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  3. Microvesicle Shedding and Lysosomal Repair Fulfill Divergent Cellular Needs during the Repair of Streptolysin O-Induced Plasmalemmal Damage
 

Microvesicle Shedding and Lysosomal Repair Fulfill Divergent Cellular Needs during the Repair of Streptolysin O-Induced Plasmalemmal Damage

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BORIS DOI
10.7892/boris.50032
Publisher DOI
10.1371/journal.pone.0089743
Description
Pathogenic bacteria secrete pore-forming toxins that permeabilize the plasma membrane of host cells. Nucleated cells possess protective mechanisms that repair toxin-damaged plasmalemma. Currently two putative repair scenarios are debated: either the isolation of the damaged membrane regions and their subsequent expulsion as microvesicles (shedding) or lysosome-dependent repair might allow the cell to rid itself of its toxic cargo and prevent lysis. Here we provide evidence that both mechanisms operate in tandem but fulfill diverse cellular needs. The prevalence of the repair strategy varies between cell types and is guided by the severity and the localization of the initial toxin-induced damage, by the morphology of a cell and, most important, by the incidence of the secondary mechanical damage. The surgically precise action of microvesicle shedding is best suited for the instant elimination of individual toxin pores, whereas lysosomal repair is indispensable for mending of self-inflicted mechanical injuries following initial plasmalemmal permeabilization by bacterial toxins. Our study provides new insights into the functioning of non-immune cellular defenses against bacterial pathogens.
Date of Publication
2014-02-21
Publication Type
Article
Subject(s)
600 - Technology::610 - Medicine & health
Language(s)
en
Contributor(s)
Atanassoff, Alexander P.
Institut für Anatomie, Zellbiologie
Wolfmeier, Heidi Annemarie
Institut für Anatomie
Schönauer, Romanorcid-logo
Institut für Anatomie
Hostettler, Andrea
Institut für Anatomie, Zellbiologie
Ring, Avi
Draeger, Annette
Lehrkörper, Medizinische Fakultät
Babiichuk, Eduard
Institut für Anatomie, Zellbiologie
Additional Credits
Institut für Anatomie, Zellbiologie
Institut für Anatomie
Lehrkörper, Medizinische Fakultät
Series
PLoS ONE
Publisher
Public Library of Science
ISSN
1932-6203
Access(Rights)
open.access
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