| Literature DB >> 9341910 |
I Mezö1, S Lovas, I Pályi, B Vincze, A Kálnay, G Turi, Z Vadász, J Seprödi, M Idei, G Tóth, E Gulyás, F Otvös, M Mák, J E Horváth, I Teplán, R F Murphy.
Abstract
Following the observation that the activity of gonadotropin-releasing hormone III (GnRH-III) in the suppression of growth of MDA-MB-231 and MCF-7 breast cancer cells surpasses that of GnRH and other analogs thereof, analogs of GnRH-III were synthesized to investigate the structural basis for the improved antitumor activity. Compounds synthesized include analogs with changes in the central sequence in which GnRH-III differs from GnRH and in the C- and N-terminal regions. The results indicate that a salt bridge between Asp6 and Lys8 stabilizes the active conformation of GnRH-III and show the importance of the Trp7. Replacement of the C-terminal Gly-NH2 with D-Ala-NH2 was not well tolerated, but replacement with ethylamide was. Replacement of pGlu1 with Ac-D-Trp appears to have a significantly deleterious effect on a unique conformation of GnRH-III which is responsible for its binding to the receptors on cancer cell lines and the resultant antitumor activity.Entities:
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Year: 1997 PMID: 9341910 DOI: 10.1021/jm9700981
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446