Literature DB >> 25648263

Host-based Prophylaxis Successfully Targets Liver Stage Malaria Parasites.

Alyse N Douglass1, Heather S Kain1, Marian Abdullahi1, Nadia Arang1, Laura S Austin2, Sebastian A Mikolajczak1, Zachary P Billman3, Jen C C Hume1, Sean C Murphy3, Stefan H I Kappe2, Alexis Kaushansky4.   

Abstract

Eliminating malaria parasites during the asymptomatic but obligate liver stages (LSs) of infection would stop disease and subsequent transmission. Unfortunately, only a single licensed drug that targets all LSs, Primaquine, is available. Targeting host proteins might significantly expand the repertoire of prophylactic drugs against malaria. Here, we demonstrate that both Bcl-2 inhibitors and P53 agonists dramatically reduce LS burden in a mouse malaria model in vitro and in vivo by altering the activity of key hepatocyte factors on which the parasite relies. Bcl-2 inhibitors act primarily by inducing apoptosis in infected hepatocytes, whereas P53 agonists eliminate parasites in an apoptosis-independent fashion. In combination, Bcl-2 inhibitors and P53 agonists act synergistically to delay, and in some cases completely prevent, the onset of blood stage disease. Both families of drugs are highly effective at doses that do not cause substantial hepatocyte cell death in vitro or liver damage in vivo. P53 agonists and Bcl-2 inhibitors were also effective when administered to humanized mice infected with Plasmodium falciparum. Our data demonstrate that host-based prophylaxis could be developed into an effective intervention strategy that eliminates LS parasites before the onset of clinical disease and thus opens a new avenue to prevent malaria.

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Year:  2015        PMID: 25648263      PMCID: PMC4427874          DOI: 10.1038/mt.2015.18

Source DB:  PubMed          Journal:  Mol Ther        ISSN: 1525-0016            Impact factor:   11.454


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Review 5.  Opportunities for Host-targeted Therapies for Malaria.

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Review 7.  Plasmodium's fight for survival: escaping elimination while acquiring nutrients.

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