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10 research outputs found

Spleen-Resident CD4+ and CD4− CD8α− Dendritic Cell Subsets Differ in Their Ability to Prime Invariant Natural Killer T Lymphocytes

One important function of conventional dendritic cells (cDC) is their high capacity to capture, process and present Ag to T lymphocytes. Mouse splenic cDC subtypes, including CD8α+ and CD8α− cDC, are not identical in their Ag presenting and T cell priming functions. Surprisingly, few studies have reported functional differences between CD4− and CD4+ CD8α− cDC subsets. We show that, when loaded in vitro with OVA peptide or whole protein, and in steady-state conditions, splenic CD4− and CD4+ cDC are equivalent in their capacity to prime and direct CD4+ and CD8+ T cell differentiation. In contrast, in response to α-galactosylceramide (α-GalCer), CD4− and CD4+ cDC differentially activate invariant Natural Killer T (iNKT) cells, a population of lipid-reactive non-conventional T lymphocytes. Both cDC subsets equally take up α-GalCer in vitro and in vivo to stimulate the iNKT hybridoma DN32.D3, the activation of which depends solely on TCR triggering. On the other hand, and relative to their CD4+ counterparts, CD4− cDC more efficiently stimulate primary iNKT cells, a phenomenon likely due to differential production of co-factors (including IL-12) by cDC. Our data reveal a novel functional difference between splenic CD4+ and CD4− cDC subsets that may be important in immune responses

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PubMed Central

HAL Université de Tours

univOAK

Comparative analysis of routes of immunization of a live porcine reproductive and respiratory syndrome virus (PRRSV) vaccine in a heterologous virus challenge study

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Sublingual Vaccination Induces Mucosal and Systemic Adaptive Immunity for Protection against Lung Tumor Challenge

Author: AH Hovav
AN Courtney
AN Courtney
AP Uldrich
C Czerkinsky
C Guillonneau
C Hervouet
C Hervouet
CK Fraser
DH Chang
DX Nguyen
EC Reilly
F Agostinis
F Lemiale
F Sandoval
G Gonzalez-Aseguinolaza
GK Pedersen
Guojun Yang
H Kamijuku
IF Hermans
JD Silk
JH Choi
JH Moon
JH Song
JH Song
JK Patel
K Fujihashi
K Matsuo
K Seino
K. Jagannadha Sastry
Kimberly S. Schluns
L Mascarell
M Brigl
M Mutsch
M Papamichail
Mauricio Martins Rodrigues
ME Armstrong
MN Kweon
MR Neutra
N Cuburu
N Kunii
N Lycke
RK Naz
S Fujii
Scott M. Anthony
Shailbala Singh
SP Leong
VV Parekh
Publication venue: 'Public Library of Science (PLoS)'
Publication date
Field of study

Crossref

Boosting the immune response: the use of iNKT cell ligands as vaccine adjuvants

Author: A. E. Hogan
A. Motsinger
A. N. Courtney
A. P. Uldrich
B. A. Sullivan
B. J. Fowlkes
C. Bauer
C. Carnaud
D. F. Clyde
D. Kim
D. Zhou
E. D. Yu
E. Kobayashi
G. Giaccone
G. Gonzalez-Aseguinolaza
G. Velmourougane
G. Yang
H. J. Ko
H. J. Vliet van der
H. J. Youn
H. Kamijuku
H. Koseki
J. D. Silk
J. H. Nam
J. K. Sandberg
J. Mattner
J. P. Vanderberg
J. Schmieg
J. Schmieg
J.W. Molling
K. Kawakami
K. Miyamoto
L. Schofield
M. L. Blauvelt
M. Niemeyer
M. W. Teng
N. Burdin
N. Y. Crowe
O. Shibolet
P. Matangkasombut
P. T. Lee
P. Thapa
R. Fleuridor
R. G. Webster
R. Nakagawa
S. A. Kopecky-Bromberg
S. Joyce
S. Porcelli
S. Y. Ko
T. J. Roberts
T. Kawano
T. Natori
T. Osada
T. R. Petersen
T. Yoshimoto
V. Sriram
V. V. Parekh
X. Li
X. Lu
Y. Chung
Y. Huang
Y. J. Kim
Y. Kinjo
Y. Kinjo
Y. Li
Y. Makino
Y. S. Lee
Y. Yamaguchi
Y. Yoshiga
Z. Rui-Hua
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Eliciting Epitope-Specific CD8+ T Cell Response by Immunization with Microbial Protein Antigens Formulated with α-Galactosylceramide: Theory, Practice, and Protocols

Author: A Lissina
AJ Tyznik
AM Birkholz
AN Courtney
AR Rees
B Adkins
B Moss
B Pulendran
B Rodenko
C Gottschalk
C Guillonneau
C Saroja
CC Duwaerts
CJ O’Connell
CR Li
CS Wagner
E Jenner
E Segura
F Zepp
G Galli
GK Swamy
H Kamijuku
H Liu
IJ Amanna
IJ Amanna
IM Belyakov
J Alexander
J Mattner
J Schmieg
JC Montero
JE Epstein
JE Kohlmeier
JJ Moon
JS Blum
JSM Woodworth
K Miyamoto
KO Yu
L Kain
LA Albacker
LE Brown
LJ Carreno
M Morita
MJ Bevan
MS Duthie
N Singh
P Gilchuk
PG Thomas
PJR Goulder
RL Coffman
S Aspeslagh
S Aspeslagh
S Fujii
S Joyce
SA Plotkin
SN Gordon
SR Hadrup
SY Ko
T Hall van
T Kawano
T Natori
T Nishimura
T Zimmerman
TM Hill
V Gerdts
V Gerdts
V Semmling
V Verhasselt
WC Koff
X Li
Y Kinjo
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Functional Invariant NKT Cells in Pig Lungs Regulate the Airway Hyperreactivity: A Potential Animal Model

Crossref

Targeting natural killer cells and natural killer T cells in cancer.

