Probing the GnRH receptor agonist binding site identifies methylated triptorelin as a new anti-proliferative agent

Kevin Morgan, Samuel P Leighton, Robert P Millar

Research output: Contribution to journalArticlepeer-review

Abstract

D-amino acid substitutions at glycine postion 6 in GnRH-I decapeptide can possess super-agonist activity and enhanced in vivo pharmacokinetics. Agonists elicit growth-inhibition in tumorigenic cells expressing the GnRH receptor above threshold levels. However, new agonists with modified properties are required to improve the anti-proliferative range. Effects of residue substitutions and methylations on tumourigenic HEK293[SCL60] and WPE-1-NB26-3 prostate cells expressing the rat GnRH receptor were compared. Peptides were ranked according to receptor binding affinity, induction of inositol phosphate production and cell growth-inhibition. Analogues possessing D-Trp(6) (including triptorelin), D-Leu(6) (including leuprolide), D-Ala(6), D-Lys(6), or D-Arg(6) exhibited agonist and anti-proliferative activity. Residues His(5) or His(5),Trp(7),Tyr(8), corresponding to residues found in GnRH-II, were tolerated, with retention of sub-nanomolar/low nanomolar binding affinities and EC50s for receptor activation and IC50s for cell growth-inhibition. His(5)D-Arg(6)-GnRH-I exhibited reduced binding affinity and potency, effective in the mid-nanomolar range. However, all GnRH-II-like analogues were less potent than triptorelin. By comparison, three methylated-Trp(6) triptorelin variants showed differential binding, receptor activation and anti-proliferation potency. Significantly, 5-Methyl-DL-Trp(6)-Triptorelin was equipotent to triptorelin. Subsequent studies should determine whether pharmacologically enhanced derivatives of triptorelin can be developed by further alkylations, without substitutions or cleavable cytotoxic adducts, to improve the extent of growth-inhibition of tumour cells expressing the GnRH receptor.
Original languageEnglish
Pages (from-to)86-98
Number of pages13
JournalJournal of molecular biochemistry
Volume1
Issue number2
Publication statusPublished - 16 Jun 2012

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