IKKβ Couples Hepatocyte Death to Cytokine-Driven Compensatory Proliferation that Promotes Chemical Hepatocarcinogenesis

Maeda, Shin; Kamata, Hideaki; Luo, Jun-Li; Leffert, Hyam L.; Karin, Michael

doi:10.1016/j.cell.2005.04.014

Cited by 1,086 publications

(1,288 citation statements)

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“…The TNAP-AID mouse model exhibits several characteristics of human HCC, in that the mice develop HCC spontaneously and the HCC tissue expresses a-fetoprotein and that it has the p53 gene mutations, some of which cause the same amino acid replacements as those seen in human tumours. Earlier HCC mouse models include mice with genetic modifications of Lkb1, Mdr2, Aox and Pten genes (Fan et al, 1998;Nakau et al, 2002;Horie et al, 2004;Katzenellenbogen et al, 2006), transgenic mice overexpressing c-myc, transforming growth factor-a, transforming growth factor-b1, HBx of hepatitis B virus and HCV core (Sandgren et al, 1989;Kim et al, 1991;Murakami et al, 1993;Koike et al, 1994Koike et al, , 2002Factor et al, 1997;Riehle et al, 2008) and chemical-or diet-induced HCC (Sell, 2001;Maeda et al, 2005;Ma et al, 2006;Sakurai et al, 2006). In contrast to these models, our TNAP-AID model is unique because it does not arbitrarily target specific oncogenes, tumour suppressors or stability genes.…”

Section: Discussionmentioning

confidence: 99%

A novel mouse model of hepatocarcinogenesis triggered by AID causing deleterious p53 mutations

et al. 2008

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Activation-induced cytidine deaminase (AID), the only enzyme that is known to be able to induce mutations in the human genome, is required for somatic hypermutation and class-switch recombination in B lymphocytes. Recently, we showed that AID is implicated in the pathogenesis of human cancers including hepatitis C virus (HCV)-induced human hepatocellular carcinoma (HCC). In this study, we established a new AID transgenic mouse model (TNAP-AID) in which AID is expressed in cells producing tissue-nonspecific alkaline phosphatase (TNAP), which is a marker of primordial germ cells and immature stem cells, including ES cells. High expression of TNAP was found in the liver of the embryos and adults of TNAP-AID mice. HCC developed in 27% of these mice at the age of approximately 90 weeks. The HCC that developed in TNAP-AID mice expressed a-fetoprotein and had deleterious mutations in the tumour suppressor gene Trp53, some of which corresponded to those found in human cancer. In conclusion, TNAP-AID is a mouse model that spontaneously develops HCC, sharing genetic and phenotypic features with human HCC, which develops in the inflamed liver as a result of the accumulation of genetic changes.

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Section: Discussionmentioning

confidence: 99%

A novel mouse model of hepatocarcinogenesis triggered by AID causing deleterious p53 mutations

et al. 2008

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“…In this study, which utilized a mouse model of spontaneous hepatitis followed by hepatocellular carcinoma, inhibition of NF-kB in hepatocytes through regulatable IkBa super-repressor expression did not block hepatitis or the earliest stages of neoplasia; however, inhibition of NF-kB at later stages (either through IkBa expression or through TNF antibodies) induced apoptosis and blocked progression to hepatocellular carcinoma. In a related study, Maeda et al (2005) showed that, although loss of IKKb in hepatocytes actually promotes chemical-induced hepatocarcinogenesis through a compensatory mechanism downstream of JNK-mediated cell death, knockout of IKKb in hemopoietic-derived Kupffer cells suppressed hepatocarcinogenesis, indicating that NF-kB expression in these cells is crucial for the inflammation-mediated neoplastic growth.…”

Section: Roles For Nf-jb In Inflammation-associated Cancersmentioning

confidence: 99%

Nuclear factor-κB and inhibitor of κB kinase pathways in oncogenic initiation and progression

2006

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“…As discussed above, TNFα production by inflammatory cells is largely dependent on p38α in chronic inflammation, such as hepatitis. Interestingly, liver cells lacking the NFkB activator IKKβ show decreased activities of DUSPs, which leads to enhanced JNK1 phosphorylation and increased liver carcinogenesis (Maeda et al, 2005).…”

Section: Crosstalk Between Mapk Signaling In Inflammation and Cancermentioning

confidence: 99%

MAPK signaling in inflammation-associated cancer development

2010

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Mitogen-activated protein (MAP) kinases comprise a family of protein-serine/threonine kinases, which are highly conserved in protein structures from unicellular eukaryotic organisms to multicellular organisms, including mammals. These kinases, including ERKs, JNKs and p38s, are regulated by a phosphorelay cascade, with a prototype of three protein kinases that sequentially phosphorylate one another. MAPKs transduce extracellular signals into a variety of cellular processes, such as cell proliferation, survival, death, and differentiation. Consistent with their essential cellular functions, MAPKs have been shown to play critical roles in embryonic development, adult tissue homeostasis and various pathologies. In this review, we discuss recent findings that reveal the profound impact of these pathways on chronic inflammation and, particularly, inflammation-associated cancer development.

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IKKβ Couples Hepatocyte Death to Cytokine-Driven Compensatory Proliferation that Promotes Chemical Hepatocarcinogenesis

Cited by 1,086 publications

References 48 publications

A novel mouse model of hepatocarcinogenesis triggered by AID causing deleterious p53 mutations

A novel mouse model of hepatocarcinogenesis triggered by AID causing deleterious p53 mutations

Nuclear factor-κB and inhibitor of κB kinase pathways in oncogenic initiation and progression

MAPK signaling in inflammation-associated cancer development

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