Hepatocellular glycogenotic foci after combined intraportal pancreatic islet transplantation and knockout of the carbohydrate responsive element binding protein in diabetic mice

Ribback, Silvia; Sonke, Jenny; Löhr, Andrea; Frohme, Josephine; Peters, Kristin; Holm, J; Peters, Michele; Cigliano, Antonio; Calvisi, Diego F.; Dombrowski, Frank

doi:10.18632/oncotarget.22234

Cited by 7 publications

(10 citation statements)

References 43 publications

(69 reference statements)

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“…They reported that ChREBP binding is enriched in pathways involved in insulin signaling, adherent junctions and cancer, suggesting a novel involvement of ChREBP in tumorigenesis and cancer progression. Further, a recent study reported the importance of ChREBP in hepatocellular carcinoma (HCC) (Ribback et al, 2017). The authors found that genetic deletion of ChREBP (in ChREBP KO mice) impaired hepatocarcinogenesis driven by protein kinase B/Akt overexpression in mice.…”

Section: Activation Of Chrebp By Glucose Metabolitesmentioning

confidence: 99%

Carbohydrate Sensing Through the Transcription Factor ChREBP

2019

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Carbohydrate response element binding protein (ChREBP) is a carbohydrate-signaling transcription factor that in the past years has emerged as a central metabolic regulator. ChREBP expression is mostly abundant in active sites of de novo lipogenesis including liver and white and brown adipose tissues. ChREBP is also expressed in pancreatic islets, small intestine and to a lesser extent in the kidney and the brain. In response to glucose, ChREBP undergoes several post-translational modifications (PTMs) (phosphorylation, acetylation and/or O -GlcNAcylation) that will either modulate its cellular location, stability and/or its transcriptional activity. ChREBPβ is a shorter isoform of ChREBP that was first described in adipose tissue and later found to be expressed in other sites including liver and pancreatic β cells. ChREBPβ lacks an important regulatory inhibitory domain, known as LID (low glucose inhibitory domain), in its N-terminal domain and is therefore reported as a highly active isoform. In this review, we recapitulate a recent progress concerning the mechanisms governing the activity of the ChREBP isoforms, including PTMs, partners/cofactors as well as novel metabolic pathways regulated by ChREBP in key metabolic tissues, by discussing phenotypes associated with tissue-specific deletion of ChREBP in knockout mice.

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Section: Activation Of Chrebp By Glucose Metabolitesmentioning

confidence: 99%

Carbohydrate Sensing Through the Transcription Factor ChREBP

2019

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“…In light of these previous findings, considerable efforts should be devoted to identify key metabolic candidates whose inactivation might severely impair hepatocarcinogenesis while sparing normal cells. Previously, it has been demonstrated that alterations of glucose and lipid metabolism in HCC of humans and rodents are paralleled by the strong upregulation of carbohydrate-responsive element binding protein (ChREBP) transcription factor [13,19,20]. Together with the sterol regulatory element binding protein-1c (SREBP-1c) gene, ChREBP is a major positive regulator of glucose and lipid metabolism in the liver [21][22][23][24][25].…”

Section: Introductionmentioning

confidence: 99%

Oncogene-dependent addiction to carbohydrate-responsive element binding protein in hepatocellular carcinoma

et al. 2018

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Metabolic reprogramming is a hallmark of many cancer types, including hepatocellular carcinoma (HCC). Identifying the critical players in this process might be crucial for the generation of novel and effective anti-neoplastic therapies. In the present investigation, we determined the importance of carbohydrate responsive element binding protein (ChREBP), a central player in the regulation of lipid and glucose metabolism in the liver, on the development of HCC in in vitro and in vivo models. We found that genetic deletion of ChREBP (that will be referred to as ChREBPKO mice) strongly delays or impairs hepatocarcinogenesis driven by AKT or AKT/c-Met overexpression in mice, respectively. In contrast, HCC development was found to be completely unaffected by ChREBP depletion in mice co-expressing AKT and N-Ras protooncogenes. In mouse and human HCC cell lines, suppression of ChREBP via specific small interfering RNAs (siRNAs) resulted in decreased proliferation and induction of apoptosis. Of note, these cellular events were strongly augmented by concomitant inhibition of the mitogen-activated protein kinase (MAPK) pathway. The present data indicate that ChREBP activity might be required or dispensable for HCC growth, depending on the oncogenes involved. In particular, the activation of Ras/MAPK signaling might represent a possible mechanism of resistance to ChREBP depletion in this tumor type. Additional studies are needed to unravel the molecular mechanisms rendering HCC cells insensitive to ChREBP suppression.

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“…Specifically, we found an increased glycogen storage, reduced glucose-6-phosphatase activity and upregulated enzymes of glycolysis and de novo lipogenesis, beta-oxidation as well as overexpression of the insulin receptor and activated AKT/mTOR and Ras/MAPK pathways in CCF from both human livers and the rat model [20]. Similiarly, in the mouse, hepatocarcinogenesis is associated with activation of the insulin/AKT/mTOR signaling pathway, the transcriptional regulator ChREBP [16,21], as well as the lipogenic pathway [18,22,23]. Although these data hint to several pathways and regulators, a comprehensive inventory of gene and protein expression in human CCF is missing.…”

Section: Introductionmentioning

confidence: 76%

Transcriptomic and Proteomic analysis of clear cell foci (CCF) in the human non-cirrhotic liver identifies several differentially expressed genes and proteins with functions in cancer cell biology and glycogen metabolism

Metzendorf

Wineberger

Rausch

et al. 2020

Preprint

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Clear cell foci (CCF) of the liver are considered to be pre-neoplastic lesions of hepatocellular adenomas and carcinomas. They are hallmarked by glycogen-overload and activation of AKT/mTOR-signaling. Here we report the transcriptome and proteome of CCF extracted from human liver biopsies by laser capture microdissection. We mainly found genes and proteins with lower expression in CCF compared to control samples. Of 14 differentially expressed transcripts only 3 were overexpressed and belong to previously uncharacterized long non-coding RNAs. At the protein level, 3 proteins were at least 1.5-fold higher expressed in CCF than in control samples, while 22 proteins were at least 1.5-fold less abundant. Using immunohistochemistry, the reduced expressions of STBD1, USP28, monad/WDR92, CYB5B and HSPE1 were validated in CCF. Knockout of STBD1, the gene coding for Starch-binding domain-containing protein 1, in mice did not have an effect on liver glycogen levels. Similiarly, Usp28 knockout in mice did not affect glycogen storage in diethylnitrosamine-induced liver carcinoma. Thus, these data indicate that reduced expression of STBD1 or USP28 in CCF is unlikely to explain glycogen overload. Our study revealed several novel proteins and RNAs that are differentially expressed in CCF and have functions relevant for carcinogenesis or the glycogen metabolism.

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Hepatocellular glycogenotic foci after combined intraportal pancreatic islet transplantation and knockout of the carbohydrate responsive element binding protein in diabetic mice

Cited by 7 publications

References 43 publications

Carbohydrate Sensing Through the Transcription Factor ChREBP

Carbohydrate Sensing Through the Transcription Factor ChREBP

Oncogene-dependent addiction to carbohydrate-responsive element binding protein in hepatocellular carcinoma

Transcriptomic and Proteomic analysis of clear cell foci (CCF) in the human non-cirrhotic liver identifies several differentially expressed genes and proteins with functions in cancer cell biology and glycogen metabolism

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