Gene/Protein
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Pivot Concepts:
Gene/Protein
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Target Concepts:
Gene/Protein
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Query: EC:2.7.11.31 (
AMP-activated protein kinase
)
13,065
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Colorectal cancer cells are unique in that they escape Fas-mediated cell death in the presence of Fas ligand, and we recently reported that
AMP-activated protein kinase
-related kinase 5 (ARK5) suppresses cell death signaling mediated by cell death receptor in Akt-dependent manner. In the current study, therefore, we examined whether ARK5 is involved in the escape from Fas-mediated cell death of colorectal cancer cells. Among 10 cell lines, ARK5 mRNA expression was observed in LoVo, SW480, and SW1116 cell lines. Interestingly, SW480 and SW1116 cell lines, but not LoVo cell line, showed expressions of both Fas ligand (FasL) and Fas mRNAs. SW620 cell line also showed FasL mRNA; however, Fas and ARK5 mRNAs were not detected. Furthermore, well-coincided expression among ARK5, FasL, and Fas mRNAs was observed in tumor tissues from patients with colorectal cancer, suggesting the suppression of FasL/Fas system-induced cell death by ARK5 in colorectal cancer cell lines. Intensive cell death, which was dependent on the FasL/Fas system was encountered when ARK5 antisense RNA (ARK5/AS) was introduced into SW480 cells. FLIP was expressed in only ARK5 mRNA-expressing cell lines, and ARK5/AS induced FLIP cleavage in a
caspase-6
-dependent manner. Amino-acid sequence analysis of
caspase-6
revealed two putative sites of phosphorylation by ARK5 at Ser80 and Ser257. Although active
caspase-6
overexpression induced cell death in SW480 and DLD-1 cell lines, SW480 cells, but not DLD-1 cells, exhibited strong resistance to procaspase-6 overexpression. Moreover, mutant
caspase-6
, in which the Ser257 was substituted by Ala (
caspase-6
/SA), induced cell death and FLIP degradation, even in SW480 cells. Active ARK5 was found to phosphorylate wild-type
caspase-6
in vitro, but not
caspase-6
/SA, and the prevented activation of
caspase-6
was promoted due to its phosphorylation by active ARK5 in vitro. On the basis of the results of this study, we propose that ARK5 negatively regulates procaspase-6 by phosphorylation at Ser257, leading to resistance to the FasL/Fas system.
...
PMID:Regulation of caspase-6 and FLIP by the AMPK family member ARK5. 1527 17
Liver cell death has an essential role in nonalcoholic steatohepatitis (NASH). The activity of the energy sensor adenosine monophosphate (AMP)-activated protein kinase (
AMPK
) is repressed in NASH. Liver-specific
AMPK
knockout aggravated liver damage in mouse NASH models.
AMPK
phosphorylated proapoptotic
caspase-6
protein to inhibit its activation, keeping hepatocyte apoptosis in check. Suppression of
AMPK
activity relieved this inhibition, rendering
caspase-6
activated in human and mouse NASH.
AMPK
activation or
caspase-6
inhibition, even after the onset of NASH, improved liver damage and fibrosis. Once phosphorylation was decreased,
caspase-6
was activated by caspase-3 or -7. Active
caspase-6
cleaved Bid to induce cytochrome c release, generating a feedforward loop that leads to hepatocyte death. Thus, the
AMPK
-
caspase-6
axis regulates liver damage in NASH, implicating
AMPK
and
caspase-6
as therapeutic targets.
...
PMID:An AMPK-caspase-6 axis controls liver damage in nonalcoholic steatohepatitis. 3207 35
Salsalate, an ester formed by 2 salicylic acid molecules, has beneficial effect against metabolic disorders in clinical trials and in animal studies. This study focused on the mechanistic aspects of salsalate activity against non-alcoholic fatty liver disease (NAFLD). Using high-fat diet (HFD) fed mice, we showed that salsalate treatment decreased body-weight gains, reduced white adipose tissue mass and improved glycaemic control. Mice in salsalate-treated group also had reduced obese adipose tissue and hepatic macrophage infiltration and inflammation and adipogenesis gene expression. Histology analysis revealed predominant decreases in hepatosteatosis, including both macrovesicular and microvesicular steatoses. The treatment reversed
AMPK
activity repression that was accompanied by reduced
caspase-6
activity and cleavage. Enzymatic assay and cell culture studies showed that salsalate promoted
AMPK
activation by directly activating
AMPK
. This study links salsalate effect against metabolic disorders to its activity on reversion of
AMPK
repression in NAFLD mice and on suppression of adipogenic gene induction.
...
PMID:Salsalate reverses metabolic disorders in a mouse model of non-alcoholic fatty liver disease through AMPK activation and caspase-6 activity inhibition. 3320 May 49
