Literature DB >> 27641613

A Triazolopyrimidine-Based Dihydroorotate Dehydrogenase Inhibitor with Improved Drug-like Properties for Treatment and Prevention of Malaria.

Margaret A Phillips, Karen L White1, Sreekanth Kokkonda2, Xiaoyi Deng, John White2, Farah El Mazouni, Kennan Marsh3, Diana R Tomchick, Krishne Manjalanagara4, Kakali Rani Rudra4, Grennady Wirjanata5, Rintis Noviyanti6, Ric N Price5,7, Jutta Marfurt5, David M Shackleford1, Francis C K Chiu1, Michael Campbell1, Maria Belen Jimenez-Diaz8, Santiago Ferrer Bazaga8, Iñigo Angulo-Barturen8, Maria Santos Martinez8, Maria Lafuente-Monasterio8, Werner Kaminsky2, Kigbafori Silue9, Anne-Marie Zeeman10, Clemens Kocken10, Didier Leroy11, Benjamin Blasco11, Emilie Rossignol11, Thomas Rueckle11, Dave Matthews11, Jeremy N Burrows11, David Waterson11, Michael J Palmer11, Pradipsinh K Rathod2, Susan A Charman1.   

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.

Entities:  

Keywords:  Plasmodium; dihydroorotate dehydrogenase; malaria; pyrimidine biosynthesis

Mesh:

Substances:

Year:  2016        PMID: 27641613      PMCID: PMC5148661          DOI: 10.1021/acsinfecdis.6b00144

Source DB:  PubMed          Journal:  ACS Infect Dis        ISSN: 2373-8227            Impact factor:   5.084


  42 in total

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