Author:
Untaroiu Ana M.,Carey Maureen A.,Guler Jennifer L.,Papin Jason A.
Abstract
AbstractMalaria is a major global health problem, with the Plasmodium falciparum protozoan parasite causing the most severe form of the disease. Prevalence of drug-resistant P. falciparum highlights the need to understand the biology of resistance and to identify novel combination therapies that are effective against resistant parasites. Resistance has compromised the therapeutic use of many antimalarial drugs, including chloroquine, and limited our ability to treat malaria across the world. Fortunately, chloroquine resistance comes at a fitness cost to the parasite; this can be leveraged in developing combination therapies or to reinstate use of chloroquine. To understand biological changes induced by chloroquine treatment, we compared transcriptomics data from chloroquine-resistant parasites in the presence or absence of the drug. Using both linear models and a genome-scale metabolic network reconstruction of the parasite to interpret the expression data, we identified targetable pathways in resistant parasites. This study identified an increased importance of lipid synthesis, glutathione production/cycling, isoprenoids biosynthesis, and folate metabolism in response to chloroquine. We identified potential drug targets for chloroquine combination therapies. Significantly, our analysis suggests that the combination of chloroquine and sulfadoxine-pyrimethamine or fosmidomycin may be more effective against chloroquine-resistant parasites than either drug alone; further studies will explore the use of these drugs as chloroquine resistance blockers. Additional metabolic weaknesses were found in glutathione generation and lipid synthesis during chloroquine treatment. These processes could be targeted with novel inhibitors to reduce parasite growth and reduce the burden of malaria infections. Thus, we identified metabolic weaknesses of chloroquine-resistant parasites and propose targeted chloroquine combination therapies.
Publisher
Cold Spring Harbor Laboratory
Reference66 articles.
1. WHO | World Malaria Report 2015 [Internet]. WHO. [cited 2017 Apr 12]. Available from: http://www.who.int/malaria/publications/world-malaria-report-2015/report/en/
2. Russell PK , Howson CP . Vaccines Against Malaria: Hope in a Gathering Storm [Internet]. National Academies Press (US); 1996 [cited 2017 Apr 18]. Available from: https://www.ncbi.nlm.nih.gov/books/NBK231030/
3. Emerging drug resistance in Plasmodium falciparum: A review of well-characterized drug targets for novel antimalarial chemotherapy;Asian Pac J Trop Dis,2016
4. Malaria: Biology and Disease
5. Spread of chloroquine resistance in Plasmodium falciparum;Parasitol Today Pers Ed,1987