Literature DB >> 35257658

Critical role for isoprenoids in apicoplast biogenesis by malaria parasites.

Megan Okada1, Krithika Rajaram2, Russell P Swift2, Amanda Mixon1, John Alan Maschek3, Sean T Prigge2, Paul A Sigala1.   

Abstract

Isopentenyl pyrophosphate (IPP) is an essential metabolic output of the apicoplast organelle in Plasmodium falciparum malaria parasites and is required for prenylation-dependent vesicular trafficking and other cellular processes. We have elucidated a critical and previously uncharacterized role for IPP in apicoplast biogenesis. Inhibiting IPP synthesis blocks apicoplast elongation and inheritance by daughter merozoites, and apicoplast biogenesis is rescued by exogenous IPP and polyprenols. Knockout of the only known isoprenoid-dependent apicoplast pathway, tRNA prenylation by MiaA, has no effect on blood-stage parasites and thus cannot explain apicoplast reliance on IPP. However, we have localized an annotated polyprenyl synthase (PPS) to the apicoplast. PPS knockdown is lethal to parasites, rescued by IPP and long- (C50) but not short-chain (≤C20) prenyl alcohols, and blocks apicoplast biogenesis, thus explaining apicoplast dependence on isoprenoid synthesis. We hypothesize that PPS synthesizes long-chain polyprenols critical for apicoplast membrane fluidity and biogenesis. This work critically expands the paradigm for isoprenoid utilization in malaria parasites and identifies a novel essential branch of apicoplast metabolism suitable for therapeutic targeting.
© 2022, Okada et al.

Entities:  

Keywords:  P. falciparum; apicoplast; biochemistry; chemical biology; infectious disease; isoprenoids; malaria; microbiology; organelle biogenesis; polyprenol synthase

Mesh:

Substances:

Year:  2022        PMID: 35257658      PMCID: PMC8959605          DOI: 10.7554/eLife.73208

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.140


  96 in total

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