2024
DOI: 10.1016/j.jbc.2023.105549
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Functional profiling of the G protein-coupled receptor C3aR1 reveals ligand-mediated biased agonism

Pedro Rodriguez,
Lauren J. Laskowski,
Jean Pierre Pallais
et al.
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Cited by 3 publications
(5 citation statements)
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“…Additionally, an obstacle in targeting C3aR lies in the lack of effective pharmacological approaches. The commonly used antagonist, SB290157, also displays agonistic effects [18,100], posing difficulties in accurately assessing the impact of pharmacological inhibition of the receptor in animal models. This challenge was further hampered by the absence of structural information of the receptor to design efficient inhibitory molecules.…”
Section: Discussionmentioning
confidence: 99%
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“…Additionally, an obstacle in targeting C3aR lies in the lack of effective pharmacological approaches. The commonly used antagonist, SB290157, also displays agonistic effects [18,100], posing difficulties in accurately assessing the impact of pharmacological inhibition of the receptor in animal models. This challenge was further hampered by the absence of structural information of the receptor to design efficient inhibitory molecules.…”
Section: Discussionmentioning
confidence: 99%
“…While some evidence in the literature suggests that C3aR activation triggers Gαi-family, other studies indicate that Gαs and Gαq are involved [14][15][16][17][18]. In a recent study it was identified that C3aR primarily couples to Gαi/o/z subtype to inhibit cAMP accumulation and mediate calcium influx [18]. The most reported downstream effect of C3aR activation is an increase in intracellular calcium [19][20][21], but other molecular pathways such as GSK3β, Wnt, ERK, JAK/STAT, and HIF1α signaling are also found to be downstream of C3aR activation [22][23][24][25][26].…”
Section: C3ar: a Review Of Structure And Intracellular Signalingmentioning
confidence: 99%
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