Gene/Protein
Disease
Symptom
Drug
Enzyme
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Pivot Concepts:
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Target Concepts:
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Query: UMLS:C0024141 (
systemic lupus erythematosus
)
44,322
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Susceptibility of activated T cells to apoptosis must be tightly regulated to ensure sufficient T cell progeny for an effective response, while allowing a rapid depletion of them at the end of the immune response. We show here that a previously isolated, NF-kappa B/rel target gene
IEX-1
(Immediate Early response gene X-1) is highly expressed in T cells at early stages of activation, but declines with a prolonged period of activation time, coincident with an increased susceptibility of T cells to apoptosis during the late phases of an immune response. Transgenic expression of
IEX-1
specifically in lymphocytes impaired apoptosis in activated T cells, extended a duration of an effector-phase of a specific immune response, and increased the accumulation of effector/memory-like T cells and the susceptibility to a
lupus
-like autoimmune disease. Our study demonstrated an antiapoptotic effect of
IEX-1
on T cell apoptosis triggered by ligation of Fas and T cell receptor (TCR)/CD3 complex. The ability of extending life expectancy of T effectors, in line with a decrease in its expression following prolonged T cell activation, suggests a key role for
IEX-1
in regulating T cell homeostasis during immune responses.
...
PMID:Impaired apoptosis, extended duration of immune responses, and a lupus-like autoimmune disease in IEX-1-transgenic mice. 1178 30
In response to changes in the external environment cells must initiate a coordinated program of gene expression for them to adapt.
IEX-1
(immediate early response gene X-1) is precisely regulated by multiple transcription factors among which p53, NF-kappaB/rel, Sp1 and c-Myc play central roles, to ensure rapid and transient expression of
IEX-1
in cells under a variety of stress conditions. Overexpression of
IEX-1
renders some cells sensitive to apoptosis and accelerates cell cycle progression, but reduces proliferation of other cells, whereas disruption of
IEX-1
expression is associated with decreases in both apoptosis and cell cycle progression. In sharp contrast to in vitro studies, in vivo constitutive expression of
IEX-1
prevents activated T cells but not B cells from apoptosis, as shown using
IEX-1
-transgenic mice that target
IEX-1
expression specifically to lymphocytes driven by the Emu enhancer. The animals developed a
lupus
-like disease and subsequently a high incidence of T cell lymphomas when they aged, due to insufficient apoptosis of T cells. These varied effects of
IEX-1
on cell death and cell cycle progression in a cell-context dependent fashion implicate that
IEX-1
is involved in more than one signaling pathway, understanding of which will certainly improve our knowledge with respect to cancer biology, cell death and cell cycle regulation.
...
PMID:Roles of the stress-induced gene IEX-1 in regulation of cell death and oncogenesis. 1251 Jan 47
