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20 research outputs found

Spleen Tyrosine Kinase (Syk) Regulates Systemic Lupus Erythematosus (SLE) T Cell Signaling

Author: Alexandros P. Grammatikos
Amy Devlin
AP Grammatikos
AP Grammatikos
C Bombardier
CG Katsiari
D Ghosh
Debjani Ghosh
G Chen
GC Tsokos
George C. Tsokos
GM Deng
J Tang
JC Crispín
JC Crispín
JC Crispín
JC Crispín
JM Oliver
K Gee
KM Dennehy
M Deckert
M Sarra
MC Hochberg
MP Nambiar
P Blanco
RA Cohen
S Krishnan
S Xu
SN Liossis
Stamatis-Nick Liossis
V Pascual
Vasileios C. Kyttaris
VC Kyttaris
VC Kyttaris
Y Li
YT Juang
YT Juang
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/01/2013
Field of study

Engagement of the CD3/T cell receptor complex in systemic lupus erythematosus (SLE) T cells involves Syk rather than the zeta-associated protein. Because Syk is being considered as a therapeutic target we asked whether Syk is central to the multiple aberrantly modulated molecules in SLE T cells. Using a gene expression array, we demonstrate that forced expression of Syk in normal T cells reproduces most of the aberrantly expressed molecules whereas silencing of Syk in SLE T cells normalizes the expression of most abnormally expressed molecules. Protein along with gene expression modulation for select molecules was confirmed. Specifically, levels of cytokine IL-21, cell surface receptor CD44, and intracellular molecules PP2A and OAS2 increased following Syk overexpression in normal T cells and decreased after Syk silencing in SLE T cells. Our results demonstrate that levels of Syk affect the expression of a number of enzymes, cytokines and receptors that play a key role in the development of disease pathogenesis in SLE and provide support for therapeutic targeting in SLE patients

Public Library of Science (PLOS)

Crossref

Harvard University - DASH

Directory of Open Access Journals

PubMed Central

The University of North Carolina at Greensboro

ScholarShip

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TNF-α and TGF-β Counter-Regulate PD-L1 Expression on Monocytes in Systemic Lupus Erythematosus

Author: A Hrycek
A La Cava
A Starke
A Studnicka-Benke
AK Abelson
AK Palucka
AL Kinter
AY Gong
B Schreiner
B Wan
C Bombardier
CG Katsiari
CM Thorburn
CO Jacob
D Ding
D Haller
DM Santer
GK Bertsias
H Dong
H Nishimura
J Massague
J Zhu
JA Brown
JA Lucas
JC Crispin
JJ O'Shea
K Ghoreschi
K Ohtsuka
KE Brown
L Ronnblom
L Zhu
LJ Zhu
LM Francisco
LM Holets
M Marzec
M Saito
M Suarez-Gestal
M Wong
MC Hochberg
ME Keir
N Mozaffarian
N Parameswaran
NJ McHugh
P Blanco
R Velazquez-Cruz
S Amarnath
S Hegde
S Kasagi
S Monrad
S Sule
SC Wang
SJ Wolfle
T Atsumi
TK Khera
U O'Doherty
V Saxena
Y Chen
Y Waeckerle-Men
YH Lee
Publication venue: Nature Publishing Group
Publication date
Field of study

Monocytes in patients with systemic lupus erythematosus (SLE) are hyperstimulatory for T lymphocytes. We previously found that the normal program for expression of a negative costimulatory molecule programmed death ligand-1 (PD-L1) is defective in SLE patients with active disease. Here, we investigated the mechanism for PD-L1 dysregulation on lupus monocytes. We found that PD-L1 expression on cultured SLE monocytes correlated with TNF-α expression. Exogenous TNF-α restored PD-L1 expression on lupus monocytes. Conversely, TGF-β inversely correlated with PD-L1 in SLE and suppressed expression of PD-L1 on healthy monocytes. Therefore, PD-L1 expression in monocytes is regulated by opposing actions of TNF-α and TGF-β. As PD-L1 functions to fine tune lymphocyte activation, dysregulation of cytokines resulting in reduced expression could lead to loss of peripheral T cell tolerance

Crossref

PubMed Central