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Query: UMLS:C0699790 (
colon cancer
)
28,837
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
A synthetic prostaglandin E1 (PGE1) analogue, misoprostol, was investigated for its effects on the growth of
colon cancer
in two in vivo models. Human
colon cancer
cell lines C170, LIM2412 and LIM2405 were grown as subcutaneous xenografts on T-lymphocyte deficient
ARC
(s) nu/nu mice. Tumour volumes were found to be significantly inhibited compared with control in misoprostol-treated animals with two cell lines. C170 was inhibited by 70.5% (P = 0.0001) and LIM2412 by 68.2% (P = 0.01). LIM2405 was inhibited by 33% (P = 0.14) which was not significantly different from the control. In a second experiment, colon cancers were induced in Sprague-Dawley rats using 1,2 dimethyl-hydrazine (DMH). After 10 weeks of treatment, rats were randomized to receive a 5 week course of 20 micrograms/kg per day of oral misoprostol. Misoprostol-treated rats were found to have a similar tumour incidence and staging compared with control animals. Oral administration of misoprostol has an inhibitory effect on early tumour growth of some colonic cancers, but not on established tumours.
...
PMID:The effect of misoprostol on colon cancer. 811
Recently, we identified a nucleoside analog named
ARC
(4-amino-6-hydrazino-7-beta-D-ribofuranosyl-7H-Pyrrolo[2,3-d]pyrimidine-5-carboxamide), which has the properties of a general transcriptional inhibitor. Here, we report the characterization of
ARC
on a panel of colorectal cancer (CRC) cell lines. Cell death induced by
ARC
in CRC cells was accompanied by caspase-3 cleavage and correlated with the downregulation of antiapoptotic proteins, survivin and Mcl-1 and with the inhibition of Akt phosphorylation. At the same time,
colon cancer
cell lines were resistant to the well-known nucleoside analog DRB (5,6-dichloro-1-beta-D-ribofuranosylbenzimidazole), which failed to downregulate Mcl-1 or survivin. Overall,
ARC
could represent an attractive candidate for anti-cancer drug development that targets multiple survival pathways in
colon cancer
cells.
...
PMID:Differential sensitivity of human colon cancer cell lines to the nucleoside analogs ARC and DRB. 1799 11
The ability of cells to escape apoptosis is critical for carcinogenesis as well as resistance to radiation and chemotherapy.
ARC
(Apoptosis Repressor with CARD (caspase recruitment domain)) is an unusual inhibitor of apoptosis in that it antagonizes both the extrinsic (death receptor) and intrinsic (mitochondrial/ER) apoptosis pathways.
ARC
is expressed predominantly in terminally differentiated cells such as cardiac and skeletal myocytes and neurons. Recently, however, the abundance of
ARC
was noted to be markedly increased in the epithelium of primary human breast cancers compared with benign breast tissue and to confer chemo- and radiation-resistance. Whether the induction of
ARC
is specific to breast cancer or a more general feature of neoplasia remains unknown. In this study, we assessed the abundance and subcellular localization of
ARC
in 21 human
colon cancer
cell lines and in 44 primary human colon adenocarcinomas and adjacent benign colonic tissue.
ARC
was present at high levels in most
colon cancer
cell lines and in almost all primary colon cancers compared with corresponding controls. Levels of
ARC
in the cytoplasm were increased in well, moderately, and poorly differentiated cancers compared with benign tissue, while levels of nuclear
ARC
were increased only in moderately differentiated tumors. Moreover, epithelial cancers of the ovary and cervix exhibited increased
ARC
abundance compared with controls. These results demonstrate that
ARC
is a novel marker of human
colon cancer
and suggest that it may be a general feature of epithelial cancers.
...
PMID:ARC (apoptosis repressor with caspase recruitment domain) is a novel marker of human colon cancer. 1846 22
Cancer cells in poorly vascularized solid tumors are constantly or intermittently exposed to stressful microenvironments, including glucose deprivation, hypoxia, and other forms of nutrient starvation. These tumor-specific conditions, especially glucose deprivation, activate a signaling pathway called the unfolded protein response (UPR), which enhances cell survival by induction of the stress proteins. We have established a screening method to discover anticancer agents that could preferentially inhibit tumor cell viability under glucose-deprived conditions. Here we identify arctigenin (ARC-G) as an active compound that shows selective cytotoxicity and inhibits the UPR during glucose deprivation. Indeed,
ARC
-G blocked expression of UPR target genes such as phosphorylated-PERK, ATF4, CHOP, and GRP78, which was accompanied by enhanced phosphorylation of eIF2 alpha during glucose deprivation. The UPR inhibition led to apoptosis involving a mitochondrial pathway by activation of caspase-9 and -3. Furthermore,
ARC
-G suppressed tumor growth of
colon cancer
HT-29 xenografts. Our results demonstrate that
ARC
-G can be served as a novel type of antitumor agent targeting the UPR in glucose-deprived solid tumors.
...
PMID:Arctigenin blocks the unfolded protein response and shows therapeutic antitumor activity. 2023
Inhibition of apoptosis is critical for carcinogenesis.
ARC
(apoptosis repressor with caspase recruitment domain) is an endogenous inhibitor of apoptosis that antagonizes both intrinsic and extrinsic apoptosis pathways. Although normally expressed in striated myocytes and neurons,
ARC
is markedly induced in a variety of primary human epithelial cancers and renders cancer cells resistant to killing. The mechanisms that mediate the induction of
ARC
in cancer are unknown. Herein we demonstrate that increases in
ARC
abundance are stimulated by Ras through effects on transcription and protein stability. Overexpression of activated N-Ras or H-Ras in normal cells is sufficient to increase
ARC
mRNA and protein levels. Similarly, transgenic expression of activated H-Ras induces
ARC
in both the normal mammary epithelium and resulting tumors of intact mice. Conversely, knockdown of endogenous N-Ras in breast and
colon cancer
cells significantly reduces
ARC
mRNA and protein levels. The promoter of the Nol3 locus, encoding
ARC
, is activated by N-Ras and H-Ras in a MEK/ERK-dependent manner. Ras also stabilizes
ARC
protein by suppressing its polyubiquitination and subsequent proteasomal degradation. In addition to the effects of Ras on
ARC
abundance,
ARC
mediates Ras-induced cell survival and cell cycle progression. Thus, Ras induces
ARC
in epithelial cancers, and
ARC
plays a role in the oncogenic actions of Ras.
...
PMID:Induction of the apoptosis inhibitor ARC by Ras in human cancers. 2039 91
