Partial ligand-receptor engagement yields functional bias at the human complement receptor, C5aR1

Pandey, Shubhi; Li, Xaria X.; Srivastava, Ashish; Baidya, Mithu; Kumari, Punita; Dwivedi, Hemlata; Ghosh, Eshan; Woodruff, Trent M.; Shukla, Arun K.

doi:10.1101/515700

Cited by 8 publications

(18 citation statements)

References 25 publications

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“…Notably, C5a also binds and activates a second receptor, C5aR2, albeit without any detectable G-protein coupling but with robust β arrestins (βarr) recruitment 33 . Three N-terminal tyrosine residues of C5aR2 may also be sulfated, but mutations of these residues did not significantly change C5a binding to C5aR2 34 , suggesting against the two-site binding mechanism for C5aR2.…”

Section: Discussionmentioning

confidence: 99%

Submolecular probing of the complement C5a receptor–ligand binding reveals a cooperative two-site binding mechanism

et al. 2020

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A current challenge to produce effective therapeutics is to accurately determine the location of the ligand-biding site and to characterize its properties. So far, the mechanisms underlying the functional activation of cell surface receptors by ligands with a complex binding mechanism remain poorly understood due to a lack of suitable nanoscopic methods to study them in their native environment. Here, we elucidated the ligand-binding mechanism of the human G protein-coupled C5a receptor (C5aR). We discovered for the first time a cooperativity between the two orthosteric binding sites. We found that the N-terminus C5aR serves as a kinetic trap, while the transmembrane domain acts as the functional site and both contributes to the overall high-affinity interaction. In particular, Asp282 plays a key role in ligand binding thermodynamics, as revealed by atomic force microscopy and steered molecular dynamics simulation. Our findings provide a new structural basis for the functional and mechanistic understanding of the GPCR family that binds large macromolecular ligands.

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Section: Discussionmentioning

confidence: 99%

Submolecular probing of the complement C5a receptor–ligand binding reveals a cooperative two-site binding mechanism

et al. 2020

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“…However, recent data obtained by our laboratory suggest that TLQP-21 has a lower potency compared with the C3aR1 agonist C3a 70–77 in guinea pigs (unpublished data), suggesting that TLQP-21 can be a safer template to target C3aR1 functions in multiple cell types, including adipocytes, while minimizing side effects. Additionally, our study revealed that murinizing hC3aR1 at five residues in the receptor binding pocket is sufficient to enhance the β-arrestin potency of mTLQP-21 (48-fold) or hTLQP-21 (28-fold) to a greater extent than C3a (8.5-fold), suggesting the existence of differences in agonist-mediated activation, possibly implying a biased agonism mechanism (Lotta et al, 2019; McCorvy et al, 2018; Pandey et al, 2019), which will be explored in future studies. A therapeutically beneficial biological activity of TLQP-21 has been established for energy balance, lipolysis, sexual behavior, blood pressure regulation, and glucose homeostasis, whereas the peptide can cause pain behavior (Bartolomucci et al, 2011; Cero et al, 2016; Doolen et al, 2017; Pinilla et al, 2011).…”

Section: Discussionmentioning

confidence: 75%

Peptide/Receptor Co-evolution Explains the Lipolytic Function of the Neuropeptide TLQP-21

et al. 2019

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SUMMARYStructural and functional diversity of peptides and GPCR result from long evolutionary processes. Even small changes in sequence can alter receptor activation, affecting therapeutic efficacy. We conducted a structure-function relationship study on the neuropeptide TLQP-21, a promising target for obesity, and its complement 3a receptor (C3aR1). After having characterized the TLQP-21/C3aR1 lipolytic mechanism, a homology modeling and molecular dynamics simulation identified the TLQP-21 binding motif and C3aR1 binding site for the human (h) and mouse (m) molecules. mTLQP-21 showed enhanced binding affinity and potency for hC3aR1 compared with hTLQP-21. Consistently, mTLQP-21, but not hTLQP-21, potentiates lipolysis in human adipocytes. These findings led us to uncover five mutations in the C3aR1 binding pocket of the rodent Murinae subfamily that are causal for enhanced calculated affinity and measured potency of TLQP-21. Identifying functionally relevant peptide/receptor co-evolution mechanisms can facilitate the development of innovative pharmacotherapies for obesity and other diseases implicating GPCRs.

