2009
DOI: 10.1002/psc.1146
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Structural determinants for selective recognition of peptide ligands for endothelin receptor subtypes ETA and ETB

Abstract: The molecular basis for recognition of peptide ligands endothelin-1, -2 and -3 in endothelin receptors is poorly understood. Especially the origin of ligand selectivity for ET(A) or ET(B) is not clearly resolved. We derived sequence-structure-function relationships of peptides and receptors from mutational data and homology modeling. Our major findings are the dissection of peptide ligands into four epitopes and the delineation of four complementary structural portions on receptor side explaining ligand recogn… Show more

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Cited by 25 publications
(26 citation statements)
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“…However, TMI-III, VII and extracellular loops appear to contain an agonist binding motif, 39,40 and the E1 loop seems to be more particularly involved in the interaction with ET-1. 41 The observation that the epitope sequences recognized by rendomab-B4 are located in a region that has not been implicated in ligand binding is consistent with our binding data showing that there was no competition between the antibody and ETs.…”
Section: Discussionsupporting
confidence: 88%
“…However, TMI-III, VII and extracellular loops appear to contain an agonist binding motif, 39,40 and the E1 loop seems to be more particularly involved in the interaction with ET-1. 41 The observation that the epitope sequences recognized by rendomab-B4 are located in a region that has not been implicated in ligand binding is consistent with our binding data showing that there was no competition between the antibody and ETs.…”
Section: Discussionsupporting
confidence: 88%
“…40,41 Collectively, these findings highlight the value of rendomab-B1 in investigating hETBR structure and in gathering more information about the location of the endothelin binding site, whose precise delineation is still unclear despite several recent publications tackling the issue. 42,43 Furthermore, this original noncompetitive inhibitory mechanism, rarely found for small inhibitory molecules like BQ788 that generally compete with natural ligands for the receptor orthosteric site, underlines the value of developing therapeutic antibodies that offer the possibility of targeting original epitopes on GPCRs, potentially linked to new pharmacological activities and better receptor selectivity. 22 To our knowledge, this is the first time that an antagonist mAb targeting hETBR has been described.…”
Section: Discussionmentioning
confidence: 99%
“…Since the major linear epitopes of our antibodies (at least those present in the two selected B3 sera) were delineated, we wondered whether these antibodies could be used to give any new insight into the localization of the ligand-binding site in hET B R, which is still a subject of great controversy (Lee et al, 1994;Wada et al, 1995;Boivin et al, 2004;Aubin et al, 2008;Lä ttig et al, 2009). For this purpose, we investigated whether endothelin-1 could compete with these antibodies for receptor binding.…”
Section: Et-1 Competes With Antibodies For Et B Receptor Bindingmentioning
confidence: 98%