPR35 and conducted experiments with mutants of both isoforms. We found that a proposed disulfide bridge between the N-terminus and extracellular loop 3, present in both isoforms, is crucial for constitutive G13 activation, while an additional cysteine contributed by the extended N-terminus of the long GPR35 isoform limits the extent of agonist-induced receptor-β-arrestin2 interaction. The pharmacological profiles and mechanistic insights of our study provide clues for the future design of isoform-specific GPR35 ligands that selectively modulate GPR35-transducer interactions and allow for mechanism-based therapies against, for example, inflammatory bowel disease or bacterial infections of the gastrointestinal system." @default.
• W4289755428 created "2022-08-04" @default.
• W4289755428 creator A5000142376 @default.
• W4289755428 creator A5014235930 @default.
• W4289755428 creator A5018147300 @default.
• W4289755428 creator A5029316422 @default.
• W4289755428 creator A5048470753 @default.
• W4289755428 creator A5059551039 @default.
• W4289755428 creator A5060927839 @default.
• W4289755428 creator A5065829427 @default.
• W4289755428 date "2022-09-01" @default.
• W4289755428 modified "2023-10-14" @default.
• W4289755428 title "Isoforms of GPR35 have distinct extracellular N-termini that allosterically modify receptor-transducer coupling and mediate intracellular pathway bias" @default.
• W4289755428 cites W1014257459 @default.
• W4289755428 cites W1496442060 @default.
• W4289755428 cites W1984584304 @default.
• W4289755428 cites W1996095240 @default.
• W4289755428 cites W2000804199 @default.
• W4289755428 cites W2013160020 @default.
• W4289755428 cites W2057885467 @default.
• W4289755428 cites W2063557162 @default.
• W4289755428 cites W2065156829 @default.
• W4289755428 cites W2074259147 @default.
• W4289755428 cites W2110877685 @default.
• W4289755428 cites W2126255798 @default.
• W4289755428 cites W2169456326 @default.
• W4289755428 cites W2171108415 @default.
• W4289755428 cites W2239632319 @default.
• W4289755428 cites W2306193122 @default.
• W4289755428 cites W2717582465 @default.
• W4289755428 cites W2785540442 @default.
• W4289755428 cites W2806449183 @default.
• W4289755428 cites W2886296986 @default.
• W4289755428 cites W2900501651 @default.
• W4289755428 cites W2902049135 @default.
• W4289755428 cites W2906670900 @default.
• W4289755428 cites W2955721734 @default.
• W4289755428 cites W2980493900 @default.
• W4289755428 cites W3020888971 @default.
• W4289755428 cites W3034718462 @default.
• W4289755428 cites W3045638775 @default.
• W4289755428 cites W3046931406 @default.
• W4289755428 cites W3083406432 @default.
• W4289755428 cites W3096284929 @default.
• W4289755428 cites W3107021591 @default.
• W4289755428 cites W3110608978 @default.
• W4289755428 cites W3161570546 @default.
• W4289755428 cites W3177828909 @default.
• W4289755428 cites W3180740192 @default.
• W4289755428 cites W3198393254 @default.
• W4289755428 cites W3201980172 @default.
• W4289755428 cites W3209908325 @default.
• W4289755428 cites W3211421769 @default.
• W4289755428 cites W3215503891 @default.
• W4289755428 cites W4210451509 @default.
• W4289755428 cites W4211205596 @default.
• W4289755428 cites W4223552703 @default.
• W4289755428 doi "https://doi.org/10.1016/j.jbc.2022.102328" @default.
• W4289755428 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/35933013" @default.
• W4289755428 hasPublicationYear "2022" @default.
• W4289755428 type Work @default.
• W4289755428 citedByCount "6" @default.
• W4289755428 countsByYear W42897554282022 @default.
• W4289755428 countsByYear W42897554282023 @default.
• W4289755428 crossrefType "journal-article" @default.
• W4289755428 hasAuthorship W4289755428A5000142376 @default.
• W4289755428 hasAuthorship W4289755428A5014235930 @default.
• W4289755428 hasAuthorship W4289755428A5018147300 @default.
• W4289755428 hasAuthorship W4289755428A5029316422 @default.
• W4289755428 hasAuthorship W4289755428A5048470753 @default.
• W4289755428 hasAuthorship W4289755428A5059551039 @default.
• W4289755428 hasAuthorship W4289755428A5060927839 @default.
• W4289755428 hasAuthorship W4289755428A5065829427 @default.
• W4289755428 hasBestOaLocation W42897554281 @default.
• W4289755428 hasConcept C104317684 @default.
• W4289755428 hasConcept C135285700 @default.
• W4289755428 hasConcept C170493617 @default.
• W4289755428 hasConcept C174510640 @default.
• W4289755428 hasConcept C53345823 @default.
• W4289755428 hasConcept C55493867 @default.
• W4289755428 hasConcept C62478195 @default.
• W4289755428 hasConcept C86803240 @default.
• W4289755428 hasConcept C95444343 @default.
• W4289755428 hasConceptScore W4289755428C104317684 @default.
• W4289755428 hasConceptScore W4289755428C135285700 @default.
• W4289755428 hasConceptScore W4289755428C170493617 @default.
• W4289755428 hasConceptScore W4289755428C174510640 @default.
• W4289755428 hasConceptScore W4289755428C53345823 @default.
• W4289755428 hasConceptScore W4289755428C55493867 @default.
• W4289755428 hasConceptScore W4289755428C62478195 @default.
• W4289755428 hasConceptScore W4289755428C86803240 @default.
• W4289755428 hasConceptScore W4289755428C95444343 @default.
• W4289755428 hasFunder F4320320879 @default.
• W4289755428 hasFunder F4320321491 @default.
• W4289755428 hasFunder F4320322315 @default.
• W4289755428 hasFunder F4320322581 @default.
• W4289755428 hasFunder F4320323584 @default.
• W4289755428 hasFunder F4320325957 @default.

• next