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CD14 Modulates PI3K/AKT/p38-MAPK Licensing of Negative Regulators of TLR Signaling to Restrain Chronic Inflammation

Author: Bikash Sahay
Christian H. Eggers
Justin D. Radolf
Nicole Whatley
Rebeca L. Patsey
Sasmita Nayak
Timothy J. Sellati
Publication venue
Publication date: 24/06/2008
Field of study

Current thinking emphasizes the primacy of CD14 in facilitating TLR recognition of microbes to initiate proinflammatory signaling events and the importance of p38-MAPK in augmenting such responses. Herein, this paradigm is challenged by demonstrating that recognition of _Borrelia burgdorferi_ not only triggers an inflammatory response in the absence of CD14, but one that is uncontrolled as a consequence of impaired PI3K/AKT/p38-MAPK signaling and negative regulation of TLR2. CD14 deficiency results in hyperphosphorylation of AKT and reduced activation of p38. Such aberrant signaling leads to decreased negative regulation by SOCS1, SOCS3, and CIS thereby engendering a more severe and persistent inflammatory response to _B. burgdorferi_. Perturbation of this CD14/p38-MAPK-dependent mechanism of immune regulation may underlie development of infectious chronic inflammatory syndromes

Nature Precedings

CD14 Signaling Restrains Chronic Inflammation through Induction of p38-MAPK/SOCS-Dependent Tolerance

Author: A Arcaro
A Haziot
A Mansell
A Marangoni
A Matsuzawa
A Pfeiffer
AB Abdel Shakor
AC Steere
AE Medvedev
AH Kim
AK Behera
AK Behera
AR Cruz
B Tamilselvam
B van den Blink
BA Croker
BE Steinberg
Bikash Sahay
C Ropert
C Werts
CH Eggers
Christian H. Eggers
CM Olson
CM Rosenberger
D Brown
D Jo
DA Brown
DE Schiff
DW Zaas
E Hollenbach
E-M Kramer
F Graeme
F Lafont
F Lafont
FY Liew
GL Schieven
H Chi
H Fan
H Gresham
H Ogura
H Saito
HJ Kim
I Diterich
I Stefanova
ID Dimitriou
IM Ferby
J Coburn
J Han
JA Boylan
JA Boylan
JC Salazar
JD Li
Jenifer Coburn
JF Dermine
JG Bode
JG Bode
JLE Dean
JM Anderson
JM Blander
JP Gratton
JS Adams
Juan C. Salazar
Justin D. Radolf
K Wehkamp
KD Moody
KGN Suzuki
KGN Suzuki
L Arbibe
LJ Reed
M Cinco
M Guerau-de-Arellano
M Orio
MK Warren
MR Benhnia
MW Moore
N Liu
O Leupin
OS Shin
OS Shin
PJ Egan
PT Liu
R Nakagawa
R Schroeder
Rebeca L. Patsey
RM Wooten
RM Wooten
RM Wooten
RM Wooten
RS Flannagan
RZ Murray
S Antal
S Antonara
S Koji
S Krisanaprakornkit
S Liu
S Mayor
S Narasimhan
SA Pancewicz
SC Gangloff
SL Foster
SP Nash
T Shouda
T Yeung
T Yeung
Timothy J. Sellati
TJ Sellati
V Albrecht
VA Dennis
X Guo
Y Ma
Z Jiang
ZA Knight
Publication venue: Public Library of Science
Publication date: 01/01/2009
Field of study

Current thinking emphasizes the primacy of CD14 in facilitating recognition of microbes by certain TLRs to initiate pro-inflammatory signaling events and the importance of p38-MAPK in augmenting such responses. Herein, this paradigm is challenged by demonstrating that recognition of live Borrelia burgdorferi not only triggers an inflammatory response in the absence of CD14, but one that is, in part, a consequence of altered PI3K/AKT/p38-MAPK signaling and impaired negative regulation of TLR2. CD14 deficiency results in increased localization of PI3K to lipid rafts, hyperphosphorylation of AKT, and reduced activation of p38. Such aberrant signaling leads to decreased negative regulation by SOCS1, SOCS3, and CIS, thereby compromising the induction of tolerance in macrophages and engendering more severe and persistent inflammatory responses to B. burgdorferi. Importantly, these altered signaling events and the higher cytokine production observed can be mimicked through shRNA and pharmacological inhibition of p38 activity in CD14-expressing macrophages. Perturbation of this CD14/p38-MAPK-dependent immune regulation may underlie development of infectious chronic inflammatory syndromes

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