Apicoplast-Resident Processes: Exploiting the Chink in the Armour of Plasmodium falciparum Parasites

Author:

Mamudu Collins Ojonugwa12ORCID,Tebamifor Mercy Eyitomi12,Sule Mary Ohunene3,Dokunmu Titilope Modupe12,Ogunlana Olubanke Olujoke124ORCID,Iheagwam Franklyn Nonso14ORCID

Affiliation:

1. Department of Biochemistry, Covenant University, Ota, Nigeria

2. Covenant Applied Informatics and Communication Africa Centre of Excellence, Ota, Nigeria

3. Confluence University of Science and Technology, Osara, Kogi, Nigeria

4. Covenant University Public Health and Wellbeing Research Cluster, Covenant University, Ota, Nigeria

Abstract

The discovery of a relict plastid, also known as an apicoplast (apicomplexan plastid), that houses housekeeping processes and metabolic pathways critical to Plasmodium parasites’ survival has prompted increased research on identifying potent inhibitors that can impinge on apicoplast-localised processes. The apicoplast is absent in humans, yet it is proposed to originate from the eukaryote’s secondary endosymbiosis of a primary symbiont. This symbiotic relationship provides a favourable microenvironment for metabolic processes such as haem biosynthesis, Fe-S cluster synthesis, isoprenoid biosynthesis, fatty acid synthesis, and housekeeping processes such as DNA replication, transcription, and translation, distinct from analogous mammalian processes. Recent advancements in comprehending the biology of the apicoplast reveal it as a vulnerable organelle for malaria parasites, offering numerous potential targets for effective antimalarial therapies. We provide an overview of the metabolic processes occurring in the apicoplast and discuss the organelle as a viable antimalarial target in light of current advances in drug discovery. We further highlighted the relevance of these metabolic processes to Plasmodium falciparum during the different stages of the lifecycle.

Funder

Covenant University Centre for Research, Innovation and Discovery

Publisher

Hindawi Limited

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