Parasite Motility is Critical for Virulence of African Trypanosomes

Overview

Journal Sci Rep

Specialty Science

Date 2018 Jun 16

PMID 29904094

Citations 29

Authors

Michelle M Shimogawa

Sunayan S Ray

Neville Kisalu

Yibo Zhang

Quanjie Geng

Aydogan Ozcan

Kent L Hill

Affiliations

Soon will be listed here.

Abstract

African trypanosomes, Trypanosoma brucei spp., are lethal pathogens that cause substantial human suffering and limit economic development in some of the world's most impoverished regions. The name Trypanosoma ("auger cell") derives from the parasite's distinctive motility, which is driven by a single flagellum. However, despite decades of study, a requirement for trypanosome motility in mammalian host infection has not been established. LC1 is a conserved dynein subunit required for flagellar motility. Prior studies with a conditional RNAi-based LC1 mutant, RNAi-K/R, revealed that parasites with defective motility could infect mice. However, RNAi-K/R retained residual expression of wild-type LC1 and residual motility, thus precluding definitive interpretation. To overcome these limitations, here we generate constitutive mutants in which both LC1 alleles are replaced with mutant versions. These double knock-in mutants show reduced motility compared to RNAi-K/R and are viable in culture, but are unable to maintain bloodstream infection in mice. The virulence defect is independent of infection route but dependent on an intact host immune system. By comparing different mutants, we also reveal a critical dependence on the LC1 N-terminus for motility and virulence. Our findings demonstrate that trypanosome motility is critical for establishment and maintenance of bloodstream infection, implicating dynein-dependent flagellar motility as a potential drug target.

Citing Articles

FAP20 is required for flagellum assembly in .

Shimogawa M, Jonnalagadda K, Hill K Mol Biol Cell. 2024; 35(11):br22.

PMID: 39382839 PMC: 11617092. DOI: 10.1091/mbc.E23-12-0497.

FAP20 is required for flagellum assembly in .

Shimogawa M, Jonnalagadda K, Hill K bioRxiv. 2024; .

PMID: 38293126 PMC: 10827224. DOI: 10.1101/2024.01.19.576295.

FLAgellum Member 8 modulates extravascular distribution of African trypanosomes.

Calvo-Alvarez E, Tsagmo Ngoune J, Sharma P, Cooper A, Camara A, Travaille C PLoS Pathog. 2023; 19(12):e1011220.

PMID: 38127941 PMC: 10769064. DOI: 10.1371/journal.ppat.1011220.

Propulsive cell entry diverts pathogens from immune degradation by remodeling the phagocytic synapse.

Zhang Z, Gaetjens T, Ou J, Zhou Q, Yu Y, Mallory D Proc Natl Acad Sci U S A. 2023; 120(49):e2306788120.

PMID: 38032935 PMC: 10710034. DOI: 10.1073/pnas.2306788120.

FAP106 is an interaction hub for assembling microtubule inner proteins at the cilium inner junction.

Shimogawa M, Wijono A, Wang H, Zhang J, Sha J, Szombathy N Nat Commun. 2023; 14(1):5225.

PMID: 37633952 PMC: 10460401. DOI: 10.1038/s41467-023-40230-z.

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