Mutations in the P-Type Cation-Transporter ATPase 4, PfATP4, Mediate Resistance to Both Aminopyrazole and Spiroindolone Antimalarials

[Image: see text] Aminopyrazoles are a new class of antimalarial compounds identified in a cellular antiparasitic screen with potent activity against Plasmodium falciparum asexual and sexual stage parasites. To investigate their unknown mechanism of action and thus identify their target, we cultured...

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Autores principales: Flannery, Erika L., McNamara, Case W., Kim, Sang Wan, Kato, Tomoyo Sakata, Li, Fengwu, Teng, Christine H., Gagaring, Kerstin, Manary, Micah J., Barboa, Rachel, Meister, Stephan, Kuhen, Kelli, Vinetz, Joseph M., Chatterjee, Arnab K., Winzeler, Elizabeth A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2014
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4340351/
https://www.ncbi.nlm.nih.gov/pubmed/25322084
http://dx.doi.org/10.1021/cb500616x
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author Flannery, Erika L.
McNamara, Case W.
Kim, Sang Wan
Kato, Tomoyo Sakata
Li, Fengwu
Teng, Christine H.
Gagaring, Kerstin
Manary, Micah J.
Barboa, Rachel
Meister, Stephan
Kuhen, Kelli
Vinetz, Joseph M.
Chatterjee, Arnab K.
Winzeler, Elizabeth A.
author_facet Flannery, Erika L.
McNamara, Case W.
Kim, Sang Wan
Kato, Tomoyo Sakata
Li, Fengwu
Teng, Christine H.
Gagaring, Kerstin
Manary, Micah J.
Barboa, Rachel
Meister, Stephan
Kuhen, Kelli
Vinetz, Joseph M.
Chatterjee, Arnab K.
Winzeler, Elizabeth A.
author_sort Flannery, Erika L.
collection PubMed
description [Image: see text] Aminopyrazoles are a new class of antimalarial compounds identified in a cellular antiparasitic screen with potent activity against Plasmodium falciparum asexual and sexual stage parasites. To investigate their unknown mechanism of action and thus identify their target, we cultured parasites in the presence of a representative member of the aminopyrazole series, GNF-Pf4492, to select for resistance. Whole genome sequencing of three resistant lines showed that each had acquired independent mutations in a P-type cation-transporter ATPase, PfATP4 (PF3D7_1211900), a protein implicated as the novel Plasmodium spp. target of another, structurally unrelated, class of antimalarials called the spiroindolones and characterized as an important sodium transporter of the cell. Similarly to the spiroindolones, GNF-Pf4492 blocks parasite transmission to mosquitoes and disrupts intracellular sodium homeostasis. Our data demonstrate that PfATP4 plays a critical role in cellular processes, can be inhibited by two distinct antimalarial pharmacophores, and supports the recent observations that PfATP4 is a critical antimalarial target.
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spelling pubmed-43403512015-10-16 Mutations in the P-Type Cation-Transporter ATPase 4, PfATP4, Mediate Resistance to Both Aminopyrazole and Spiroindolone Antimalarials Flannery, Erika L. McNamara, Case W. Kim, Sang Wan Kato, Tomoyo Sakata Li, Fengwu Teng, Christine H. Gagaring, Kerstin Manary, Micah J. Barboa, Rachel Meister, Stephan Kuhen, Kelli Vinetz, Joseph M. Chatterjee, Arnab K. Winzeler, Elizabeth A. ACS Chem Biol [Image: see text] Aminopyrazoles are a new class of antimalarial compounds identified in a cellular antiparasitic screen with potent activity against Plasmodium falciparum asexual and sexual stage parasites. To investigate their unknown mechanism of action and thus identify their target, we cultured parasites in the presence of a representative member of the aminopyrazole series, GNF-Pf4492, to select for resistance. Whole genome sequencing of three resistant lines showed that each had acquired independent mutations in a P-type cation-transporter ATPase, PfATP4 (PF3D7_1211900), a protein implicated as the novel Plasmodium spp. target of another, structurally unrelated, class of antimalarials called the spiroindolones and characterized as an important sodium transporter of the cell. Similarly to the spiroindolones, GNF-Pf4492 blocks parasite transmission to mosquitoes and disrupts intracellular sodium homeostasis. Our data demonstrate that PfATP4 plays a critical role in cellular processes, can be inhibited by two distinct antimalarial pharmacophores, and supports the recent observations that PfATP4 is a critical antimalarial target. American Chemical Society 2014-10-16 2015-02-20 /pmc/articles/PMC4340351/ /pubmed/25322084 http://dx.doi.org/10.1021/cb500616x Text en Copyright © 2014 American Chemical Society This is an open access article published under an ACS AuthorChoice License (http://pubs.acs.org/page/policy/authorchoice_termsofuse.html) , which permits copying and redistribution of the article or any adaptations for non-commercial purposes.
spellingShingle Flannery, Erika L.
McNamara, Case W.
Kim, Sang Wan
Kato, Tomoyo Sakata
Li, Fengwu
Teng, Christine H.
Gagaring, Kerstin
Manary, Micah J.
Barboa, Rachel
Meister, Stephan
Kuhen, Kelli
Vinetz, Joseph M.
Chatterjee, Arnab K.
Winzeler, Elizabeth A.
Mutations in the P-Type Cation-Transporter ATPase 4, PfATP4, Mediate Resistance to Both Aminopyrazole and Spiroindolone Antimalarials
title Mutations in the P-Type Cation-Transporter ATPase 4, PfATP4, Mediate Resistance to Both Aminopyrazole and Spiroindolone Antimalarials
title_full Mutations in the P-Type Cation-Transporter ATPase 4, PfATP4, Mediate Resistance to Both Aminopyrazole and Spiroindolone Antimalarials
title_fullStr Mutations in the P-Type Cation-Transporter ATPase 4, PfATP4, Mediate Resistance to Both Aminopyrazole and Spiroindolone Antimalarials
title_full_unstemmed Mutations in the P-Type Cation-Transporter ATPase 4, PfATP4, Mediate Resistance to Both Aminopyrazole and Spiroindolone Antimalarials
title_short Mutations in the P-Type Cation-Transporter ATPase 4, PfATP4, Mediate Resistance to Both Aminopyrazole and Spiroindolone Antimalarials
title_sort mutations in the p-type cation-transporter atpase 4, pfatp4, mediate resistance to both aminopyrazole and spiroindolone antimalarials
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4340351/
https://www.ncbi.nlm.nih.gov/pubmed/25322084
http://dx.doi.org/10.1021/cb500616x
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