Reduced survival of patients with hepatocellular carcinoma expressing hexokinase II

Gong, Lan; Cui, Zhuqingqing; Chen, Pengcheng; Han, Hui; Peng, Jie; Leng, Xi-sheng

doi:10.1007/s12032-011-9841-z

Cited by 56 publications

(41 citation statements)

References 31 publications

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“…The specimens were stained simultaneously under the same conditions, reducing the possibility that inter-batch differences in staining technique impacted the results. In contrast to previous works that reported HKII expression in only 45–56 % of samples [24, 25], the current study identified HKII expression in all 45 HCC specimens with an average value of 64.42 (±34.89) ppc/mm 2 . The differences between the results cannot be explained by variation in antibody or IHC methodology.…”

Section: Discussioncontrasting

confidence: 99%

“…Consistent with recent publications, we noted HKII immunoexpression was more pronounced in poorly differentiated, pleomorphic, and in higher stage HCC [23–25], thereby adding to the evidence that HKII is a likely marker for increased metabolic activity that occurs in HCC in humans. The potential use of HK II inhibitors for the treatment of advanced HCCs was described in a mouse tumor model [43], and the question remains whether HKII provides an attractive target for the development of new agents for the treatment of HCC in humans.…”

Section: Discussionsupporting

confidence: 92%

“…The expression of HKII in HCC cells distinguishes them from normal hepatocytes. Recent observations in humans have shown an association between increased HKII immuno-expression and higher HCC tumor grade, stage [23, 24], and poorer patient survival [24, 25]. However, it is not known when HKII expression becomes up-regulated in the sequence of hepatocarcinogenesis.…”

Section: Introductionmentioning

confidence: 99%

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Evidence for Heightened Hexokinase II Immunoexpression in Hepatocyte Dysplasia and Hepatocellular Carcinoma

et al. 2014

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Background Normal hepatocytes exhibit low-affinity hexokinase (glucokinase [HKIV]), but during oncogenesis, there is a switch from HKIV to HKII expression. The aims of this study were to compare the immunoexpression of HKII in non-dysplastic cirrhosis (NDC), liver cell change/dysplasia in cirrhosis (LCD), HCC, and normal liver control tissues, and to correlate HKII expression with clinical and histopathological parameters. Design Immunohistochemistry was performed on a liver cancer progression tissue array consisting of specimens from explants with cirrhosis, including 45 tissue samples with HCC, 108 without HCC, 143 with LCD, and 8 normal liver control tissues. HKII expression was quantified as positive pixel counts/square millimeter (ppc/mm2) by image analysis. Results There was a stepwise increase in HKII level from normal liver tissue to NDC, to LCD, and to HCC (p = 0.001). HKII levels were significantly higher in areas of LCD versus NDC (p ≤ 0.001), and in LCD and HCC versus NDC (p = 0.007). HKII levels were similar in LCD and HCC (p = 0.124). HKII levels were higher in grade 2–4 versus grade 1 HCCs (p = 0.044), and in pleomorphic versus non-pleomorphic HCC variants (p = 0.041). Higher levels of HKII expression in LCD and HCC versus NDC and in higher tumor grade remained significant in multivariate analysis. Conclusions Higher levels of HKII immunoexpression in LDC and HCC compared with NDC suggest that upregulation of HKII occurs during the process of hepatocarcinogenesis in humans. In HCC, higher levels of HKII are associated with more aggressive histological features.

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Section: Discussioncontrasting

confidence: 99%

Section: Discussionsupporting

confidence: 92%

Section: Introductionmentioning

confidence: 99%

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Evidence for Heightened Hexokinase II Immunoexpression in Hepatocyte Dysplasia and Hepatocellular Carcinoma

et al. 2014

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“…Silibinin dosedependently suppressed the expression of cortactin, CXCR4, GLI2, ID1, KIAA0101, mortalin, PAK1, RHOA, SPINK1, STAT3, and STMN1 in both cell types. The overexpression of these genes have been associated with cellular invasion and some serious life-threatening clinical features in HCC such as advanced histological grades, metastasis, and/or poor prognosis (19)(20)(21)(22)(23)(24)(25)(26)(27)(28)(29). In another aspect, ANGPT2 (overexpressed in HCC) and ID1 (in coordination with MMP-2) may induce angiogenesis in HCC, a hypervascular tumor (20,30).…”

