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1. Deletion of Gpatch2 does not alter Tnf expression in mice

2. Ubiquitylation of RIPK3 beyond-the-RHIM can limit RIPK3 activity and cell death

3. A missense mutation in the MLKL brace region promotes lethal neonatal inflammation and hematopoietic dysfunction

4. Deletion of intestinal Hdac3 remodels the lipidome of enterocytes and protects mice from diet-induced obesity

5. Correction: TRAF2 regulates TNF and NF-κB signalling to suppress apoptosis and skin inflammation independently of Sphingosine kinase 1

6. TRAF2 regulates TNF and NF-κB signalling to suppress apoptosis and skin inflammation independently of Sphingosine kinase 1

7. TNFR1-dependent cell death drives inflammation in Sharpin-deficient mice

8. MLKL deficiency protects against low-grade, sterile inflammation in aged mice

9. Cell death in skin function, inflammation, and disease

11. ZC3H12C expression in dendritic cells is necessary to prevent lymphadenopathy of skin‐draining lymph nodes

12. Human LUBAC deficiency leads to autoinflammation and immunodeficiency by dysregulation in TNF-mediated cell death

13. Cell death in chronic inflammation: breaking the cycle to treat rheumatic disease

14. A missense mutation in the MLKL brace region promotes lethal neonatal inflammation and hematopoietic dysfunction

15. Mutations that prevent caspase cleavage of RIPK1 cause autoinflammatory disease

16. EHF is essential for epidermal and colonic epithelial homeostasis, and suppresses Apc-initiated colonic tumorigenesis

17. EHF is essential for epidermal and colonic epithelial homeostasis and suppresses Apc-initiated colonic tumorigenesis

18. Langerhans cells are an essential cellular intermediary in chronic dermatitis

19. Interferon-γ primes macrophages for pathogen ligand-induced killing via a caspase-8 and mitochondrial cell death pathway

20. RIPK1 prevents TRADD-driven, but TNFR1 independent, apoptosis during development

21. Deletion of intestinal Hdac3 remodels the lipidome of enterocytes and protects mice from diet-induced obesity

22. Missense mutations in the MLKL ‘brace’ region lead to lethal neonatal inflammation in mice and are present in high frequency in humans

23. RIPK1 and Caspase-8 Ensure Chromosome Stability Independently of Their Role in Cell Death and Inflammation

24. Inhibitor of Apoptosis Proteins (IAPs) Limit RIPK1-Mediated Skin Inflammation

25. RIPK1 Regulates RIPK3-MLKL-Driven Systemic Inflammation and Emergency Hematopoiesis

26. cIAPs and XIAP regulate myelopoiesis through cytokine production in an RIPK1- and RIPK3-dependent manner

28. IAPs limit activation of RIP kinases by TNF receptor 1 during development

29. Linear ubiquitination prevents inflammation and regulates immune signalling

30. Cyclic‐AMP‐dependent protein kinase A regulates apoptosis by stabilizing the BH3‐only protein Bim

31. RIPK1 is not essential for TNFR1-induced activation of NF-kappaB

32. Whatever Happened to 'Always Cite the Source?'

33. Author response: TRAF2 regulates TNF and NF-κB signalling to suppress apoptosis and skin inflammation independently of Sphingosine kinase 1

34. Targeting of Fn14 prevents cancer-induced cachexia and prolongs survival

35. TRAF2 regulates TNF and NF-kappa B signalling to suppress apoptosis and skin inflammation independently of Sphingosine kinase 1

36. Tumor necrosis factor (TNF) signaling, but not TWEAK (TNF-like weak inducer of apoptosis)-triggered cIAP1 (cellular inhibitor of apoptosis protein 1) degradation, requires cIAP1 RING dimerization and E2 binding

37. Author response: TNFR1-dependent cell death drives inflammation in Sharpin-deficient mice

38. TNFR1-dependent cell death drives inflammation in Sharpin-deficient mice

39. IAPs limit activation of RIP kinases by TNF receptor 1 during development

40. Inhibitor of apoptosis proteins limit RIP3 kinase-dependent interleukin-1 activation

41. In TNF-stimulated Cells, RIPK1 Promotes Cell Survival by Stabilizing TRAF2 and cIAP1, which Limits Induction of Non-canonical NF-κB and Activation of Caspase-8*

42. Deletion of cIAP1 and cIAP2 in murine B lymphocytes constitutively activates cell survival pathways and inactivates the germinal center response

43. [Untitled]

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