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Lead optimization of phthalazinone phosphodiesterase inhibitors as novel antitrypanosomal compounds

Tijdschriftbijdrage - Tijdschriftartikel

Human African trypanosomiasis is causing thousands of deaths every year in the rural areas of Africa. In this manuscript we describe the optimization of a family of phtalazinone derivatives. Phosphodiesterases have emerged as attractive molecular targets for a novel treatment for a variety of neglected parasitic diseases. Compound 1 resulted in being a potent TbrPDEB1 inhibitor with interesting activity against T. brucei in a phenotypic screen. Derivative 1 was studied in an acute in vivo mouse disease model but unfortunately showed no efficacy due to low metabolic stability. We report structural modifications to achieve compounds with an improved metabolic stability while maintaining high potency against TbrPDEB1 and T. brucei. Compound 14 presented a good microsomal stability in mouse and human microsomes and provides a good starting point for future efforts.

Tijdschrift: Journal of medicinal chemistry

ISSN: 0022-2623

Volume: 63

Pagina's: 3485 - 3507

Jaar van publicatie:2020

Trefwoorden:A1 Journal article

WoS Id: 000526405300007
DOI: https://doi.org/10.1021/acs.jmedchem.9b00985
Handle: https://hdl.handle.net/10067/1685520151162165141

BOF-keylabel:ja

BOF-publication weight:6

CSS-citation score:1

Auteurs:International

Authors from:Higher Education

Toegankelijkheid:Closed

Zie ook: Lead Optimization of Phthalazinone Phosphodiesterase Inhibitors as Novel Antitrypanosomal Compounds

Publicatie

Lead optimization of phthalazinone phosphodiesterase inhibitors as novel antitrypanosomal compounds

Tijdschriftbijdrage - Tijdschriftartikel

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