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Query: UMLS:C0038187 (
starvation
)
24,951
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The process of autophagy has been described in detail at the molecular level in normal cells, but less is known of its regulation in cancer cells. Aplasia Ras homolog member I (ARHI;
DIRAS3
) is an imprinted tumor suppressor gene that is downregulated in multiple malignancies including ovarian cancer. Re-expression of ARHI slows proliferation, inhibits motility, induces autophagy and produces tumor dormancy. Our previous studies have implicated autophagy in the survival of dormant ovarian cancer cells and have shown that ARHI is required for autophagy induced by
starvation
or rapamycin treatment. Re-expression of ARHI in ovarian cancer cells blocks signaling through the PI3K and Ras/MAP pathways, which, in turn, downregulates mTOR and initiates autophagy. Here we show that ARHI is required for autophagy-meditated cancer cell arrest and ARHI inhibits signaling through PI3K/AKT and Ras/MAP by enhancing internalization and degradation of the epidermal growth factor receptor. ARHI-mediated downregulation of PI3K/AKT and Ras/ERK signaling also decreases phosphorylation of FOXo3a, which sequesters this transcription factor in the nucleus. Nuclear retention of FOXo3a induces ATG4 and MAP-LC3-I, required for maturation of autophagosomes, and also increases the expression of Rab7, required for fusion of autophagosomes with lysosomes. Following the knockdown of FOXo3a or Rab7, autophagolysosome formation was observed but was markedly inhibited, resulting in numerous enlarged autophagosomes. ARHI expression correlates with LC3 expression and FOXo3a nuclear localization in surgical specimens of ovarian cancer. Thus, ARHI contributes to the induction of autophagy through multiple mechanisms in ovarian cancer cells.
...
PMID:ARHI (DIRAS3) induces autophagy in ovarian cancer cells by downregulating the epidermal growth factor receptor, inhibiting PI3K and Ras/MAP signaling and activating the FOXo3a-mediated induction of Rab7. 2476 29
DIRAS3
is an imprinted tumor suppressor gene that is downregulated in 60% of human ovarian cancers. Re-expression of
DIRAS3
at physiological levels inhibits proliferation, decreases motility, induces autophagy, and regulates tumor dormancy. Functional inhibition of autophagy with choroquine in dormant xenografts that express
DIRAS3
significantly delays tumor regrowth after
DIRAS3
levels are reduced, suggesting that autophagy sustains dormant ovarian cancer cells. This study documents a newly discovered role for
DIRAS3
in forming the autophagosome initiation complex (AIC) that contains BECN1, PIK3C3, PIK3R4, ATG14, and
DIRAS3
. Participation of BECN1 in the AIC is inhibited by binding of BECN1 homodimers to BCL2.
DIRAS3
binds BECN1, disrupting BECN1 homodimers and displacing BCL2. Binding of
DIRAS3
to BECN1 increases the association of BECN1 with PIK3C3 and ATG14, facilitating AIC activation. Amino acid
starvation
of cells induces
DIRAS3
expression, reduces BECN1-BCL2 interaction and promotes autophagy, whereas
DIRAS3
depletion blocks amino acid
starvation
-induced autophagy. In primary ovarian cancers, punctate expression of
DIRAS3
, BECN1, and the autophagic biomarker MAP1LC3 are highly correlated (P<0.0001), underlining the clinical relevance of these mechanistic studies. Punctate expression of
DIRAS3
and MAP1LC3 was detected in only 21-23% of primary ovarian cancers but in 81-84% of tumor nodules found on the peritoneal surface at second-look operations following primary chemotherapy. This reflects a 4-fold increase (P<0.0001) in autophagy between primary disease and post-treatment recurrence. We suggest that
DIRAS3
not only regulates the AIC, but induces autophagy in dormant, nutrient-deprived ovarian cancer cells that remain after conventional chemotherapy, facilitating their survival.
...
PMID:DIRAS3 regulates the autophagosome initiation complex in dormant ovarian cancer cells. 2487 54
Autophagy can protect cancer cells from acute
starvation
and enhance resistance to chemotherapy. Previously, we reported that autophagy plays a critical role in the survival of dormant, drug resistant ovarian cancer cells using human xenograft models and correlated the up-regulation of autophagy and
DIRAS3
expression in clinical samples obtained during "second look" operations.
DIRAS3
is an imprinted tumor suppressor gene that encodes a 26 kD GTPase with homology to RAS that inhibits cancer cell proliferation and motility. Re-expression of
DIRAS3
in ovarian cancer xenografts also induces dormancy and autophagy.
DIRAS3
can bind to Beclin1 forming the Autophagy Initiation Complex that triggers autophagosome formation. Both the N-terminus of
DIRAS3
(residues 15-33) and the switch II region of
DIRAS3
(residues 93-107) interact directly with BECN1. We have identified an autophagy-inhibiting peptide based on the switch II region of
DIRAS3
linked to Tat peptide that is taken up by ovarian cancer cells, binds Beclin1 and inhibits
starvation
-induced
DIRAS3
-mediated autophagy.
...
PMID:DIRAS3-Derived Peptide Inhibits Autophagy in Ovarian Cancer Cells by Binding to Beclin1. 3100 88
Failure to cure ovarian cancer relates to the persistence of dormant, drug-resistant cancer cells following surgery and chemotherapy. "Second look" surgery can detect small, poorly vascularized nodules of persistent ovarian cancer in ~50% of patients, where >80% are undergoing autophagy and express
DIRAS3
. Autophagy is one mechanism by which dormant cancer cells survive in nutrient poor environments.
DIRAS3
is a tumor suppressor gene downregulated in >60% of primary ovarian cancers by genetic, epigenetic, transcriptional and post-transcriptional mechanisms, that upon re-expression can induce autophagy and dormancy in a xenograft model of ovarian cancer. We examined the expression of
DIRAS3
and autophagy in ovarian cancer cells following nutrient deprivation and the mechanism by which they are upregulated. We have found that
DIRAS3
mediates autophagy induced by amino acid
starvation
, where nutrient sensing by mTOR plays a central role. Withdrawal of amino acids downregulates mTOR, decreases binding of E2F1/4 to the
DIRAS3
promoter, upregulates
DIRAS3
and induces autophagy. By contrast, acute amino acid deprivation did not affect epigenetic regulation of
DIRAS3
or expression of miRNAs that regulate
DIRAS3
. Under nutrient poor conditions
DIRAS3
can be transcriptionally upregulated, inducing autophagy that could sustain dormant ovarian cancer cells.
...
PMID:Amino Acid Deprivation-Induced Autophagy Requires Upregulation of DIRAS3 through Reduction of E2F1 and E2F4 Transcriptional Repression. 3105 66
