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The Chemokine CXCL12 Is Essential for the Clearance of the Filaria Litomosoides sigmodontis in Resistant Mice

Author: A Amara
A Coulomb-L'Hermin
A Foussat
A Goostrey
A Hoerauf
A Khan
A Zlotnik
B Haribabu
C Martin
C Martin
C Martin
C Martin
C Martin
Catherine Moulia
CC Bleul
CC Bleul
Coralie Martin
CR Anderson
CS Colmont
DL Lee
E Ferri
EH Choi
Emilie Brotin
F Bachelerie
F Sierro
Françoise Bachelerie
G Petit
Gaelle Dénécé
GR Ihaka R
H Kajiyama
H Katayama
JD Turner
JE Allen
Jean Luc Galzi
JH Park
JS Hu
JS Park
K Balabanian
K Tachibana
Katharina Ehrhardt
KM Al-Qaoud
KM Al-Qaoud
L Volkmann
Laurent Gavotte
Laurent Rénia
M Diagne
M Hachet-Haas
M Kucia
MA Kowalska
MC Negrete-Garcia
ME DeVries
MR Garnica
Muriel Hachet-Haas
N Karin
N Kuroda
N Topley
Nathaly Lhermitte-Vallarino
NW Brattig
NW Lukacs
O Bain
Odile Bain
P Marechal
P Salvatore
PJ McCormick
Q Ma
R Forster
R Fredriksson
R Mohle
RM Maizels
S Babayan
S Babayan
S Babu
S Liekens
S Mancardi
SA Babayan
T Attout
T Nagasawa
Tarik Attout
Tiffany Bouchery
TM Doyle
V Machelon
VB Antony
W Hartmann
YR Zou
Publication venue: Public Library of Science
Publication date: 12/04/2012
Field of study

Litomosoides sigmodontis is a cause of filarial infection in rodents. Once infective larvae overcome the skin barrier, they enter the lymphatic system and then settle in the pleural cavity, causing soft tissue infection. The outcome of infection depends on the parasite's modulatory ability and also on the immune response of the infected host, which is influenced by its genetic background. The goal of this study was to determine whether host factors such as the chemokine axis CXCL12/CXCR4, which notably participates in the control of immune surveillance, can influence the outcome of the infection. We therefore set up comparative analyses of subcutaneous infection by L. sigmodontis in two inbred mouse strains with different outcomes: one susceptible strain (BALB/c) and one resistant strain (C57BL/6). We showed that rapid parasite clearance was associated with a L. sigmodontis-specific CXCL12-dependent cell response in C57BL/6 mice. CXCL12 was produced mainly by pleural mesothelial cells during infection. Conversely, the delayed parasite clearance in BALB/c mice was neither associated with an increase in CXCL12 levels nor with cell influx into the pleural cavity. Remarkably, interfering with the CXCL12/CXCR4 axis in both strains of mice delayed filarial development, as evidenced by the postponement of the fourth molting process. Furthermore, the in vitro growth of stage 4 filariae was favored by the addition of low amounts of CXCL12. The CXCL12/CXCR4 axis thus appears to have a dual effect on the L. sigmodontis life cycle: by acting as a host-cell restriction factor for infection, and as a growth factor for worms

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HAL - Normandie Université

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Public Library of Science (PLOS)

Biology of urothelial tumorigenesis: insights from genetically engineered mice

Author: A Chapelle de la
A Cristofano Di
A Flesken-Nikitin
A Garcia-Espana
A Sun
A Suzuki
A Vidal
AH Jebar
AM Puzio-Kuter
AR Clarke
BW Rhijn van
C Cordon-Cardo
CA Reznikoff
CD Hurst
CP Dinney
D Ahuja
D Cappellen
D Cappellen
D Hanahan
D MacPherson
D Malkin
DS Wang
E Monsonego-Ornan
EA Kurzrock
EM Messing
EM Messing
EY Lee
F Vazquez
FM Deng
FM Watt
FP Li
H Tsuruta
HB Grossman
HO Negrete
I Nathke
J Cheng
J Cheng
J Gao
J Kagan
J Li
J Liu
J Yu
J Yu
JH Lin
JJ Gildea
JS Aveyard
K Podsypanina
K Sibley
KM Rieger-Christ
KR Porter
KW Gripp
KW Gripp
KW Hunter
KW Kinzler
L Mo
L Mo
LA Donehower
LC Pagliaro
LG Koss
LI Yoo
LM Chow
M Kanai
M Rassoulzadegan
M Tanaka
M Tartaglia
MC Naski
ME Crosby
MF Lara
MR Stratton
N Ghebranious
NH Chow
NR Leslie
NS Fracchiolla
P Cairns
P Franceschini
PA Jones
PJ Grippo
R Moll
R Wu
RE Walker
RJ Cote
RL Wu
RM Hicks
RM Hicks
S Gustafson
S Marino
S Signoretti
S Urakami
SA Lewis
SH Ali
SM Cohen
SV Madhunapantula
T Jacks
TT Sun
WM Linehan
WY Kim
X Ma
X Zhang
X-R Wu
XR Wu
XR Wu
XR Wu
XR Wu
Xue-Ru Wu
Y Aoki
YM Agazie
ZT Zhang
ZT Zhang
Publication venue: Springer US
Publication date: 01/01/2009
Field of study

Urothelium, one of the slowest cycling epithelia in the body, embodies a unique biological context for cellular transformation. Introduction of oncogenes into or removing tumor suppressor genes from the urothelial cells or a combination of both using the transgenic and/or knockout mouse approaches has provided useful insights into the molecular mechanisms of urothelial transformation and tumorigenesis. It is becoming increasingly clear that over-activation of the receptor tyrosine kinase (RTK) pathway, as exemplified by the constitutively activated Ha-ras oncogene, is both necessary and sufficient to initiate the low-grade, non-invasive urothelial carcinomas. Dosage of the mutated Ha-ras, but not concurrent inactivation of pro-senescence molecules p16Ink4a and p19Arf, dictates whether and when the low-grade urothelial carcinomas arise. Inactivation of both p53 and pRb, a prevailing paradigm previously proposed for muscle-invasive urothelial tumorigenesis, is found to be necessary but insufficient to initiate this urothelial carcinoma variant. Instead, downregulation in p53/pRb co-deficient urothelial cells of p107, a pRb family member, is associated with the genesis of the muscle-invasive bladder cancers. p53 deficiency also seems to be capable of cooperating with that of PTEN in eliciting invasive urothelial carcinomas. The genetically engineered mice have improved the molecular definition of the divergent pathways of urothelial tumorigenesis and progression, helped delineate the intricate crosstalk among different genetic alterations within a urothelium-specific context, identified new prognostic markers and novel therapeutic targets potentially applicable for clinical intervention, and provided in vivo platforms for testing preventive strategies of bladder cancer