Selective Hexapeptide Agonists and Antagonists for Human Complement C3a Receptor

Human anaphylatoxin C3a, formed through cleavage of complement protein C3, is a potent effector of innate immunity via activation of its G protein coupled receptor, human C3aR. Previously reported short peptide ligands for this receptor either have low potency or lack receptor selectivity. Here we r...

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Veröffentlicht in:	Journal of medicinal chemistry 2010-07, Vol.53 (13), p.4938-4948
Hauptverfasser:	Scully, Conor C. G, Blakeney, Jade S, Singh, Ranee, Hoang, Huy N, Abbenante, Giovanni, Reid, Robert C, Fairlie, David P
Format:	Artikel
Sprache:	eng
Schlagworte:	Binding, Competitive Calcium - metabolism Complement C3a - metabolism Humans Inhibitory Concentration 50 Magnetic Resonance Spectroscopy Oligopeptides - chemical synthesis Oligopeptides - chemistry Oligopeptides - pharmacology Receptors, Complement - agonists Receptors, Complement - antagonists & inhibitors Receptors, Complement - metabolism Spectrometry, Mass, Electrospray Ionization Structure-Activity Relationship U937 Cells
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container_title	Journal of medicinal chemistry
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creator	Scully, Conor C. G Blakeney, Jade S Singh, Ranee Hoang, Huy N Abbenante, Giovanni Reid, Robert C Fairlie, David P
description	Human anaphylatoxin C3a, formed through cleavage of complement protein C3, is a potent effector of innate immunity via activation of its G protein coupled receptor, human C3aR. Previously reported short peptide ligands for this receptor either have low potency or lack receptor selectivity. Here we report the first small peptide agonists that are both potent and selective for human C3aR, derived from structure−activity relationships of peptides based on the C-terminus of C3a. Affinity for C3aR was examined by competitive binding with 125I-labeled C3a to human macrophages, agonist versus antagonist activity measured using fluorescence detection of intracellular calcium, and general selectivity monitored by C3a-induced receptor desensitization. An NMR structure for an agonist in DMSO showed a β-turn motif that may be important for C3aR binding and activation. Derivatization produced a noncompetitive and insurmountable antagonist of C3aR. Small molecule C3a agonists and antagonists may be valuable probes of immunity and inflammatory diseases.
doi_str_mv	10.1021/jm1003705
format	Article
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Affinity for C3aR was examined by competitive binding with 125I-labeled C3a to human macrophages, agonist versus antagonist activity measured using fluorescence detection of intracellular calcium, and general selectivity monitored by C3a-induced receptor desensitization. An NMR structure for an agonist in DMSO showed a β-turn motif that may be important for C3aR binding and activation. Derivatization produced a noncompetitive and insurmountable antagonist of C3aR. 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Affinity for C3aR was examined by competitive binding with 125I-labeled C3a to human macrophages, agonist versus antagonist activity measured using fluorescence detection of intracellular calcium, and general selectivity monitored by C3a-induced receptor desensitization. An NMR structure for an agonist in DMSO showed a β-turn motif that may be important for C3aR binding and activation. Derivatization produced a noncompetitive and insurmountable antagonist of C3aR. 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Here we report the first small peptide agonists that are both potent and selective for human C3aR, derived from structure−activity relationships of peptides based on the C-terminus of C3a. Affinity for C3aR was examined by competitive binding with 125I-labeled C3a to human macrophages, agonist versus antagonist activity measured using fluorescence detection of intracellular calcium, and general selectivity monitored by C3a-induced receptor desensitization. An NMR structure for an agonist in DMSO showed a β-turn motif that may be important for C3aR binding and activation. Derivatization produced a noncompetitive and insurmountable antagonist of C3aR. Small molecule C3a agonists and antagonists may be valuable probes of immunity and inflammatory diseases.</abstract><cop>United States</cop><pub>American Chemical Society</pub><pmid>20527893</pmid><doi>10.1021/jm1003705</doi><tpages>11</tpages></addata></record>
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source	MEDLINE; ACS Publications
subjects	Binding, Competitive Calcium - metabolism Complement C3a - metabolism Humans Inhibitory Concentration 50 Magnetic Resonance Spectroscopy Oligopeptides - chemical synthesis Oligopeptides - chemistry Oligopeptides - pharmacology Receptors, Complement - agonists Receptors, Complement - antagonists & inhibitors Receptors, Complement - metabolism Spectrometry, Mass, Electrospray Ionization Structure-Activity Relationship U937 Cells
title	Selective Hexapeptide Agonists and Antagonists for Human Complement C3a Receptor
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