Author: A Bendelac
A Cerwenka
A Curti
A Diefenbach
A Gratwohl
A Ishikawa
A Lundqvist
A Moretta
A Moretta
A Moretta
A Poggi
A Shimoni
A Soriani
AJ Tyznik
AK Savage
AK Stanic
AM Unni
B Beutler
B Pei
BA Sullivan
BN Savani
C Bottino
C Bottino
C Brehm
C Carnaud
C Chen
C Menard
C Paget
C Sola
C Vilches
CA Janeway Jr
Christian Chabannon
CS Brandt
D Blaise
D Blaise
D Cho
D Cosman
D De Santis
D Hanahan
D Kovalovsky
D Pende
D Pende
D Zhou
DB Stetson
DG Pellicci
DG Wei
DH Chang
DH Kim
DH McKenna Jr.
DH Raulet
DH Raulet
DH Raulet
DI Godfrey
DI Marks
Didier Blaise
DL Porter
DM Andrews
DM Benson
DM Benson Jr.
DM Gascoyne
DN Burshtyn
DY Wu
E Alici
E Holler
E Thomas
E Vivier
E Vivier
EM Dunbar
EP Alyea
Eric Vivier
F Aversa
F Dazzi
F Larosa
F Romagne
F Romagne
F Tilloy
FL Schneiders
FL Schneiders
FM Karlhofer
G Cartron
G Eberl
G Galli
G Giaccone
G Gonzalez-Aseguinolaza
G Wingender
GJ Renukaradhya
H Kamijuku
H Spits
H Wang
HG Ljunggren
HJ Kolb
IF Hermans
J Clausen
J Eckl
J Mattner
J Schmieg
J Schumann
J Shi
JB Swann
JB Swann
JC Sun
JC Sun
JD Bignon
JD Wesley
JD Wesley
JF Bukowski
JG O'Leary
JL Ferrara
JL Matsuda
JL Matsuda
JM Brand
JM Elliott
JR Carlyle
JR Passweg
JS Im
JS Miller
JS Miller
JS Orange
K Benlagha
K Benlagha
K Imai
K Kärre
K Kärre
K Miyamoto
K Shimizu
K Yamasaki
K Yanagisawa
KL McQueen
KO Yu
L Barkholt
L Chiche
L De Somer
L Gapin
L Moretta
L Olcese
L Olcese
L Ruggeri
L Ruggeri
L Song
Laurent Brossay
LL Lanier
LM Hix
LN Carayannopoulos
LS Metelitsa
M Bellone
M Brigl
M Brigl
M Brigl
M Cook
M Guo
M Kijima
M Kronenberg
M Kronenberg
M Mohty
M Nieda
M Nowak
M Salio
M Terabe
M Terme
M Vitale
MA Cooper
MA Exley
MA Geller
MD Vesely
MJ Smyth
MJ Smyth
MJ Smyth
MJ Townsend
MM Venkataswamy
MT Orr
MT Orr
MW Teng
N Anfossi
N Guerra
N Halama
N Kroger
N Kunii
N Schleinitz
N Vey
N-S Liao
NC Fernandez
NT Joncker
NT Joncker
NY Crowe
O Lantz
P Barral
P Barral
P Brodin
P Brodin
P Carrega
P Hoglund
P Parham
PJ Brennan
PL Weiden
R Castriconi
R Childs
R Kiessling
R Storb
R Storb
RB Herberman
RE Vance
RK Oldham
S Akira
S Arai
S Bauer
S Gasser
S Giebel
S Giralt
S Guia
S Kamizono
S Kim
S Kim
S Motohashi
S Nguyen
S Ogino
S Oki
S Oki
S Paust
S Platonova
S Porcelli
S Sivori
S Slavin
S Veeramani
S Verheyden
SC Yue
SH Park
SM Tahir
SN Waggoner
Sophie Ugolini
T Egawa
T Kawano
T Ranson
T Tachibana
T Walzer
Thomas Kammertoens
V Bachanova
V Cerundolo
V Kumar
VM Braud
VV Parekh
WM Yokoyama
Y Huang
Y Li
Z Dong
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2012
Field of study

International audienceNatural killer (NK) cells and natural killer T (NKT) cells are subsets of lymphocytes that share some phenotypical and functional similarities. Both cell types can rapidly respond to the presence of tumour cells and participate in antitumour immune responses. This has prompted interest in the development of innovative cancer therapies that are based on the manipulation of NK and NKT cells. Recent studies have highlighted how the immune reactivity of NK and NKT cells is shaped by the environment in which they develop. The rational use of these cells in cancer immunotherapies awaits a better understanding of their effector functions, migratory patterns and survival properties in humans