Malaria remains a serious global health challenge, yet treatment and control programs are threatened by drug resistance. Dihydroorotate dehydrogenase (DHODH) was clinically validated as a target for treatment and prevention of malaria through human studies with DSM265, but currently no drugs against this target are in clinical use. We used structure-based computational tools including free energy perturbation (FEP+) to discover highly ligand efficient, potent, and selective pyrazole-based Plasmodium DHODH inhibitors through a scaffold hop from a pyrrole-based series. Optimized pyrazole-based compounds were identified with low nM-to-pM Plasmodium falciparum cell potency and oral activity in a humanized SCID mouse malaria infection model. The lead compound DSM1465 is more potent and has improved absorption, distribution, metabolism and excretion/pharmacokinetic (ADME/PK) properties compared to DSM265 that support the potential for once-monthly chemoprevention at a low dose. This compound meets the objective of identifying compounds with potential to be used for monthly chemoprevention in Africa to support malaria elimination efforts.
Structure-Based Discovery and Development of Highly Potent Dihydroorotate Dehydrogenase Inhibitors for Malaria Chemoprevention.
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作者:Nie Zhe, Bonnert Roger, Tsien Jet, Deng Xiaoyi, Higgs Christopher, El Mazouni Farah, Zhang Xiaoyu, Li Renzhe, Ho Nhi, Feher Victoria, Paulsen Janet, Shackleford David M, Katneni Kasiram, Chen Gong, Ng Alice C F, McInerney Mitchell, Wang Wen, Saunders Jessica, Collins Daniel, Yan Dandan, Li Peng, Campbell Michael, Patil Rahul, Ghoshal Atanu, Mondal Pallab, Kundu Abhijit, Chittimalla Rajesh, Mahadeva Muralikumar, Kokkonda Sreekanth, White John, Das Rishi, Mukherjee Partha, Angulo-Barturen Iñigo, Jiménez-DÃaz MarÃa Belén, Malmstrom Robert, Lawrenz Morgan, Rodriguez-Granillo Agustina, Rathod Pradipsinh K, Tomchick Diana R, Palmer Michael J, Laleu Benoît, Qin Tian, Charman Susan A, Phillips Margaret A
| 期刊: | Journal of Medicinal Chemistry | 影响因子: | 6.800 |
| 时间: | 2025 | 起止号: | 2025 Jan 9; 68(1):590-637 |
| doi: | 10.1021/acs.jmedchem.4c02394 | ||
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