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Target Concepts:
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Query: UMLS:C0019204 (
hepatocellular carcinoma
)
71,386
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
METTL3 is an RNA methyltransferase implicated in the control of cell differentiation and proliferation in embryonic development and cancer. The current study was aimed to explore the function and underlying mechanism of METTL3 in
hepatocellular carcinoma
(
HCC
). We evaluated the expression and prognostic significance of METTL3 in 100
HCC
cases and TCGA dataset. In
HCC
cases, both the RNA and protein expression of METTL3 were significantly upregulated and associated with poor prognosis. Gene set enrichment analysis of transcriptional profiles in
HCC
specimens revealed that METTL3 expression was associated with impaired glucose metabolism and mTOR signal pathway. In Huh-7 and SMMC-7721
HCC
cells, downregulation of METTL3 by siRNA interference inhibited glycolytic capacity, which was proved by the decreased intracellular glucose uptake and lactate production. In terms of mechanism, we found mTORC1 activity was impaired by downregulation of METTL3, additional silencing of METTL3 cannot further decrease the phosphorylation level of mTORC1 and glycolysis activity in
Rapamycin
-treated
HCC
cells. At last, we observed that downregulation of METTL3 synergizes with the glycolysis inhibitor 2-deoxyglucose (2-DG) to inhibit tumor growth in vitro. Our study provided evidence that METTL3 is involved in the regulation of glycolysis activity in
HCC
, suggesting that suppression of glycolysis via METTL3 inhibition was a potential treating strategy against
HCC
.
...
PMID:METTL3 expression is associated with glycolysis metabolism and sensitivity to glycolytic stress in hepatocellular carcinoma. 3206 77
Sirolimus
(
SRL
) has been reported to benefit patients undergoing liver transplantation (LT) for
hepatocellular carcinoma
(
HCC
). This study aimed to compare
SRL
with tacrolimus (TAC) in living-donor LT (LDLT) recipients beyond the Milan criteria. This study was initially designed to enrol 45 recipients who underwent LDLT for
HCC
beyond the Milan criteria. At 1 month after LT, the patients were randomly assigned to either
SRL
or TAC-based treatment, with both groups receiving mycophenolate mofetil. The primary outcome was three-year recurrence-free survival (RFS) and the secondary outcome was overall survival (OS). A total of 42 patients completed the study.
HCC
recurrence occurred in 8 of 22 (36.4%) patients in the
SRL
group and in 5 of 22 (25%) patients in the TAC group. No differences in RFS and OS were found between the two groups in simple comparison. The type of immunosuppressant remained a nonsignificant factor for recurrence in multivariate analysis; however,
SRL
significantly prolonged OS (TAC hazard ratio: 15 [1.3-172.85],
p
= 0.03) after adjusting for alpha-fetoprotein and positron emission tomography standardised uptake value ratio (tumour/background liver). In conclusion,
SRL
does not decrease
HCC
recurrence but prolongs OS after LDLT for
HCC
beyond the Milan criteria.
...
PMID:Sirolimus Prolongs Survival after Living Donor Liver Transplantation for Hepatocellular Carcinoma Beyond Milan Criteria: A Prospective, Randomised, Open-Label, Multicentre Phase 2 Trial. 3305 49
Hepatocellular carcinoma
(
HCC
) is a deadly form of liver malignancy with limited treatment options. Amplification and/or overexpression of
c-MYC
is one of the most frequent genetic events in human
HCC
. The mammalian target of
Rapamycin
Complex 1 (mTORC1) is a major functional axis regulating various aspects of cellular growth and metabolism. Recently, we demonstrated that mTORC1 is necessary for c-Myc driven hepatocarcinogenesis as well as for
HCC
cell growth in vitro. Among the pivotal downstream effectors of mTORC1, upregulation of Fatty Acid Synthase (FASN) and its mediated de novo lipogenesis is a hallmark of human
HCC
. Here, we investigated the importance of FASN on c-Myc-dependent hepatocarcinogenesis using in vitro and in vivo approaches. In mouse and human
HCC
cells, we found that FASN suppression by either gene silencing or soluble inhibitors more effectively suppressed proliferation and induced apoptosis in the presence of high c-MYC expression. In c-Myc/Myeloid cell leukemia 1 (MCL1) mouse liver tumor lesions, FASN expression was markedly upregulated. Most importantly, genetic ablation of
Fasn
profoundly delayed (without abolishing) c-Myc/MCL1 induced
HCC
formation. Liver tumors developing in c-Myc/MCL1 mice depleted of
Fasn
showed a reduction in proliferation and an increase in apoptosis when compared with corresponding lesions from c-Myc/MCL1 mice with an intact
Fasn
gene. In human
HCC
samples, a significant correlation between the levels of c-MYC transcriptional activity and the expression of
FASN
mRNA was detected. Altogether, our study indicates that FASN is an important effector downstream of mTORC1 in c-MYC induced
HCC
. Targeting FASN may be helpful for the treatment of human
HCC
, at least in the tumor subset displaying c-MYC amplification or activation.
...
PMID:Pivotal Role of Fatty Acid Synthase in c-MYC Driven Hepatocarcinogenesis. 3318 30
Studies on effective immunosuppressive strategies for the management of patients undergoing a liver transplantation (LT) due to
hepatocellular carcinoma
(
HCC
) are limited. In the present study, immunosuppressive candidates predicted to exhibit beneficial immunosuppressive and tumor-suppressive effects in patients with
HCC
were assessed using Huh7 and HEP3B
HCC
cells, which have high proportions of CD133+EpCAM+ cancer stem cell (CSC) populations. The immunosuppressants assessed were sirolimus, tacrolimus, cyclosporine A and mycophenolate mofetil (MMF), and their activities were assessed on CSCs.
Sirolimus
and MMF reduced the proliferation of Huh7 and HEP3B cells; however, the proportion of CD133+EpCAM+ was notably increased in treated Huh7 cells.
Sirolimus
treatment alone resulted in G0-G1 cell cycle arrest at all doses in all Huh7 and CD133-EpCAM- populations; however, CD133+EpCAM+ populations showed only slight G1 arrest at higher doses only. In contrast, S-phase arrest was induced at all doses in the Huh7, CD133-EpCAM- and CD133+EpCAM+ populations by MMF.
Sirolimus
and MMF effectively reduced the proliferation of Huh7 and HEP3B cells, but did not exert a notable effect on the CD133+EpCAM+ cells. Therefore, therapeutic strategies utilizing
Sirolimus
and MMF should be further studied
in vivo
for regulation of CSC populations in order to reduce
HCC
recurrence rates.
...
PMID:Sirolimus and MMF are insufficient immunosuppressants for regulation of the proliferation of CD133+EpCAM+ cell populations in HCC cell lines. 3319 93
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