Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:3.4.22.36 (
caspase-1
)
6,285
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
ETS1
is a cellular homologue of the product of the viral ets oncogene of the E26 virus, and it functions as a tissue-specific transcription factor. It plays an important role in cell proliferation, differentiation, lymphoid cell development, transformation, angiogenesis, and apoptosis.
ETS1
controls the expression of critical genes involved in these processes by binding to ets binding sites present in the transcriptional regulatory regions. The
ETS1
gene generates two proteins, p51 and a spliced variant, p42, lacking exon VII. In this paper we show that p42-
ETS1
expression bypasses the damaged Fas-induced apoptotic pathway in DLD1 colon carcinoma cells by up-regulating
interleukin 1beta-converting enzyme
(
ICE
)/
caspase-1
and causes these cancer cells to become susceptible to the effects of the normal apoptosis activation system.
ICE
/
caspase-1
is a redundant system in many cells and tissues, and here we demonstrate that it is important in activating apoptosis in cells where the normal apoptosis pathway is blocked. Blocking
ICE
/
caspase-1
activity by using specific inhibitors of this protease prevents the p42-
ETS1
-induced apoptosis from occurring, indicating that the induced
ICE
/
caspase-1
enzyme is responsible for killing the cancer cells. p42-
ETS1
activates a critical alternative apoptosis pathway in cancer cells that are resistant to normal immune attack, and thus it may be useful as an anticancer therapeutic.
...
PMID:The p42 variant of ETS1 protein rescues defective Fas-induced apoptosis in colon carcinoma cells. 1009 31
ETS1
, the founding member of Ets transcriptional factor family, plays an important role in cell proliferation, differentiation, lymphoid cell development, transformation, angiogenesis, and apoptosis. Previous work has shown that
ETS1
represses tumorigenicity of colon carcinoma cells in vivo, and that the p42-ETS1 protein bypasses a defect in apoptosis in colon carcinoma cells through the up-regulation of
caspase-1
expression. In this report, we show that expression of p42-
ETS1
inhibits tumorigenicity of colon cancer DLD-1 cells through induction of apoptosis in vivo. In support of the hypothesis that
caspase-1
might be a target involved in the sensitization of DLD-1 cells to Fas-induced apoptosis by
ETS1
, overexpression of
caspase-1
bypasses Fas-induced apoptosis in these cells as well. Furthermore,
ETS1
-mediated apoptosis was observed in MOP8 cells, a transformed mouse NIH3T3 cell line. To determine whether
ETS1
activates the transcription of
caspase-1
, luciferase reporters driven by the wild-type and mutant
caspase-1
promoters were generated. Both p51-
ETS1
and p42-
ETS1
transactivated the
caspase-1
transcription and a functional Ets binding site is identified in the
caspase-1
promoter. Wild-type
caspase-1
promoter (pGL3-
ICE
) was strongly transactivated by
ETS1
and this transactivation was dramatically diminished by the mutation of the potential Ets binding site (-525 bp). In addition, electrophoretic mobility shift assay and chromatin immunoprecipitation assay showed complex formation between this binding site and
ETS1
proteins. Taken together,
ETS1
transcriptionally induces the expression of
caspase-1
; as such, the regulatory control of
caspase-1
expression by
ETS1
may underlie the apoptotic susceptibility modulated by
ETS1
in specific tumor cells.
...
PMID:Caspase-1 is a direct target gene of ETS1 and plays a role in ETS1-induced apoptosis. 1610 71
