TY - JOUR
T1 - Assessing drug efficacy against Plasmodium falciparum liver stages in vivo
AU - Flannery, Erika L.
AU - Foquet, Lander
AU - Chuenchob, Vorada
AU - Fishbaugher, Matthew
AU - Billman, Zachary
AU - Navarro, Mary Jane
AU - Betz, William
AU - Olsen, Tayla M.
AU - Lee, Joshua
AU - Camargo, Nelly
AU - Nguyen, Thao
AU - Schafer, Carola
AU - Sack, Brandon K.
AU - Wilson, Elizabeth M.
AU - Saunders, Jessica
AU - Bial, John
AU - Campo, Brice
AU - Charman, Susan A.
AU - Murphy, Sean C.
AU - Phillips, Margaret A.
AU - Kappe, Stefan Hi
AU - Mikolajczak, Sebastian A.
PY - 2018/1/11
Y1 - 2018/1/11
N2 - Malaria eradication necessitates new tools to fight the evolving and complex Plasmodium pathogens. These tools include prophylactic drugs that eliminate Plasmodium liver stages and consequently prevent clinical disease, decrease transmission, and reduce the propensity for resistance development. Currently, the identification of these drugs relies on in vitro P. falciparum liver stage assays or in vivo causal prophylaxis assays using rodent malaria parasites; there is no method to directly test in vivo liver stage activity of candidate antimalarials against the human malaria-causing parasite P. falciparum. Here, we use a liver-chimeric humanized mouse (FRG huHep) to demonstrate in vivo P. falciparum liver stage development and describe the efficacy of clinically used and candidate antimalarials with prophylactic activity. We show that daily administration of atovaquone-proguanil (ATQ-PG; ATQ, 30 mg/kg, and PG, 10 mg/kg) protects 5 of 5 mice from liver stage infection, consistent with the use in humans as a causal prophylactic drug. Single-dose primaquine (60 mg/kg) has similar activity to that observed in humans, demonstrating the activity of this drug (and its active metabolites) in FRG huHep mice. We also show that DSM265, a selective Plasmodial dihydroorotate dehydrogenase inhibitor with causal prophylactic activity in humans, reduces liver stage burden in FRG huHep mice. Finally, we measured liver stage-to-blood stage transition of the parasite, the ultimate readout of prophylactic activity and measurement of infective capacity of parasites in the liver, to show that ATQ-PG reduces blood stage patency to below the limit of quantitation by quantitative PCR (qPCR). The FRG huHep model, thus, provides a platform for preclinical evaluation of drug candidates for liver stage causal prophylactic activity, pharmacokinetic/pharmacodynamics studies, and biological studies to investigate the mechanism of action of liver stage active antimalarials.
AB - Malaria eradication necessitates new tools to fight the evolving and complex Plasmodium pathogens. These tools include prophylactic drugs that eliminate Plasmodium liver stages and consequently prevent clinical disease, decrease transmission, and reduce the propensity for resistance development. Currently, the identification of these drugs relies on in vitro P. falciparum liver stage assays or in vivo causal prophylaxis assays using rodent malaria parasites; there is no method to directly test in vivo liver stage activity of candidate antimalarials against the human malaria-causing parasite P. falciparum. Here, we use a liver-chimeric humanized mouse (FRG huHep) to demonstrate in vivo P. falciparum liver stage development and describe the efficacy of clinically used and candidate antimalarials with prophylactic activity. We show that daily administration of atovaquone-proguanil (ATQ-PG; ATQ, 30 mg/kg, and PG, 10 mg/kg) protects 5 of 5 mice from liver stage infection, consistent with the use in humans as a causal prophylactic drug. Single-dose primaquine (60 mg/kg) has similar activity to that observed in humans, demonstrating the activity of this drug (and its active metabolites) in FRG huHep mice. We also show that DSM265, a selective Plasmodial dihydroorotate dehydrogenase inhibitor with causal prophylactic activity in humans, reduces liver stage burden in FRG huHep mice. Finally, we measured liver stage-to-blood stage transition of the parasite, the ultimate readout of prophylactic activity and measurement of infective capacity of parasites in the liver, to show that ATQ-PG reduces blood stage patency to below the limit of quantitation by quantitative PCR (qPCR). The FRG huHep model, thus, provides a platform for preclinical evaluation of drug candidates for liver stage causal prophylactic activity, pharmacokinetic/pharmacodynamics studies, and biological studies to investigate the mechanism of action of liver stage active antimalarials.
KW - Drug screens
KW - Infectious disease
KW - Malaria
KW - Microbiology
KW - Mouse models
UR - http://www.scopus.com/inward/record.url?scp=85044230116&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=85044230116&partnerID=8YFLogxK
U2 - 10.1172/jci.insight.92587
DO - 10.1172/jci.insight.92587
M3 - Article
C2 - 29321371
AN - SCOPUS:85044230116
SN - 2379-3708
VL - 3
JO - JCI Insight
JF - JCI Insight
IS - 1
ER -