Biogenesis of Peroxisomes and Glycosomes: Trypanosomatid Glycosome Assembly is a Promising New Drug Target

Overview

Journal FEMS Microbiol Rev

Publisher Oxford University Press

Specialty Microbiology

Date 2004 Nov 13

PMID 15539076

Citations 32

Authors

Juliette Moyersoen

Jungwoo Choe

Erkang Fan

Wim G J Hol

Paul A M Michels

Affiliations

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Abstract

In trypanosomatids (Trypanosoma and Leishmania), protozoa responsible for serious diseases of mankind in tropical and subtropical countries, core carbohydrate metabolism including glycolysis is compartmentalized in peculiar peroxisomes called glycosomes. Proper biogenesis of these organelles and the correct sequestering of glycolytic enzymes are essential to these parasites. Biogenesis of glycosomes in trypanosomatids and that of peroxisomes in other eukaryotes, including the human host, occur via homologous processes involving proteins called peroxins, which exert their function through multiple, transient interactions with each other. Decreased expression of peroxins leads to death of trypanosomes. Peroxins show only a low level of sequence conservation. Therefore, it seems feasible to design compounds that will prevent interactions of proteins involved in biogenesis of trypanosomatid glycosomes without interfering with peroxisome formation in the human host cells. Such compounds would be suitable as lead drugs against trypanosomatid-borne diseases.

Citing Articles

PEX1 is essential for glycosome biogenesis and trypanosomatid parasite survival.

Mahadevan L, Arya H, Droste A, Schliebs W, Erdmann R, Kalel V Front Cell Infect Microbiol. 2024; 14:1274506.

PMID: 38510966 PMC: 10952002. DOI: 10.3389/fcimb.2024.1274506.

Molecular basis of the glycosomal targeting of PEX11 and its mislocalization to mitochondrion in trypanosomes.

Krishna C, Schmidt N, Tippler B, Schliebs W, Jung M, Winklhofer K Front Cell Dev Biol. 2023; 11:1213761.

PMID: 37664461 PMC: 10469627. DOI: 10.3389/fcell.2023.1213761.

A Novel Group of Dynamin-Related Proteins Shared by Eukaryotes and Giant Viruses Is Able to Remodel Mitochondria From Within the Matrix.

Sheikh S, Panek T, Gahura O, Tyc J, Zahonova K, Lukes J Mol Biol Evol. 2023; 40(6).

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The History of the ABC Proteins in Human Trypanosomiasis Pathogens.

Da Costa K, Valente R, Fonseca L, Freire-de-Lima L, Previato J, Mendonca-Previato L Pathogens. 2022; 11(9).

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Microorganisms as a Potential Source of Molecules to Control Trypanosomatid Diseases.

Chan-Bacab M, Reyes-Estebanez M, Camacho-Chab J, Ortega-Morales B Molecules. 2021; 26(5).

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