MK-5204: An orally active β-1,3-glucan synthesis inhibitor

James M Apgar; Robert R Wilkening; Dann L Parker Jr; Dongfang Meng; Kenneth J Wildonger; Donald Sperbeck; Mark L Greenlee; James M Balkovec; Amy M Flattery; George K Abruzzo; Andrew M Galgoci; Robert A Giacobbe; Charles J Gill; Ming-Jo Hsu; Paul Liberator; Andrew S Misura; Mary Motyl; Jennifer Nielsen Kahn; Maryann Powles; Fred Racine; Jasminka Dragovic; Weiming Fan; Robin Kirwan; Shu Lee; Hao Liu; Ahmed Mamai; Kingsley Nelson; Michael Peel

doi:10.1016/j.bmcl.2020.127357

MK-5204: An orally active β-1,3-glucan synthesis inhibitor

Bioorg Med Chem Lett. 2020 Sep 1;30(17):127357. doi: 10.1016/j.bmcl.2020.127357. Epub 2020 Jun 19.

Authors

James M Apgar¹, Robert R Wilkening², Dann L Parker Jr², Dongfang Meng², Kenneth J Wildonger², Donald Sperbeck², Mark L Greenlee², James M Balkovec², Amy M Flattery², George K Abruzzo², Andrew M Galgoci², Robert A Giacobbe², Charles J Gill², Ming-Jo Hsu², Paul Liberator², Andrew S Misura², Mary Motyl², Jennifer Nielsen Kahn², Maryann Powles², Fred Racine², Jasminka Dragovic², Weiming Fan³, Robin Kirwan³, Shu Lee³, Hao Liu³, Ahmed Mamai³, Kingsley Nelson³, Michael Peel³

Affiliations

¹ Merck & Co. Inc., 2000 Galloping Hill Road, Kenilworth, NJ 07033, USA. Electronic address: james_apgar@merck.com.
² Merck & Co. Inc., 2000 Galloping Hill Road, Kenilworth, NJ 07033, USA.
³ Scynexis Inc., 1 Evertrust Plaza, Jersey City, NJ 07302, USA.

PMID: 32738971
DOI: 10.1016/j.bmcl.2020.127357

Abstract

Our previously reported efforts to produce an orally active β-1,3-glucan synthesis inhibitor through the semi-synthetic modification of enfumafungin focused on replacing the C2 acetoxy moiety with an aminotetrazole and the C3 glycoside with a N,N-dimethylaminoether moiety. This work details further optimization of the C2 heterocyclic substituent, which identified 3-carboxamide-1,2,4-triazole as a replacement for the aminotetrazole with comparable antifungal activity. Alkylation of either the carboxamidetriazole at C2 or the aminoether at C3 failed to significantly improve oral efficacy. However, replacement of the isopropyl alpha amino substituent with a t-butyl, improved oral exposure while maintaining antifungal activity. These two structural modifications produced MK-5204, which demonstrated broad spectrum activity against Candida species and robust oral efficacy in a murine model of disseminated Candidiasis without the N-dealkylation liability observed for the previous lead.

Keywords: Antifungal; Candidiasis; Enfumafungin; MK-5204; β-1,3-Glucan synthesis inhibitor.

MeSH terms

Administration, Oral
Animals
Antifungal Agents / chemistry*
Antifungal Agents / metabolism
Antifungal Agents / pharmacology
Antifungal Agents / therapeutic use
Candida / drug effects
Candidiasis / drug therapy
Disease Models, Animal
Glucosyltransferases / antagonists & inhibitors
Glucosyltransferases / metabolism
Glycosides / chemistry
Half-Life
Mice
Microbial Sensitivity Tests
Stereoisomerism
Structure-Activity Relationship
Triazoles / chemistry*
Triazoles / metabolism
Triazoles / pharmacology
Triazoles / therapeutic use
Triterpenes / chemistry
beta-Glucans / chemistry
beta-Glucans / metabolism*

Substances

Antifungal Agents
Glycosides
Triazoles
Triterpenes
beta-Glucans
enfumafungin
1,2,4-triazole
beta-1,3-glucan
Glucosyltransferases

Supplementary concepts

Systemic candidiasis