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The entry of Salmonella in a distinct tight compartment revealed at high temporal and ultrastructural resolution

Authors :
Michael Elbaum
Virginie Stévenin
Jacomine Krijnse-Locker
Katya Rechav
Jennifer Fredlund
Patricia Latour-Lambert
Jost Enninga
Adeline Mallet
Allon Weiner
José Carlos Santos
Dynamique des Interactions Hôte-Pathogène - Dynamics of Host-Pathogen Interactions
Institut Pasteur [Paris]-Centre National de la Recherche Scientifique (CNRS)
Department of Materials and Interfaces [Rehovot, Israël]
Weizmann Institute of Science [Rehovot, Israël]
Microscopie ultrastructurale - Ultrapole (CITECH)
Institut Pasteur [Paris]
This work was funded by grants from the Pasteur‐Weizmann Foundation to J. E., by a fellowship from the Pasteur Foundation to J. F. by the FCT (SFRH/BD/51006/2010), and an Institut Pasteur PTR grant to J. C. S. by fellowships from the Pasteur‐Weizmann Foundation and the FRM to A. W., by a fellowship from the University Paris Diderot allocated by the ENS Cachan, Université Paris‐Saclay, and a grant from the FRM to V.S., and by grants from the ANR (StopBugEntry), and the European Research Council (Starting grant 'Rupteffects' and Consolidator grant 'EndoSubvert') to J. E.
ANR-15-CE15-0017,StopBugEntry,Identification des nouvelles molécules cellulaires cibles pour combattre les infections bactériennes(2015)
European Project: 261166,EC:FP7:ERC,ERC-2010-StG_20091118,RUPTEFFECTS(2011)
European Project: 682809,EndoSubvert(2017)
Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS)
Institut Pasteur [Paris] (IP)
Source :
Cellular Microbiology, Cellular Microbiology, Wiley, 2018, 20 (4), ⟨10.1111/cmi.12816⟩, Cellular Microbiology, 2018, 20 (4), ⟨10.1111/cmi.12816⟩

Abstract

International audience; Salmonella enterica induces membrane ruffling and genesis of macropinosomes during its interactions with epithelial cells. This is achieved through the type three secretion system-1, which first mediates bacterial attachment to host cells and then injects bacterial effector proteins to alter host behaviour. Next, Salmonella enters into the targeted cell within an early membrane-bound compartment that matures into a slow growing, replicative niche called the Salmonella Containing Vacuole (SCV). Alternatively, the pathogen disrupts the membrane of the early compartment and replicate at high rate in the cytosol. Here, we show that the in situ formed macropinosomes, which have been previously postulated to be relevant for the step of Salmonella entry, are key contributors for the formation of the mature intracellular niche of Salmonella. We first clarify the primary mode of type three secretion system-1 induced Salmonella entry into epithelial cells by combining classical fluorescent microscopy with cutting edge large volume electron microscopy. We observed that Salmonella, similarly to Shigella, enters epithelial cells inside tight vacuoles rather than in large macropinosomes. We next apply this technology to visualise rupturing Salmonella containing compartments, and we use extended time-lapse microscopy to establish early markers that define which Salmonella will eventually hyper replicate. We show that at later infection stages, SCVs harbouring replicating Salmonella have previously fused with the in situ formed macropinosomes. In contrast, such fusion events could not be observed for hyper-replicating Salmonella, suggesting that fusion of the Salmonella entry compartment with macropinosomes is the first committed step of SCV formation.

Details

Language :
English
ISSN :
14625814 and 14625822
Volume :
20
Issue :
4
Database :
OpenAIRE
Journal :
Cellular Microbiology
Accession number :
edsair.doi.dedup.....b38becc7fbdbd78e55d8fc7f1dab860b
Full Text :
https://doi.org/10.1111/cmi.12816