Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
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Drug
Enzyme
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Query: UMLS:C1864663 (
HCC
)
2,985
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Clusterin (CLU) is a stress-activated chaperone, which plays an important role in cancer development and progression through promoting cell survival. However, the exact mechanism of how CLU exerts its cell protective role under ER stress condition is still unclear. Therefore, in order to explore the molecular mechanisms by which CLU inhibited ER stress-induced apoptosis,
HCC
cell lines were treated with tunicamycin (TN), an ER stress inducer. We found that the expressions of both CLU and
GRP78
were increased after TN treatment. Knockdown of CLU expression in SMMC7721 and HCCLM3 cells inhibited
GRP78
expression after TN treatment and enhanced ER stress-induced apoptosis, whereas over-expression of CLU in HepG2 cells increased
GRP78
expression after TN induction and abolished the effect of TN on cell apoptosis. Furthermore, knockdown of
GRP78
expression in CLU-HepG2 cells abrogated the protective role of CLU under ER stress condition. Co-immunoprecipitation (co-IP) and confocal microscopy experiments confirmed the direct interaction between CLU and
GRP78
under ER stress condition. The effect of CLU knockdown on
GRP78
expression and cell apoptosis in
HCC
tumors were further determined in orthotopic xenograft tumor model. Knockdown of CLU expression in HCCLM3 cells inhibited
GRP78
expression in tumor tissues, accompanied with increased number of apoptotic cancer cells. Moreover, the correlation between CLU and
GRP78
expression was further determined in clinical
HCC
specimens. Taken together, these findings reveal that CLU protects
HCC
cells from ER stress induced apoptosis at least partially through interacting with
GRP78
.
...
PMID:Clusterin protects hepatocellular carcinoma cells from endoplasmic reticulum stress induced apoptosis through GRP78. 2345 89
5-FU is a common first-line chemotherapeutic drug for the treatment of hepatocellular carcinoma. However the development of acquired resistance to 5-FU confines its clinical usages. Although this phenomenon has been the subject of intense investigation, the exact mechanism of acquired resistance to 5-FU remains elusive. Here, we report that over-expression of
GRP78
contributes to acquired resistance to 5-FU in
HCC
by up-regulating the c-Src/LSF/TS axis. Moreover, we found that the resistance to 5-FU conferred by
GRP78
is mediated by its ATPase domain. The ATPase domain differentially increased the expression of LSF, TS and promoted the phosphorylation of ERK and Akt. We further identified that
GRP78
interacts physically with c-Src through its ATPase domain and promotes the phosphorylation of c-Src, which in turn increases the expression of LSF in the nucleus. Together,
GRP78
confers the resistance to 5-FU by up-regulating the c-Src/LSF/TS axis via its ATPase domain.
...
PMID:GRP78 confers the resistance to 5-FU by activating the c-Src/LSF/TS axis in hepatocellular carcinoma. 2637 40
Acquired resistance is a common phenomenon for
HCC
patients who undergone sorafenib treatment, however the mechanism by which acquired resistance develops remains elusive. In this study, we found that
GRP78
could be detected in the serum samples of
HCC
patients and the conditional medium of multiple
HCC
cell lines, suggesting that
GRP78
is secreted by
HCC
cells. Further studies showed that secreted
GRP78
facilitated the proliferation and inhibited the apoptosis induced by sorafenib both in
HCC
cell lines and in tumor xenografts. We further found that secreted
GRP78
could interact physically with EGFR, therefore activates EGFR signaling pathway. knockdown of EGFR decreased secreted
GRP78
induced phosphorylation of SRC and STAT3. By contrast, overexpression of EGFR further enhanced the phosphorylation of SRC and STAT3 induced by secreted
GRP78
, suggesting the critical role of EGFR in secreted
GRP78
conferred resistance to sorafeinib. Moreover, inhibition of SRC by PP2 antagonized the resistance to sorafenib and inhibited the activation of STAT3 conferred by secreted
GRP78
. Taken together, our results showed that secreted
GRP78
could interact with EGFR, activate EGFR-SRC-STAT3 signaling, conferring the resistance to sorafenib.
...
PMID:Secreted GRP78 activates EGFR-SRC-STAT3 signaling and confers the resistance to sorafeinib in HCC cells. 2842 13
The cancer stem cells (CSCs) theory recently became a focus of heightened attention in cancer biology, with the proposition that CSCs may constitute an important therapeutic target for effective anticancer therapy, because of their demonstrated role in tumor initiation, chemo-, and radio-resistance. Liver CSCs are a small subpopulation of poorly- or undifferentiated liver tumor cells, implicated in tumorigenesis, metastasis, resistance to therapy and disease relapse, enriched with and associated with the functional markers corresponding to the CSCs-enriched side population (SP), high aldehyde dehydrogenase (ALDH) activity, and enhanced formation of in vitro liver CSCs models, referred to herein as hepatospheres. In this study, we found YAP1 was significantly expressed in the SP cells, as well as in generated hepatospheres compared to non-SP or parental
HCC
cells, at transcript and/or protein levels. In addition, downregulation of YAP1 expression levels by small molecule inhibitor and siRNA transfection, in the
HCC
cell lines, PLC/PRF/5 and Mahlavu, were associated with marked loss of ability to form hepatospheres and increased sensitivity to sorafenib. Consistent with the above, we demonstrated that YAP1 expression positively correlated with that of Sox2, Oct4, c-Myc and
GRP78
, markers of stemness and drug resistance. This is suggestive of YAP1's role as a modulator of cancer stemness, ER stress and chemoresistance. For the first time, we demonstrate that Ovatodiolide significantly attenuates YAP1 expression and subsequently suppressed YAP1-modulated CSCs phenotypes and associated disease progression, consistent with our previous finding in breast cancer. Taken together, our findings suggest that YAP1, highly expressed in malignant liver tumours, contributes to hepatocellular CSCs phenotype and is a molecular target of interest for CSCs targeted therapy in liver cancer patients.
...
PMID:Ovatodiolide suppresses yes-associated protein 1-modulated cancer stem cell phenotypes in highly malignant hepatocellular carcinoma and sensitizes cancer cells to chemotherapy in vitro. 2969 66
