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Literature DB >> 28927276

Alkoxycarbonate Ester Prodrugs of Preclinical Drug Candidate ELQ-300 for Prophylaxis and Treatment of Malaria.

Lisa Frueh^1,2, Yuexin Li¹, Michael W Mather³, Qigui Li⁴, Sovitj Pou², Aaron Nilsen¹, Rolf W Winter¹, Isaac P Forquer¹, April M Pershing³, Lisa H Xie⁴, Martin J Smilkstein¹, Diana Caridha⁴, Dennis R Koop⁵, Robert F Campbell⁴, Richard J Sciotti⁴, Mara Kreishman-Deitrick⁴, Jane X Kelly¹, Brian Vesely⁴, Akhil B Vaidya³, Michael K Riscoe¹.

Abstract

ELQ-300 is a preclinical antimalarial drug candidate that is active against liver, blood, and transmission stages of Plasmodium falciparum. While ELQ-300 is highly effective when administered in a low multidose regimen, poor aqueous solubility and high crystallinity have hindered its clinical development. To overcome its challenging physiochemical properties, a number of bioreversible alkoxycarbonate ester prodrugs of ELQ-300 were synthesized. These bioreversible prodrugs are converted to ELQ-300 by host and parasite esterase action in the liver and bloodstream of the host. One such alkoxycarbonate prodrug, ELQ-331, is curative against Plasmodium yoelii with a single low dose of 3 mg/kg in a murine model of patent malaria infection. ELQ-331 is at least as fully protective as ELQ-300 in a murine malaria prophylaxis model when delivered 24 h before sporozoite inoculation at an oral dose of 1 mg/kg. Here, we show that ELQ-331 is a promising prodrug of ELQ-300 with improved physiochemical and metabolic properties and excellent potential for clinical formulation.

Entities: CellLine Chemical Disease Gene Species

Keywords: Plasmodium falciparum; cytochrome bc1; malaria; prodrug

Mesh：

Substances：

Year: 2017 PMID： 28927276 PMCID： PMC5947850 DOI： 10.1021/acsinfecdis.7b00062

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

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