Section: Discussionmentioning

confidence: 99%

Multitargeting and Antimetastatic Potentials of Silibinin in Human HepG-2 and PLC/PRF/5 Hepatoma Cells

Ghasemi¹,

Ghaffari²,

Momeny³

et al. 2013

Nutrition and Cancer

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Hepatocellular carcinoma (HCC) is the most common sort of primary liver malignancy with poor prognosis. This study aimed at examining the effects of silibinin (a putative antimetastatic agent) on some transcriptional markers mechanistically related to HCC recurrence and metastasis in HepG-2 [hepatitis B virus (HBV)-negative and P53 intact) and PLC/PRF/5 (HBV-positive and P53 mutated) cells. The expression of 27 genes in response to silibinin was evaluated by real-time RT-PCR. The MMP gelatinolytic assay and microculture tetrazolium test (MTT) were tested. Silibinin was capable of suppressing the transcriptional levels of ANGPT2, ATP6L, CAP2, CCR6, CCR7, CLDN-10, cortactin, CXCR4, GLI2, HK2, ID1, KIAA0101, mortalin, PAK1, RHOA, SPINK1, and STMN1 as well as the enzymatic activity of MMP-2 but promoted the transcripts of CREB3L3, DDX3X, and PROX1 in both cells. Some significant differences between the cells in response to silibinin were detected that might be related to the differences of the cells in terms of HBV infection and/or P53 mutation, suggesting the possible influence of silibinin on HCC through biological functions of these 2 prognostic factors. In conclusion, our findings suggest that silibinin could potentially function as a multitargeting antimetastatic agent and might provide new insights for HCC therapy particularly for HBV-related and/or P53-mutated HCCs.

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“…While this may seem to be a wasteful form of energy production for highly proliferative cells since glycolysis nets only 2 ATP while the process of oxygen-dependent energy generation nets 36 ATP molecules, the upregulation of glucose transporters (e.g., GLUT-1) that allows for an increase in glucose uptake, combined with an increase in enzymes that contribute to glycolysis such as phosphoglycerate kinase-1 (PGK-1), hexokinase (HK), and phosphofructokinase L (PFK-L) [55,56], may allow the glycolytic flux to be high enough for the ATP production to match the seemingly more efficient ETC and coupled OXPHOS [57]. This upregulation of glycolytic metabolism participants has been correlated to poor prognosis in a variety of cancer types [58][59][60][61].…”

Section: Glucose Metabolismmentioning

confidence: 99%

Regulation of Cancer Cell Metabolism by Hypoxia

Pulkoski‐Gross

Evensen

Cao

2014

Cancer Drug Discovery and Development

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The growth of a tumor usually results in the development of hypoxia, which is primarily a consequence of the tumor outgrowing existing vasculature and the disorganized nature of vascular growth induced by the tumor itself. The low oxygen tension at the site of neoplastic growth has a significant effect on the metabolic status of the cells involved. In order for the cells to survive the harsh conditions of low oxygen and nutrition, the metabolism of the cell switches from an aerobic type of metabolism to an anaerobic one, relying primarily on glycolysis for the production of energy and metabolic intermediates that feed various biosynthetic pathways. Because this phenotype is associated with increased cell survival, drug resistance, and ultimately poor patient prognosis, the metabolic components and the mediators of the hypoxic response are viable targets in the war on cancer. Currently, a variety of drugs are being explored that influence the mediators of the hypoxic response, such as hypoxia-inducible factor-1 (HIF-1), and those that target metabolic enzymes directly. These agents show promise in improving the current standard of care by acting in a synergistic manner with current cancer therapies.

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Reduced survival of patients with hepatocellular carcinoma expressing hexokinase II

Cited by 56 publications

References 31 publications

Evidence for Heightened Hexokinase II Immunoexpression in Hepatocyte Dysplasia and Hepatocellular Carcinoma

Evidence for Heightened Hexokinase II Immunoexpression in Hepatocyte Dysplasia and Hepatocellular Carcinoma

Multitargeting and Antimetastatic Potentials of Silibinin in Human HepG-2 and PLC/PRF/5 Hepatoma Cells

Regulation of Cancer Cell Metabolism by Hypoxia

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