TRAF2 is a biologically important necroptosis suppressor

Petersen, Sean; Chen, T T; Lawrence, David A.; Marsters, Scot A.; Gonzalvez, François; Ashkenazi, Avi

doi:10.1038/cdd.2015.35

Cited by 80 publications

(75 citation statements)

References 56 publications

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“…Accordingly, the RIPK1-deubiquitinating enzyme cylindromatosis (CYLD) is required for optimal necroptotic responses following TNFR1 ligation (78–80), whereas the ubiquitin-modifying TNF alpha induced protein 3 (TNFAIP3; best known as A20) and LUBAC limit TNFR1-driven necroptosis by favoring RIPK1 ubiquitination (81–85). A20 also suppresses necroptosis by deubiquitinating RIPK3 at K5 (86), whereas CYLD mediates necroptotic effects by deubiquitinating TNF receptor associated factor 2 (TRAF2) (87). …”

Section: Molecular Mechanisms Of Necroptosismentioning

confidence: 99%

“…Aside from being involved in the regulation of extrinsic apoptosis, TRAF2 inhibits necroptosis driven by TNFR1 and other death receptors by directly interacting with MLKL (87, 88). Accordingly, the whole-body deletion of Traf2 in adult mice is lethal, owing to an acute hepatotoxic response that can be prevented by deleting Ripk3 (87).…”

Section: Molecular Mechanisms Of Necroptosismentioning

confidence: 99%

Section: Molecular Mechanisms Of Necroptosismentioning

confidence: 99%

“…Accordingly, the whole-body deletion of Traf2 in adult mice is lethal, owing to an acute hepatotoxic response that can be prevented by deleting Ripk3 (87). Mice lacking Traf2 and Ripk3 , however, succumb in a delayed manner upon the hyperactivation of Casp8 in the intestinal epithelium, and this process can be completely blocked with a cocktail of monoclonal antibodies that antagonize TNFR1 and other death receptors (87). Of note, whereas some authors propose that mitogen-activated protein kinase kinase kinase 7 (MAP3K7; best known as TAK1) mediates antinecroptotic effects by preventing RIPK1 signaling (77, 89, 90), others suggest that prolonged TAK1 activation (which is usually a transient consequence of TNFR1 ligation) may result in RIPK3 phosphorylation and the consequent initiation of a feedforward amplification circuitry with potent pronecroptotic activity (91).…”

Section: Molecular Mechanisms Of Necroptosismentioning

confidence: 99%

See 3 more Smart Citations

Necroptosis: Mechanisms and Relevance to Disease

Galluzzi

Kepp

Chan

2017

Annu. Rev. Pathol. Mech. Dis.

479

398

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Necroptosis is a form of regulated cell death that critically depends on receptor-interacting serine-threonine kinase 3 (RIPK3) and mixed lineage kinase domain-like (MLKL) and generally manifests with morphological features of necrosis. The molecular mechanisms that underlie distinct instances of necroptosis have just begun to emerge. Nonetheless, it has already been shown that necroptosis contributes to cellular demise in various pathophysiological conditions, including viral infection, acute kidney injury, and cardiac ischemia/reperfusion. Moreover, human tumors appear to obtain an advantage from the downregulation of key components of the molecular machinery for necroptosis. Although such an advantage may stem from an increased resistance to adverse microenvironmental conditions, accumulating evidence indicates that necroptosis-deficient cancer cells are poorly immunogenic and hence escape natural and therapy-elicited immunosurveillance. Here, we discuss the molecular mechanisms and relevance to disease of necroptosis.

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Section: Molecular Mechanisms Of Necroptosismentioning

confidence: 99%

Section: Molecular Mechanisms Of Necroptosismentioning

confidence: 99%

Section: Molecular Mechanisms Of Necroptosismentioning

confidence: 99%

Section: Molecular Mechanisms Of Necroptosismentioning

confidence: 99%

See 2 more Smart Citations

Necroptosis: Mechanisms and Relevance to Disease

Galluzzi

Kepp

Chan

2017

Annu. Rev. Pathol. Mech. Dis.