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“…Despite evidence from the present study and others (43) that C5a can activate tumorigenic signaling pathways, in our hands, treatment of B16.F0 melanoma cells with recombinant mC5a had minimal effects on cell proliferation and migration. It should be noted, however, that although C5a-mediated ERK and p38 phosphorylation was detectible in B16.F0 cells, much greater increases in MAPK activation are observed in myeloid cells following C5a stimulation (;50-100-fold vs. the 1.5-2-fold observed for B16.F0 cells) (32), which may explain the lack of C5a functional activity observed in vitro. Nevertheless, the growth of C5aR1-expressing B16.F0 melanoma tumors was significantly reduced in C5aR1-deficient mice compared with wild-type mice, suggesting a predominant role for C5aR1-expressing host immune cells in the antitumor response.…”

Section: Discussionmentioning

confidence: 83%

“…However, the lack of a reliable antibody (31) precluded us from confirming C5aR2 protein expression in these cells. Both ERK and p38 MAPK are wellrecognized C5aR1-mediated signaling pathways (32). Incubation of B16.F0 cells with recombinant mC5a resulted in a modest (1.5-2-fold) increase in phosphorylation of ERK and p38 MAPK( Fig.…”

Section: C5ars Are Expressed By B16f0 Melanoma Cellsmentioning

confidence: 92%

C5a receptors C5aR1 and C5aR2 mediate opposing pathologies in a mouse model of melanoma

et al. 2019

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The canonical complement component 5a (C5a) receptor (C5aR) 1 has well‐described roles in tumorigenesis but the contribution of the second receptor, C5aR2, is unclear. The present study demonstrates that B16.F0 melanoma cells express mRNA for both C5aR1 and C5aR2 and signal through ERK and p38 MAPKs in response to C5a. Despite this, C5a had no impact on melanoma cell proliferation or migration in vitro. In vivo studies demonstrated that the growth of B16.F0 melanoma tumors was increased in C5aR2–/– mice but reduced in C5aR1–/– mice and wild‐type mice treated with a C5aR1 antagonist. Analysis of tumor‐infiltrating leukocyte populations showed no significant differences between wild‐type and C5aR2–/– mice. Conversely, percentages of myeloid‐derived suppressor cells, macrophages, and regulatory T lymphocytes were lower in tumors from C5aR1–/– mice, whereas total (CD3+) T lymphocytes and CD4+ subsets were higher. Analysis of cytokine and chemokine levels also showed plasma IFN‐γ was higher and tumor C‐C motif chemokine ligand 2 was lower in the absence of C5aR1. The results suggest that C5aR1 signaling supports melanoma growth by promoting infiltration of immunosuppressive leukocyte populations into the tumor microenvironment, whereas C5aR2 has a more restricted but beneficial role in limiting tumor growth. Overall, these data support the potential of C5aR1‐inhibitory therapies for melanoma.—Nabizadeh, J. A., Manthey, H. D., Panagides, N., Steyn, F. J., Lee, J. D., Li, X. X., Akhir, F. N. M., Chen, W., Boyle, G. M., Taylor, S. M., Woodruff, T. M., Rolfe, B. E. C5a receptors C5aR1 and C5aR2 mediate opposing pathologies in a mouse model of melanoma. FASEB J. 33, 11060–11071 (2019).http://www.fasebj.org

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Partial ligand-receptor engagement yields functional bias at the human complement receptor, C5aR1

Cited by 8 publications

References 25 publications

Submolecular probing of the complement C5a receptor–ligand binding reveals a cooperative two-site binding mechanism

Submolecular probing of the complement C5a receptor–ligand binding reveals a cooperative two-site binding mechanism

Peptide/Receptor Co-evolution Explains the Lipolytic Function of the Neuropeptide TLQP-21

C5a receptors C5aR1 and C5aR2 mediate opposing pathologies in a mouse model of melanoma

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