Please use this identifier to cite or link to this item: https://cris.library.msu.ac.zw//handle/11408/6260
Title: Controlling drug resistance by targeting Plasmodium falciparum heat shock protein 70-1, a chaperone at the centre of protein quality control mechanism: a review
Authors: Douglas A. M. Ruhwaya
Brilliant Nyathi
Gadzikano Munyuki
Ryman Shoko
Grace Mugumbate
Department of Chemistry, Chinhoyi University of Technology, Chinhoyi, Zimbabwe
Department of Chemistry, Chinhoyi University of Technology, Chinhoyi, Zimbabwe
Department of Chemistry, Chinhoyi University of Technology, Chinhoyi, Zimbabwe
Department of Biology, Chinhoyi University of Technology, Chinhoyi, Zimbabwe
Department of Chemical Sciences, Midlands State University, Gweru, Zimbabwe
Keywords: Malaria
P. falciparum
PfHSP70-1
chaperone
protein folding
Issue Date: 21-Apr-2023
Publisher: Taylor and Francis Group
Abstract: The survival of the malaria parasite is highly dependent on withstanding physiological stresses, which are a proportional response to parasite invasion within the hostile human host environment. Plasmodium falciparum heat shock protein 70-1 (PfHSP70-1) plays a significant role through its network of interactions with the substrate scanners PfHSP40s, the functional maturation protein PfHSP90, the nucleotide exchange factor PfHSP110c/PfHSP70-z, apoptosis and parasite homeostasis agent PfHSP60, also the Clp machinery for the unfolding and degrading of misfolded proteins PfHSP100. These proteins work together to maintain the health and function of the parasite, but also possess individual functionalities. Here, we review the functional interplay between these heat shock proteins (HSPs), highlighting the central role of PfHSP70-1, its prospects in antimalarial drug discovery and possible implications in drug resistance.
URI: https://cris.library.msu.ac.zw//handle/11408/6260
Appears in Collections:Research Papers

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