UCT943, a Next-Generation Plasmodium falciparum PI4K Inhibitor Preclinical Candidate for the Treatment of Malaria

被引:0
作者
Brunschwig, Christel [1 ]
Lawrence, Nina [1 ]
Taylor, Dale [1 ]
Abay, Efrem [1 ]
Njoroge, Mathew [1 ]
Basarab, Gregory S. [1 ]
Le Manach, Claire [2 ]
Paquet, Tanya [2 ]
Cabrera, Diego Gonzalez [2 ]
Nchinda, Aloysius T. [2 ]
de Kock, Carmen [1 ]
Wiesner, Lubbe [3 ]
Denti, Paolo [3 ]
Waterson, David [4 ]
Blasco, Benjamin [4 ]
Leroy, Didier [4 ]
Witty, Michael J. [4 ]
Donini, Cristina [4 ]
Duffy, James [4 ]
Wittlin, Sergio [5 ,6 ]
White, Karen L. [7 ]
Charman, Susan A. [7 ]
Belen Jimenez-Diaz, Maria [8 ]
Angulo-Barturen, Inigo [8 ]
Herreros, Esperanza [8 ]
Javier Gamo, Francisco [8 ]
Rochford, Rosemary [9 ]
Mancama, Dalu [10 ]
Coetzer, Theresa L. [11 ,12 ]
van der Watt, Mariette E. [13 ,14 ]
Reader, Janette [13 ,14 ]
Birkholtz, Lyn-Marie [13 ,14 ]
Marsh, Kennan C. [15 ]
Solapure, Suresh M. [16 ]
Burke, John E. [27 ]
McPhail, Jacob A. [27 ]
Vanaerschot, Manu [17 ]
Fidock, David A. [17 ,18 ]
Fish, Paul V. [19 ]
Siegl, Peter [20 ]
Smith, Dennis A.
Wirjanata, Grennady [21 ]
Noviyanti, Rintis [22 ]
Price, Ric N. [21 ,23 ]
Marfurt, Jutta [21 ]
Silue, Kigbafori D. [24 ]
Street, Leslie J. [2 ]
Chibale, Kelly [2 ,25 ,26 ]
机构
[1] Univ Cape Town, Dept Med, Div Clin Pharmacol, Drug Discovery & Dev Ctr H3D, Observatory, South Africa
[2] Univ Cape Town, Dept Chem, Drug Discovery & Dev Ctr H3D, Rondebosch, South Africa
[3] Univ Cape Town, Dept Med, Div Clin Pharmacol, Observatory, South Africa
[4] Med Malaria Venture, Geneva, Switzerland
[5] Swiss Trop & Publ Hlth Inst, Basel, Switzerland
[6] Univ Basel, Basel, Switzerland
[7] Monash Univ, Ctr Drug Candidate Optimisat, Melbourne, Vic, Australia
[8] GlaxoSmithKline, Tres Cantos Med Dev Campus, Madrid, Spain
[9] Univ Colorado, Dept Immunol & Microbiol, Aurora, CO USA
[10] CSIR, Biosci, Pretoria, South Africa
[11] Univ Witwatersrand, Wits Res Inst Malaria, Plasmodium Mol Res Unit, Dept Mol Med & Haematol,Sch Pathol,Fac Hlth Sci, Johannesburg, South Africa
[12] Natl Hlth Lab Serv, Johannesburg, South Africa
[13] Univ Pretoria, Inst Sustainable Malaria Control, Dept Biochem, Pretoria, South Africa
[14] Univ Pretoria, South African Med Res Council, Collaborating Ctr Malaria Res, Pretoria, South Africa
[15] AbbVie, N Chicago, IL USA
[16] Nagarjuna Gardens, Bangalore, Karnataka, India
[17] Columbia Univ, Med Ctr, Dept Microbiol & Immunol, New York, NY USA
[18] Columbia Univ, Med Ctr, Dept Med, Div Infect Dis, New York, NY USA
[19] UCL, Fac Brain Sci, Alzheimers Res UK UCL Drug Discovery Inst, London, England
[20] Siegl Pharma Consulting LLC, Blue Bell, PA USA
[21] Charles Darwin Univ, Menzies Sch Hlth Res, Global & Trop Hlth Div, Darwin, NT, Australia
[22] Eijkman Inst Mol Biol, Jakarta, Indonesia
[23] Univ Oxford, Nuffield Dept Clin Med, Ctr Trop Med & Global Hlth, Oxford, England
[24] Ctr Suisse Rech Sci Cote Ivoire, Abidjan, Cote Ivoire
[25] Univ Cape Town, Inst Infect Dis & Mol Med, Rondebosch, South Africa
[26] Univ Cape Town, Dept Chem, South African Med Res Council, Drug Discovery & Dev Res Unit, Rondebosch, South Africa
[27] Univ Victoria, Dept Biochem & Microbiol, Victoria, BC, Canada
来源
ANTIMICROBIAL AGENTS AND CHEMOTHERAPY | 2018年 / 62卷 / 09期
基金
英国医学研究理事会;
关键词
1-phosphatidylinositol 4-kinase inhibitor; absorption; distribution metabolism; excretion; pharmacokinetic/pharmacodynamic modeling; Plasmodium spp; drug discovery; human dose prediction; in vivo efficacy; malaria; pharmacokinetics; IN-VITRO; ASSAY; MODELS; PHARMACOKINETICS; OPTIMIZATION; PREDICTION; RESISTANCE; MECHANISM; TOXICITY; INVITRO;
D O I
10.1128/AAC.00012-18
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
The 2-aminopyridine MMV048 was the first drug candidate inhibiting Plasmodium phosphatidylinositol 4-kinase (PI4K), a novel drug target for malaria, to enter clinical development. In an effort to identify the next generation of PI4K inhibitors, the series was optimized to improve properties such as solubility and antiplasmodial potency across the parasite life cycle, leading to the 2-aminopyrazine UCT943. The compound displayed higher asexual blood stage, transmission-blocking, and liver stage activities than MMV048 and was more potent against resistant Plasmodium falciparum and Plasmodium vivax clinical isolates. Excellent in vitro antiplasmodial activity translated into high efficacy in Plasmodium berghei and humanized P. falciparum NOD-scid IL-2R gamma(null) mouse models. The high passive permeability and high aqueous solubility of UCT943, combined with low to moderate in vivo intrinsic clearance, resulted in sustained exposure and high bioavailability in preclinical species. In addition, the predicted human dose for a curative single administration using monkey and dog pharmacokinetics was low, ranging from 50 to 80 mg. As a next-generation Plasmodium PI4K inhibitor, UCT943, based on the combined preclinical data, has the potential to form part of a single-exposure radical cure and prophylaxis (SERCaP) to treat, prevent, and block the transmission of malaria.
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