Targeting Host Glycolysis as a Strategy for Antimalarial Development

Andrew J. Jezewski; Yu Hsi Lin; Julie A. Reisz; Rachel Culp-Hill; Yasaman Barekatain; Victoria C. Yan; Angelo D’Alessandro; Florian L. Muller; Audrey R. Odom John

doi:10.3389/fcimb.2021.730413

Targeting Host Glycolysis as a Strategy for Antimalarial Development

Andrew J. Jezewski, Yu Hsi Lin, Julie A. Reisz, Rachel Culp-Hill, Yasaman Barekatain, Victoria C. Yan, Angelo D’Alessandro, Florian L. Muller, Audrey R. Odom John

Cancer Systems Imaging

Research output: Contribution to journal › Article › peer-review

5 Scopus citations

Abstract

Glycolysis controls cellular energy, redox balance, and biosynthesis. Antiglycolytic therapies are under investigation for treatment of obesity, cancer, aging, autoimmunity, and microbial diseases. Interrupting glycolysis is highly valued as a therapeutic strategy, because glycolytic disruption is generally tolerated in mammals. Unfortunately, anemia is a known dose-limiting side effect of these inhibitors and presents a major caveat to development of antiglycolytic therapies. We developed specific inhibitors of enolase – a critical enzyme in glycolysis – and validated their metabolic and cellular effects on human erythrocytes. Enolase inhibition increases erythrocyte susceptibility to oxidative damage and induces rapid and premature erythrocyte senescence, rather than direct hemolysis. We apply our model of red cell toxicity to address questions regarding erythrocyte glycolytic disruption in the context of Plasmodium falciparum malaria pathogenesis. Our study provides a framework for understanding red blood cell homeostasis under normal and disease states and clarifies the importance of erythrocyte reductive capacity in malaria parasite growth.

Original language	English (US)
Article number	730413
Journal	Frontiers in Cellular and Infection Microbiology
Volume	11
DOIs	https://doi.org/10.3389/fcimb.2021.730413
State	Published - Sep 16 2021

Keywords

Plasmodium
antimalarial
enolase
erythrocyte
glycolysis
malaria
oxidative stress
red blood cells

ASJC Scopus subject areas

Microbiology
Immunology
Microbiology (medical)
Infectious Diseases

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10.3389/fcimb.2021.730413

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title = "Targeting Host Glycolysis as a Strategy for Antimalarial Development",

abstract = "Glycolysis controls cellular energy, redox balance, and biosynthesis. Antiglycolytic therapies are under investigation for treatment of obesity, cancer, aging, autoimmunity, and microbial diseases. Interrupting glycolysis is highly valued as a therapeutic strategy, because glycolytic disruption is generally tolerated in mammals. Unfortunately, anemia is a known dose-limiting side effect of these inhibitors and presents a major caveat to development of antiglycolytic therapies. We developed specific inhibitors of enolase – a critical enzyme in glycolysis – and validated their metabolic and cellular effects on human erythrocytes. Enolase inhibition increases erythrocyte susceptibility to oxidative damage and induces rapid and premature erythrocyte senescence, rather than direct hemolysis. We apply our model of red cell toxicity to address questions regarding erythrocyte glycolytic disruption in the context of Plasmodium falciparum malaria pathogenesis. Our study provides a framework for understanding red blood cell homeostasis under normal and disease states and clarifies the importance of erythrocyte reductive capacity in malaria parasite growth.",

keywords = "Plasmodium, antimalarial, enolase, erythrocyte, glycolysis, malaria, oxidative stress, red blood cells",

author = "Jezewski, {Andrew J.} and Lin, {Yu Hsi} and Reisz, {Julie A.} and Rachel Culp-Hill and Yasaman Barekatain and Yan, {Victoria C.} and Angelo D{\textquoteright}Alessandro and Muller, {Florian L.} and {Odom John}, {Audrey R.}",

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AU - Lin, Yu Hsi

AU - Reisz, Julie A.

AU - Culp-Hill, Rachel

AU - Barekatain, Yasaman

AU - Yan, Victoria C.

AU - D’Alessandro, Angelo

AU - Muller, Florian L.

AU - Odom John, Audrey R.

PY - 2021/9/16

Y1 - 2021/9/16

N2 - Glycolysis controls cellular energy, redox balance, and biosynthesis. Antiglycolytic therapies are under investigation for treatment of obesity, cancer, aging, autoimmunity, and microbial diseases. Interrupting glycolysis is highly valued as a therapeutic strategy, because glycolytic disruption is generally tolerated in mammals. Unfortunately, anemia is a known dose-limiting side effect of these inhibitors and presents a major caveat to development of antiglycolytic therapies. We developed specific inhibitors of enolase – a critical enzyme in glycolysis – and validated their metabolic and cellular effects on human erythrocytes. Enolase inhibition increases erythrocyte susceptibility to oxidative damage and induces rapid and premature erythrocyte senescence, rather than direct hemolysis. We apply our model of red cell toxicity to address questions regarding erythrocyte glycolytic disruption in the context of Plasmodium falciparum malaria pathogenesis. Our study provides a framework for understanding red blood cell homeostasis under normal and disease states and clarifies the importance of erythrocyte reductive capacity in malaria parasite growth.

AB - Glycolysis controls cellular energy, redox balance, and biosynthesis. Antiglycolytic therapies are under investigation for treatment of obesity, cancer, aging, autoimmunity, and microbial diseases. Interrupting glycolysis is highly valued as a therapeutic strategy, because glycolytic disruption is generally tolerated in mammals. Unfortunately, anemia is a known dose-limiting side effect of these inhibitors and presents a major caveat to development of antiglycolytic therapies. We developed specific inhibitors of enolase – a critical enzyme in glycolysis – and validated their metabolic and cellular effects on human erythrocytes. Enolase inhibition increases erythrocyte susceptibility to oxidative damage and induces rapid and premature erythrocyte senescence, rather than direct hemolysis. We apply our model of red cell toxicity to address questions regarding erythrocyte glycolytic disruption in the context of Plasmodium falciparum malaria pathogenesis. Our study provides a framework for understanding red blood cell homeostasis under normal and disease states and clarifies the importance of erythrocyte reductive capacity in malaria parasite growth.

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KW - malaria

KW - oxidative stress

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Targeting Host Glycolysis as a Strategy for Antimalarial Development

Abstract

Keywords

ASJC Scopus subject areas

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