Epithelial NEMO links innate immunity to chronic intestinal inflammation

Nenci, Arianna; Becker, Christoph; Wullaert, Andy; Gareus, Ralph; Loo, Geert; Danese, Silvio; Huth, Marion; Nikolaev, Alexei; Neufert, Clemens; Madison, Blair B.; Gumucio, Deborah L.; Neurath, Markus F.; Pasparakis, Manolis

doi:10.1038/nature05698

Cited by 949 publications

(844 citation statements)

References 31 publications

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“…55,56 Hepatocyte-specific deletion of TAK1 triggers TNFa-dependent liver injury and hepatocellular carcinoma within 6 weeks of age, whereas loss of NF-kB activation by NEMO deletion causes much milder liver injury around 20 weeks of age. 57 Furthermore, it appears that NF-kB activity is not always regulated by TAK1 in some tissues in vivo.…”

Section: Tak1 Control Of Cell Death Sr Mihaly Et Almentioning

confidence: 99%

TAK1 control of cell death

2014

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Programmed cell death, a physiologic process for removing cells, is critically important in normal development and for elimination of damaged cells. Conversely, unattended cell death contributes to a variety of human disease pathogenesis. Thus, precise understanding of molecular mechanisms underlying control of cell death is important and relevant to public health. Recent studies emphasize that transforming growth factor-b-activated kinase 1 (TAK1) is a central regulator of cell death and is activated through a diverse set of intra-and extracellular stimuli. The physiologic importance of TAK1 and TAK1-binding proteins in cell survival and death has been demonstrated using a number of genetically engineered mice. These studies uncover an indispensable role of TAK1 and its binding proteins for maintenance of cell viability and tissue homeostasis in a variety of organs. TAK1 is known to control cell viability and inflammation through activating downstream effectors such as NF-jB and mitogen-activated protein kinases (MAPKs). It is also emerging that TAK1 regulates cell survival not solely through NF-jB but also through NF-jB-independent pathways such as oxidative stress and receptor-interacting protein kinase 1 (RIPK1) kinase activity-dependent pathway. Moreover, recent studies have identified TAK1's seemingly paradoxical role to induce programmed necrosis, also referred to as necroptosis. This review summarizes the consequences of TAK1 deficiency in different cell and tissue types from the perspective of cell death and also focuses on the mechanism by which TAK1 complex inhibits or promotes programmed cell death. This review serves to synthesize our current understanding of TAK1 in cell survival and death to identify promising directions for future research and TAK1's potential relevance to human disease pathogenesis.

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Section: Tak1 Control Of Cell Death Sr Mihaly Et Almentioning

confidence: 99%

TAK1 control of cell death

2014

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“…In several genetically engineered and T-cell transfer models, luminal bacterial proteins provide the dominant antigenic stimulation for eff ector T helper 1 and T helper 17 cells (42,44) . Moreover, intestinal epithelial-specifi c defects in Toll-like receptor and nuclear factor-κ B signaling can lead to mucosal barrier defects, mucosal luminal bacterial translocation, and immune-mediated intestinal infl ammation ( 45 ). Finally, a primary etiologic role for intestinal dysbiosis is supported by transmission of colitis with fecal transplant ( 46,47 ).…”

Section: Therapeutic Approachesmentioning

confidence: 99%

Intestinal Microbes in Inflammatory Bowel Diseases

Sartor¹,

Mazmanian²

2012

Am J Gastroenterol Suppl

177

151

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“…If PRRs are expressed in the intestinal epithelium but do not induce signaling leading to the transcription of proinflammatory cytokines or to Paneth cell degranulation, what could be the other effects of stimulation? Previous studies in mice have elegantly linked PRR signaling to epithelial homeostasis (Nenci et al, 2007;Rakoff-Nahoum et al, 2004). Organoid studies could now show that PAMPs have a direct effect on epithelial regeneration.…”

Section: Pattern Recognitionmentioning

confidence: 99%