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Target Concepts:
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Query: UMLS:C0345904 (
liver cancer
)
15,188
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Our team was at the origin of the discovery of the relationship between rearrangements in genes encoding the retinoic acid receptors and tumorigenesis in human. Studying the molecular basis for hepatitis B virus (HBV)-associated
liver cancer
, we demonstrated that the viral DNA can behave as an insertional mutagen. This work also led to the identification of the first gene (RAR beta) encoding a receptor for the active derivative of vitamin A, retinoid acid. In collaboration with L. Degos, we then demonstrated the existence a systematic alteration of another retinoic acid receptor, RAR alpha, in acute promyelocytic leukemia (APL). Most recent work allowed us to involve a novel subnuclear organelle, the so-called
PML
Nuclear Bodies, in APL pathogenesis, underlying the major role played by the functional organization of the nucleus both in the normal and the pathological cell.
...
PMID:[Retinoic acid nuclear receptors: a common molecular basis for liver cancer and acute promyelocytic leukemia]. 1241 72
IFNs are pleiotropic cytokines that have been shown to be important regulators of cell growth. IFN-alpha has recently been recognized to harbor therapeutic potential in prevention and treatment of hepatocellular carcinoma (HCC). However, HCC cells respond differentially to IFN treatment, the mechanism of which is largely unknown. To address this issue, we analyzed the effect of IFN-alpha on different liver tumor cell lines. We found that growth inhibiting effects of IFN-alpha in hepatoma cells require
PML
-NB induction and, moreover, tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) expression on the mRNA and protein level. RNAi silencing of
PML
down-regulates TRAIL expression in hepatoma cells and correspondingly blocks IFN-alpha-induced apoptosis. In addition,
PML
-deficient primary hepatocytes fail to up-regulate TRAIL upon IFN-alpha-treatment in contrast to their wild-type counterparts. These data identify TRAIL as a novel downstream transcriptional target of
PML
-mediated apoptosis in hepatomas and suggest that
PML
and TRAIL play important roles in IFN-regulated apoptosis in HCC. Furthermore, the mechanism is independent of the p53 status of the tumor cells. In summary, our results identify central molecules mediating IFN-alpha induced apoptosis in liver tumors, shed light on the differential response of hepatoma cells to IFN exposure and, thus, may contribute to an efficient application of this substance in the treatment of
liver cancer
.
...
PMID:IFN-alpha-induced apoptosis in hepatocellular carcinoma involves promyelocytic leukemia protein and TRAIL independently of p53. 1914 42
DNA damage response and repair pathways are important barriers to carcinogenesis. Here, we show that promyelocytic leukaemia (
PML
, also known as TRIM19), involved in sensing DNA damage and executing homologous recombination repair, is down-regulated in non-tumour liver cells surrounding hepatitis B virus (HBV)-related hepatocellular carcinoma (HCC). No
PML
mutation or deletion was found in HBV-infected liver or HCC cells. Immunohistochemical analysis of liver biopsies from patients with breast or
liver cancer
and HBV reactivation after chemotherapy revealed
PML
up-regulation and HBV exacerbation in normal liver tissue in response to DNA damage (functional
PML
),
PML
down-regulation in HCC peritumour cells associated with high HBsAg accumulation and low HBV replication activity (suppressive
PML
), and heterogeneous nuclear
PML
expression in HCC cells that lost HBV DNA and HBsAg and were non-reactive to DNA damage (dysregulated
PML
). Loss of
PML
in HBsAg-transgenic mice promoted chromosome breaks in liver cells and accelerated the accumulation of body and liver fat and the development of a liver steatosis-dysplasia-adenoma-carcinoma sequence in an inflammation-independent and male-predominant manner, compared to
PML
knock-out or HBsAg-transgenic mice during the same time period. These results indicate that
PML
deficiency facilitates genomic instability and promotes HBsAg-related hepatocarcinogenesis, which also involves androgen and lipid metabolism. These findings uncover a novel
PML
link between HBV-related tumourigenesis, DNA repair, and metabolism.
...
PMID:Promyelocytic leukaemia protein links DNA damage response and repair to hepatitis B virus-related hepatocarcinogenesis. 2362 81
Cancer stem cells (CSCs) can form new tumors and contribute to post-operative recurrence and metastasis. We showed that CD133
+
CD13
+
hepatocytes isolated from HuH7 cells and primary
HCC
cells display biochemical and functional characteristics typical of CSCs, suggesting that CD133
+
CD13
+
hepatocytes in primary
HCC
tumors function as CSCs. We also found that arsenite treatment reduced the viability and stemness of CD133
+
CD13
+
hepatocytes, enhanced the sensitivity of HuH7 cells to pirarubicin, and reduced the tumorigenicity of CD133
+
CD13
+
hepatocytes xenografts in mice. The effects of sodium arsenite treatment in CD133
+
CD13
+
hepatocytes were mediated by the post-transcriptional suppression of
PML
expression and the inhibition of Oct4, Sox2, and Klf4 expression at the transcriptional level. Incomplete rescue of Oct4 expression in arsenic-treated cells ectopically expressing an siRNA-resistant
PML
transcript suggested that OCT4 regulation in liver CSCs involves other factors in addition to
PML
. Our findings provide evidence of a specific role for
PML
in regulating Oct4 levels in liver CSCs and highlight the clinical importance of arsenic for improving the efficacy of other chemotherapeutic agents and the prevention of post-operative
HCC
recurrence and metastasis.
...
PMID:Arsenite inhibits the function of CD133
+
CD13
+
liver cancer stem cells by reducing PML and Oct4 protein expression. 2751 64
