Glucose 6-phosphate dehydrogenase 6-phosphogluconolactonase: characterization of the Plasmodium vivax enzyme and inhibitor studies.

Kristina HaeusslerIsabell BerneburgEsther JortzikJulia HahnMahsa RahbariNorma SchulzJanina PreussViktor A Zapol'skiiLars BodeAnthony B PinkertonDieter E KaufmannStefan RahlfsKatja Becker

Published in: Malaria journal (2019)

The characterization of PvG6PD makes this enzyme accessible to further drug discovery activities. In contrast to naturally occurring G6PD variants in the human host that can alter the kinetic properties of the enzyme and thus the redox homeostasis of the cells, the naturally occurring PfGluPho variants studied here are unlikely to have a major impact on the parasites' redox homeostasis. Several classes of inhibitors have been successfully tested and are presently being followed up.

Keyphrases

drug discovery
copy number
induced apoptosis
endothelial cells
magnetic resonance
cell cycle arrest
oxidative stress
blood glucose
blood pressure
gene expression
adipose tissue
metabolic syndrome
signaling pathway
pluripotent stem cells
cell proliferation
case control
insulin resistance
solid state