Abstract
Cyclotides are useful scaffolds to stabilize bioactive peptides. Four melanocortin analogues of kalata B1 were synthesized. One is a selective MC4R agonist. The analogues retain the native kalata B1 scaffold and introduce a designed pharmacological activity, validating cyclotides as protein engineering scaffolds. A novel type of melanocortin agonist has been developed, with potential as a drug lead for treating obesity. Obesity is an increasingly important global health problem that lacks current treatment options. The melanocortin receptor 4 (MC4R) is a target for obesity therapies because its activation triggers appetite suppression and increases energy expenditure. Cyclotides have been suggested as scaffolds for the insertion and stabilization of pharmaceutically active peptides. In this study, we explored the development of appetite-reducing peptides by synthesizing MC4R agonists based on the insertion of the His-Phe-Arg-Trp sequence into the cyclotide kalata B1. The ability of the analogues to fold similarly to kalata B1 but display MC4R activity were investigated. Four peptides were synthesized using t-butoxycarbonyl peptide chemistry with a C-terminal thioester to facilitate backbone cyclization. The structures of the peptides were found to be similar to kalata B1, evaluated by Hα NMR chemical shifts. KB1(GHFRWG;23-28) had a K(i) of 29 nm at the MC4R and was 107 or 314 times more selective over this receptor than MC1R or MC5R, respectively, and had no detectable binding to MC3R. The peptide had higher affinity for the MC4R than the endogenous agonist, α-melanocyte stimulation hormone, but it was less potent at the MC4R, with an EC(50) of 580 nm for activation of the MC4R. In conclusion, we synthesized melanocortin analogues of kalata B1 that preserve the structural scaffold and display receptor binding and functional activity. KB1(GHFRWG;23-28) is potent and selective for the MC4R. This compound validates the use of cyclotides as scaffolds and has the potential to be a new lead for the treatment of obesity.
Highlights
Cyclotides are useful scaffolds to stabilize bioactive peptides
We explored the development of appetite-reducing peptides by synthesizing MC4R agonists based on the insertion of the His-Phe-Arg-Trp sequence into the cyclotide kalata B1
melanocortin receptors (MCR) tested, highlighting the potential of the cyclic cystine-knotted (CCK) scaffold for targeting specific interactions implicated in the regulation of appetite and energy homeostasis and providing a possible lead molecule for the treatment of obesity
Summary
Cyclotides are useful scaffolds to stabilize bioactive peptides. Results: Four melanocortin analogues of kalata B1 were synthesized. We explored the development of appetite-reducing peptides by synthesizing MC4R agonists based on the insertion of the His-Phe-Arg-Trp sequence into the cyclotide kalata B1. A truncated analogue of the inverse agonist agouti-related protein was turned into a full agonist by exchanging the binding sequence with His-D-Phe-ArgTrp [22] These findings suggest that it might be possible to graft the His-Phe-Arg-Trp sequence and related modified sequences into stable peptide frameworks to develop novel MCR agonists. These analogues have the potential to become leads for a new class of melanocortin receptor agonists for the treatment of obesity. They will expand knowledge on the applicability of cyclotides as scaffolds
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