Unravelling the complexities of the NF-κB signalling pathway using mouse knockout and transgenic models

Gerondakis, Steve; Grumont, Raelene J.; Gugasyan, Raffi; Wong, Wendy Wei-Lynn; Isomura, Iwao; Ho, Wai Chi; Banerjee, Aditi

doi:10.1038/sj.onc.1209944

Cited by 287 publications

(290 citation statements)

References 190 publications

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“…27 This phenotype was reproduced in mice with constitutive global deletion of ikk␤ or NEMO, confirming that the IKK/NF-B system plays a critical role in hepatocyte survival, at least during embryogenesis. 28 At the same time, data from in vitro studies with human HCC cell lines consistently demonstrate that NF-B is cytoprotective via its ability to prevent apoptosis. Furthermore, the oncogenic HBV protein HBx and the HCV core and NS5B proteins were reported to induce NF-B.…”

Section: Nf-b As a Tumor Suppressor In Hepatocytesmentioning

confidence: 75%

Nuclear factor‐κB and the hepatic inflammation‐fibrosis‐cancer axis†

2007

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Nuclear factor-B (NF-B) is a transcriptional regulator of genes involved in immunity, inflammatory response, cell fate, and function. Recent attention has focused on the pathophysiological role of NF-B in the diseased liver. In vivo studies using rodent models of liver disease and cell-targeted perturbation of NF-B activity have revealed complex and multicellular functions in hepatic inflammation, fibrosis, and the development of hepatocellular carcinoma-a process we have termed the "inflammation-fibrosis-cancer axis". This review summarizes the current state of knowledge and provides insight into the vast complexity of the hepatic NF-B signaling system, which should provide a rich source of new therapeutic targets. (HEPATOLOGY 2007;46:590-597.)

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Section: Nf-b As a Tumor Suppressor In Hepatocytesmentioning

confidence: 75%

Nuclear factor‐κB and the hepatic inflammation‐fibrosis‐cancer axis†

2007

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“…In addition, specific C-terminal Ser to Ala mutations are sometimes included to reduce the constitutive turnover of IkBa (van Antwerp et al, 1996). Such SR molecules have been used successfully to inhibit NF-kB activity in a variety of in vitro cell culture studies (e.g., van Antwerp et al, 1996;Wang et al, 1996;Bushdid et al, 1998;Kanegae et al, 1998) and in several in vivo transgenic mouse studies (see Gerondakis et al, 2006). In general, the use of the IkBa-SR has been taken as one of the best evidences for the involvement of NF-kB in a given physiological process; however, because IkBa does not bind well to RelB-containing complexes, the IkBa-SR is probably primarily a blocker of the canonical NF-kB pathway.…”

Section: Ikb Super-repressorsmentioning

confidence: 99%

“…For example, as described above, IKKa and IKKb are active as dimers. However, they appear to have distinct physiological functions in that disruption of each IKK gene in mice leads to quite different phenotypes (Gerondakis et al, 2006). Furthermore, IKKa and IKKb can be activated independently by different upstream signals.…”

Section: Introductionmentioning

confidence: 99%

Inhibitors of NF-κB signaling: 785 and counting

2006

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“…These stimuli may trigger inflammation, innate immune responses, adaptive immune responses, secondary lymphoid organ development and osteoclastogenesis. Studies with knockout mice have revealed NF-kB's critical involvement in all of these processes (Gerondakis et al, 2006). NF-kB was first identified as a biochemical activity capable of binding to a 10 base pairs (bp) sequence within the transcriptional enhancer of the immunoglobulin (Ig) k light chain gene.…”

Section: Introductionmentioning

confidence: 99%

Transcriptional regulation via the NF-κB signaling module

2006

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Stimulus-induced nuclear factor-jB (NF-jB) activity, the central mediator of inflammatory responses and immune function, comprises a family of dimeric transcription factors that regulate diverse gene expression programs consisting of hundreds of genes. A family of inhibitor of jB (IjB) proteins controls NF-jB DNA-binding activity and nuclear localization. IjB protein metabolism is intricately regulated through stimulus-induced degradation and feedback re-synthesis, which allows for dynamic control of NF-jB activity. This network of interactions has been termed the NF-jB signaling module. Here, we summarize the current understanding of the molecular structures and biochemical mechanisms that determine NF-jB dimer formation and the signal-processing characteristics of the signaling module. We identify NF-jB-jB site interaction specificities and dynamic control of NF-jB activity as mechanisms that generate specificity in transcriptional regulation. We discuss examples of gene regulation that illustrate how these mechanisms may interface with other transcription regulators and promoter-associated events, and how these mechanisms suggest regulatory principles for NF-jB-mediated gene activation.

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Unravelling the complexities of the NF-κB signalling pathway using mouse knockout and transgenic models

Cited by 287 publications

References 190 publications

Nuclear factor‐κB and the hepatic inflammation‐fibrosis‐cancer axis†

Nuclear factor‐κB and the hepatic inflammation‐fibrosis‐cancer axis†

Inhibitors of NF-κB signaling: 785 and counting

Transcriptional regulation via the NF-κB signaling module

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