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A triazolopyrimidine-based dihydroorotate dehydrogenase inhibitor (DSM421) with improved drug-like properties for treatment and prevention of malaria

Abstract:
The emergence of drug resistant malaria parasites continues to hamper efforts to control this lethal disease. Dihydroorotate dehydrogenase has recently been validated as a new target for the treatment of malaria and a selective inhibitor (DSM265) of the Plasmodium enzyme is currently in clinical development. With the goal of identifying a backup compound to DSM265, we explored replacement of the SF5-aniline moiety of DSM265 with a series of CF3-pyridinyls, while maintaining the core triazolopyrimidine scaffold. This effort led to the identification of DSM421, which has improved solubility, lower intrinsic clearance and increased plasma exposure after oral dosing compared to DSM265, while maintaining a long predicted human half-life. Its improved physical and chemical properties will allow it to be formulated more readily than DSM265. DSM421 showed excellent efficacy in the SCID mouse model of P. falciparum malaria that supports the prediction of a low human dose (<200 mg). Importantly DSM421 showed equal activity against both P. falciparum and P. vivax field isolates, while DSM265 was more active on P. falciparum. DSM421 has the potential to be developed as a single dose cure or once-weekly chemopreventative for both P. falciparum and P. vivax malaria leading to its advancement as a preclinical development candidate.
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.1021/acsinfecdis.6b00144

Authors



Publisher:
American Chemical Society
Journal:
ACS infectious diseases More from this journal
Volume:
2
Issue:
12
Pages:
945–957
Publication date:
2016-09-17
Acceptance date:
2016-09-17
DOI:
ISSN:
2373-8227
Pmid:
27641613


Language:
English
Keywords:
Pubs id:
pubs:648069
UUID:
uuid:4305dc5a-dee4-45ac-af84-37a1d07a1d4d
Local pid:
pubs:648069
Source identifiers:
648069
Deposit date:
2016-10-11

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