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Potent Cyclic Antagonists of the Complement C5a Receptor on Human Polymorphonuclear Leukocytes. Relationships between Structures and Activity
Human C5a is a plasma protein with potent chemoattractant and pro-inflammatory properties, and its overexpression correlates with severity of inflammatory diseases. C5a binds to its G protein-coupled receptor (C5aR) on polymorphonuclear leukocytes (PMNLs) through a high-affinity helical bundle and a...
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Published in: | Molecular pharmacology 2004-04, Vol.65 (4), p.868-879 |
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Main Authors: | , , , , , , , , , , , |
Format: | Article |
Language: | English |
Subjects: | |
Citations: | Items that this one cites Items that cite this one |
Online Access: | Get full text |
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Summary: | Human C5a is a plasma protein with potent chemoattractant and pro-inflammatory properties, and its overexpression correlates
with severity of inflammatory diseases. C5a binds to its G protein-coupled receptor (C5aR) on polymorphonuclear leukocytes
(PMNLs) through a high-affinity helical bundle and a low-affinity C terminus, the latter being solely responsible for receptor
activation. Potent and selective C5a antagonists are predicted to be effective anti-inflammatory drugs, but no pharmacophore
for small molecule antagonists has yet been developed, and it would significantly aid drug design. We have hypothesized that
a turn conformation is important for activity of the C terminus of C5a and herein report small cyclic peptides that are stable
turn mimics with potent antagonism at C5aR on human PMNLs. A comparison of solution structures for the C terminus of C5a,
small acyclic peptide ligands, and cyclic antagonists supports the importance of a turn for receptor binding. Competition
between a cyclic antagonist and either C5a or an acyclic agonist for C5aR on PMNLs supports a common or overlapping binding
site on the C5aR. Structure-activity relationships for 60 cyclic analogs were evaluated by competitive radioligand binding
with C5a (affinity) and myeloperoxidase release (antagonist potency) from human PMNLs, with 20 compounds having high antagonist
potencies (IC 50 , 20 nM-1 μM). Computer modeling comparisons reveal that potent antagonists share a common cyclic backbone shape, with affinity-determining
side chains of defined volume projecting from the cyclic scaffold. These results define a new pharmacophore for C5a antagonist
development and advance our understanding of ligand recognition and receptor activation of this G protein-coupled receptor. |
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ISSN: | 0026-895X 1521-0111 |
DOI: | 10.1124/mol.65.4.868 |