Repair of a Bacterial Small β-Barrel Toxin Pore Depends on Channel Width

Gisela von Hoven; Amable J Rivas; Claudia Neukirch; Martina Meyenburg; Qianqian Qin; Sapun Parekh; Nadja Hellmann; Matthias Husmann

doi:10.1128/mBio.02083-16

Repair of a Bacterial Small β-Barrel Toxin Pore Depends on Channel Width

mBio. 2017 Feb 14;8(1):e02083-16. doi: 10.1128/mBio.02083-16.

Authors

Gisela von Hoven¹, Amable J Rivas¹, Claudia Neukirch¹, Martina Meyenburg¹, Qianqian Qin¹, Sapun Parekh², Nadja Hellmann³, Matthias Husmann⁴

Affiliations

¹ Institute of Medical Microbiology and Hygiene, University Medical Center, Johannes Gutenberg University, Mainz, Germany.
² Max Planck Institute for Polymer Research, Mainz, Germany.
³ Institute of Molecular Biophysics, Faculty of Biology, Johannes Gutenberg University Mainz, Mainz, Germany nhellmann@uni-mainz.de husmann@uni-mainz.de.
⁴ Institute of Medical Microbiology and Hygiene, University Medical Center, Johannes Gutenberg University, Mainz, Germany nhellmann@uni-mainz.de husmann@uni-mainz.de.

Abstract

Membrane repair emerges as an innate defense protecting target cells against bacterial pore-forming toxins. Here, we report the first paradigm of Ca²⁺-dependent repair following attack by a small β-pore-forming toxin, namely, plasmid-encoded phobalysin of Photobacterium damselae subsp. damselae In striking contrast, Vibrio cholerae cytolysin, the closest ortholog of phobalysin, subverted repair. Mutational analysis uncovered a role of channel width in toxicity and repair. Thus, the replacement of serine at phobalysin´s presumed channel narrow point with the bulkier tryptophan, the corresponding residue in Vibrio cholerae cytolysin (W318), modulated Ca²⁺ influx, lysosomal exocytosis, and membrane repair. And yet, replacing tryptophan (W318) with serine in Vibrio cholerae cytolysin enhanced toxicity. The data reveal divergent strategies evolved by two related small β-pore-forming toxins to manipulate target cells: phobalysin leads to fulminant perturbation of ion concentrations, closely followed by Ca²⁺ influx-dependent membrane repair. In contrast, V. cholerae cytolysin causes insidious perturbations and escapes control by the cellular wounded membrane repair-like response.IMPORTANCE Previous studies demonstrated that large transmembrane pores, such as those formed by perforin or bacterial toxins of the cholesterol-dependent cytolysin family, trigger rapid, Ca²⁺ influx-dependent repair mechanisms. In contrast, recovery from attack by the small β-pore-forming Staphylococcus aureus alpha-toxin or aerolysin is slow in comparison and does not depend on extracellular Ca²⁺ To further elucidate the scope of Ca²⁺ influx-dependent repair and understand its limitations, we compared the cellular responses to phobalysin and V. cholerae cytolysin, two related small β-pore-forming toxins which create membrane pores of slightly different sizes. The data indicate that the channel width of a small β-pore-forming toxin is a critical determinant of both primary toxicity and susceptibility to Ca²⁺-dependent repair.

MeSH terms

Bacterial Toxins / chemistry*
Bacterial Toxins / metabolism
Calcium
Cell Membrane / chemistry
Cell Membrane / metabolism*
Cell Membrane / ultrastructure
Humans
Nanopores*
Perforin / metabolism*
Vibrio cholerae / chemistry

Substances

Bacterial Toxins
Perforin
Calcium