Loss of a Cardiolipin Synthase in Helicobacter pylori G27 Blocks Flagellum Assembly

Joshua K Chu; Shiwei Zhu; Carmen M Herrera; Jeremy C Henderson; Jun Liu; M Stephen Trent; Timothy R Hoover

doi:10.1128/JB.00372-19

Loss of a Cardiolipin Synthase in Helicobacter pylori G27 Blocks Flagellum Assembly

J Bacteriol. 2019 Oct 4;201(21):e00372-19. doi: 10.1128/JB.00372-19. Print 2019 Nov 1.

Authors

Joshua K Chu¹, Shiwei Zhu², Carmen M Herrera³, Jeremy C Henderson³, Jun Liu², M Stephen Trent³, Timothy R Hoover⁴

Affiliations

¹ Department of Microbiology, University of Georgia, Athens, Georgia, USA.
² Department of Microbial Pathogenesis, Microbial Sciences Institute, Yale University, West Haven, Connecticut, USA.
³ Department of Infectious Diseases, University of Georgia, Athens, Georgia, USA.
⁴ Department of Microbiology, University of Georgia, Athens, Georgia, USA trhoover@uga.edu.

Abstract

Helicobacter pylori uses a cluster of polar, sheathed flagella for motility, which it requires for colonization of the gastric epithelium in humans. As part of a study to identify factors that contribute to localization of the flagella to the cell pole, we disrupted a gene encoding a cardiolipin synthase (clsC) in H. pylori strains G27 and B128. Flagellum biosynthesis was abolished in the H. pylori G27 clsC mutant but not in the B128 clsC mutant. Transcriptome sequencing analysis showed that flagellar genes encoding proteins needed early in flagellum assembly were expressed at wild-type levels in the G27 clsC mutant. Examination of the G27 clsC mutant by cryo-electron tomography indicated the mutant assembled nascent flagella that contained the MS ring, C ring, flagellar protein export apparatus, and proximal rod. Motile variants of the G27 clsC mutant were isolated after allelic exchange mutagenesis using genomic DNA from the B128 clsC mutant as the donor. Genome resequencing of seven motile G27 clsC recipients revealed that each isolate contained the flgI (encodes the P-ring protein) allele from B128. Replacing the flgI allele in the G27 clsC mutant with the B128 flgI allele rescued flagellum biosynthesis. We postulate that H. pylori G27 FlgI fails to form the P ring when cardiolipin levels in the cell envelope are low, which blocks flagellum assembly at this point. In contrast, H. pylori B128 FlgI can form the P ring when cardiolipin levels are low and allows for the biosynthesis of mature flagella.IMPORTANCEH. pylori colonizes the epithelial layer of the human stomach, where it can cause a variety of diseases, including chronic gastritis, peptic ulcer disease, and gastric cancer. To colonize the stomach, H. pylori must penetrate the viscous mucous layer lining the stomach, which it accomplishes using its flagella. The significance of our research is identifying factors that affect the biosynthesis and assembly of the H. pylori flagellum, which will contribute to our understanding of motility in H. pylori, as well as other bacterial pathogens that use their flagella for host colonization.

Keywords: Helicobacter pylori; cardiolipin; cardiolipin synthase; flagellum.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Alleles
Bacterial Proteins
Flagella / genetics*
Gene Expression Regulation, Bacterial / genetics
Helicobacter pylori / genetics*
Humans
Membrane Proteins / genetics*
Mutagenesis / genetics
Mutation / genetics
Transcriptome / genetics
Transferases (Other Substituted Phosphate Groups) / genetics*

Substances

Bacterial Proteins
Membrane Proteins
Transferases (Other Substituted Phosphate Groups)
cardiolipin synthetase

Abstract

Publication types

MeSH terms

Substances

Grants and funding