479

398

View full text Add to dashboard Cite

show abstract

“…Nevertheless, TRAF2 knockout cells exhibit increased sensitivity to TNF-α-induced apoptosis, suggesting that TRAF2 is required for NF-κB-independent mechanisms that protect against TNF-α-induced apoptosis. Similar effects of TRAF2 on cell death have been demonstrated in Fas or tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) receptor signaling [25,26]. Moreover, a recent report has demonstrated that TRAF2 suppresses the induction of apoptosis through the mechanism of K48-linked polyubiquitination of activated caspase-8, which can account for the NF-κB-independent mechanism by which TRAF2 exerts anti-apoptotic activity [27].…”

Section: Introductionmentioning

confidence: 72%

Brefeldin A-Inhibited Guanine Nucleotide-Exchange Factor 1 (BIG1) Governs the Recruitment of Tumor Necrosis Factor Receptor-Associated Factor 2 (TRAF2) to Tumor Necrosis Factor Receptor 1 (TNFR1) Signaling Complexes

Noguchi

Tsuchida

Kogue

et al. 2016

IJMS

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Tumor necrosis factor receptor-associated factor 2 (TRAF2) is a critical mediator of tumor necrosis factor-α (TNF-α) signaling. However, the regulatory mechanisms of TRAF2 are not fully understood. Here we show evidence that TRAF2 requires brefeldin A-inhibited guanine nucleotide-exchange factor 1 (BIG1) to be recruited into TNF receptor 1 (TNFR1) signaling complexes. In BIG1 knockdown cells, TNF-α-induced c-Jun N-terminal kinase (JNK) activation was attenuated and the sensitivity to TNF-α-induced apoptosis was increased. Since these trends correlated well with those of TRAF2 deficient cells as previously demonstrated, we tested whether BIG1 functions as an upstream regulator of TRAF2 in TNFR1 signaling. As expected, we found that knockdown of BIG1 suppressed TNF-α-dependent ubiquitination of TRAF2 that is required for JNK activation, and impaired the recruitment of TRAF2 to the TNFR1 signaling complex (complex I). Moreover, we found that the recruitment of TRAF2 to the death-inducing signaling complex termed complex II was also impaired in BIG1 knockdown cells. These results suggest that BIG1 is a key component of the machinery that drives TRAF2 to the signaling complexes formed after TNFR1 activation. Thus, our data demonstrate a novel and unexpected function of BIG1 that regulates TNFR1 signaling by targeting TRAF2.

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Moderate Folic Acid Supplementation in Pregnant Mice Results in Altered Methyl Metabolism and in Sex‐Specific Placental Transcription Changes

Liang

Leclerc

Cosín-Tomás

et al. 2021

Molecular Nutrition Food Res

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Scope: Many pregnant women have higher folic acid (FA) intake due to food fortification and increased vitamin use. It is reported that diets containing five-fold higher FA than recommended for mice (5xFASD) during pregnancy resulted in methylenetetrahydrofolate reductase (MTHFR) deficiency and altered choline/methyl metabolism, with neurobehavioral abnormalities in newborns. The goal is to determine whether these changes have their origins in the placenta during embryonic development. Methods and Results: Female mice are fed control diet or 5xFASD for a month before mating and maintained on these diets until embryonic day 17.5. 5xFASD led to pseudo-MTHFR deficiency in maternal liver and altered choline/methyl metabolites in maternal plasma (increased methyltetrahydrofolate and decreased betaine). Methylation potential (S-adenosylmethionine:S-adenosylhomocysteine ratio) and glycerophosphocholine are decreased in placenta and embryonic liver. Folic acid supplemented diet results in sex-specific transcriptome profiles in placenta, with validation of dietary expression changes of 29 genes involved in angiogenesis, receptor biology or neurodevelopment, and altered methylation of the serotonin receptor 2A gene. Conclusion: Moderate increases in folate intake during pregnancy result in placental metabolic and gene expression changes, particularly in angiogenesis, which may contribute to abnormal behavior in pups. These results are relevant for determining a safe upper limit for folate intake during pregnancy.

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TRAF2 is a biologically important necroptosis suppressor

Cited by 80 publications

References 56 publications

Necroptosis: Mechanisms and Relevance to Disease

Necroptosis: Mechanisms and Relevance to Disease

Brefeldin A-Inhibited Guanine Nucleotide-Exchange Factor 1 (BIG1) Governs the Recruitment of Tumor Necrosis Factor Receptor-Associated Factor 2 (TRAF2) to Tumor Necrosis Factor Receptor 1 (TNFR1) Signaling Complexes

Moderate Folic Acid Supplementation in Pregnant Mice Results in Altered Methyl Metabolism and in Sex‐Specific Placental Transcription Changes

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