Mapping the malaria parasite druggable genome by using in vitro evolution and chemogenomics
- Cowell, Annie N.
- Istvan, Eva S.
- Lukens, Amanda K.
- Gomez-Lorenzo, Maria G.
- Vanaerschot, Manu
- Sakata-Kato, Tomoyo
- Flannery, Erika L.
- Magistrado, Pamela
- Owen, Edward
- Abraham, Matthew
- LaMonte, Gregory
- Painter, Heather J.
- Williams, Roy M.
- Franco, Virginia
- Linares, Maria
- Arriaga, Ignacio
- Bopp, Selina
- Corey, Victoria C.
- Gnädig, Nina F.
- Coburn-Flynn, Olivia
- Reimer, Christin
- Gupta, Purva
- Murithi, James M.
- Moura, Pedro A.
- Fuchs, Olivia
- Sasaki, Erika
- Kim, Sang W.
- Teng, Christine H.
- Wang, Lawrence T.
- Akidil, Aslı
- Adjalley, Sophie
- Willis, Paul A.
- Siegel, Dionicio
- Tanaseichuk, Olga
- Zhong, Yang
- Zhou, Yingyao
- Llinás, Manuel
- Ottilie, Sabine
- Gamo, Francisco-Javier
- Lee, Marcus C. S.
- Goldberg, Daniel E.
- Fidock, David A.
- Wirth, Dyann F.
- Winzeler, Elizabeth A.
DOIAbstract
Chemogenetic characterization through in vitro evolution combined with whole-genome analysis can identify antimalarial drug targets and drug-resistance genes. We performed a genome analysis of 262 Plasmodium falciparum parasites resistant to 37 diverse compounds. We found 159 gene amplifications and 148 nonsynonymous changes in 83 genes associated with drug-resistance acquisition, where gene amplifications contributed to one-third of resistance acquisition events. Beyond confirming previously identified multidrug-resistance mechanisms, we discovered hitherto unrecognized drug target–inhibitor pairs, including thymidylate synthase and a benzoquinazolinone, farnesyltransferase and a pyrimidinedione, and a dipeptidylpeptidase and an arylurea. ...
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