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The Pore-Forming Toxin Listeriolysin O Mediates a Novel Entry Pathway of L. monocytogenes into Human Hepatocytes

Author: A Bavdek
A Camejo
A Camilli
A Grundling
A Krawczyk-Balska
A Sukeno
AC Haghighat
AI Bakardjiev
AI Iliev
AJ Farrand
Anne-Cécile Haghighat
B Bergmann
B Joseph
BG Gellin
BH Jost
BH Russell
C Alvarez-Dominguez
C Parsot
C Sabet
D Cabanes
DA Portnoy
DW Schuerch
E Arnett
E Milohanic
E Veiga
Elisabeth M. Wilson-Kubalek
EM Hotze
Eusondia Arnett
F Nato
F Stavru
FC Los
Guy Tran Van Nhieu
HM Marriott
I Iacovache
IJ Glomski
J Bielecki
J Mengaud
J Pizarro-Cerda
J Pizarro-Cerda
J Pizarro-Cerda
J Thiery
JA Ibarra
JA Vazquez-Boland
JA Vazquez-Boland
JC Madden
JE Galan
JL Gaillard
JL Gaillard
JL Gaillard
JR Zhang
K Ireton
K Rottner
K Smith
KA Jackson
KE Price
KM Burkholder
KS Giddings
KS Giddings
L Braun
LA Shepard
LG Tilney
LK Logsdon
M Lara-Tejero
M Lecuit
M Pentecost
M Pentecost
M Suarez
MC Fernandes
MG Ammendolia
MM Gedde
MR Gonzalez
N Magassa
NO Gekara
O Disson
O Reis
O Reis
P Cossart
P Cossart
P Cossart
P Cossart
P Glaser
P Schnupf
R Henry
R Ramachandran
RK Tweten
Rodney K. Tweten
S Dramsi
S Dramsi
S Dramsi
S Jones
S Kumari
S Mayor
S Seveau
S Seveau
S Seveau
SC Sahu
SE Gelber
SE Wickham
SJ Billington
SK Linden
Stephanie Seveau
Stephen Vadia
T Nagai
TJ Mitchell
UM Talbot
V Idone
VI Pushkareva
Y Shen
Y Valdez
Publication venue: Public Library of Science
Publication date: 01/11/2011
Field of study

Intracellular pathogens have evolved diverse strategies to invade and survive within host cells. Among the most studied facultative intracellular pathogens, Listeria monocytogenes is known to express two invasins-InlA and InlB-that induce bacterial internalization into nonphagocytic cells. The pore-forming toxin listeriolysin O (LLO) facilitates bacterial escape from the internalization vesicle into the cytoplasm, where bacteria divide and undergo cell-to-cell spreading via actin-based motility. In the present study we demonstrate that in addition to InlA and InlB, LLO is required for efficient internalization of L. monocytogenes into human hepatocytes (HepG2). Surprisingly, LLO is an invasion factor sufficient to induce the internalization of noninvasive Listeria innocua or polystyrene beads into host cells in a dose-dependent fashion and at the concentrations produced by L. monocytogenes. To elucidate the mechanisms underlying LLO-induced bacterial entry, we constructed novel LLO derivatives locked at different stages of the toxin assembly on host membranes. We found that LLO-induced bacterial or bead entry only occurs upon LLO pore formation. Scanning electron and fluorescence microscopy studies show that LLO-coated beads stimulate the formation of membrane extensions that ingest the beads into an early endosomal compartment. This LLO-induced internalization pathway is dynamin-and F-actin-dependent, and clathrin-independent. Interestingly, further linking pore formation to bacteria/bead uptake, LLO induces F-actin polymerization in a tyrosine kinase-and pore-dependent fashion. In conclusion, we demonstrate for the first time that a bacterial pathogen perforates the host cell plasma membrane as a strategy to activate the endocytic machinery and gain entry into the host cell

Public Library of Science (PLOS)

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