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1. Injury-induced pulmonary tuft cells are heterogenous, arise independent of key Type 2 cytokines, and are dispensable for dysplastic repair

2. NAIP/NLRC4 inflammasome activation in MRP8+ cells is sufficient to cause systemic inflammatory disease

5. Genetic mapping reveals Pou2af2/ OCA-T1–dependent tuning of tuft cell differentiation and intestinal type 2 immunity

6. E-Protein Inhibition in ILC2 Development Shapes the Function of Mature ILC2s during Allergic Airway Inflammation

7. Tuft cell-derived acetylcholine regulates epithelial fluid secretion

8. Injury-induced pulmonary tuft cells are heterogenous, arise independent of key Type 2 cytokines, and are dispensable for dysplastic repair

9. Helminth-induced reprogramming of the stem cell compartment inhibits type 2 immunity

10. TSLP, IL-33, and IL-25: Not just for allergy and helminth infection

11. Multiomic analysis defines the first microRNA atlas across all small intestinal epithelial lineages and reveals novel markers of almost all major cell types

12. Direct reprogramming of the intestinal epithelium by parasitic helminths subverts type 2 immunity

13. Epithelial STAT6 O-GlcNAcylation drives a concerted anti-helminth alarmin response dependent on tuft cell hyperplasia and Gasdermin C

14. PGD2 and CRTH2 counteract Type 2 cytokine–elicited intestinal epithelial responses during helminth infection

15. Epithelial STAT6 O-GlcNAcylation Drives Anti-Helminth Immunity via a Concerted Alarmin Response

16. Tuning tuft cells: new ligands and effector functions reveal tissue-specific function

17. The Immune Function of Tuft Cells at Gut Mucosal Surfaces and Beyond

18. Thymic tuft cells promote an IL4-enriched medulla and shape thymocyte development

19. Sentinels of the Type 2 Immune Response

20. NAIP/NLRC4 inflammasome activation in MRP8+ cells is sufficient to cause systemic inflammatory disease

21. MicroRNA regulation of type 2 innate lymphoid cell homeostasis and function in allergic inflammation

22. CIRCling the wagons to protect intestinal stem cells

23. A three course menu for ILC and bystander T cell activation

24. The cysteinyl leukotriene 3 receptor regulates expansion of IL-25–producing airway brush cells leading to type 2 inflammation

25. Differential Activation of the Transcription Factor IRF1 Underlies the Distinct Immune Responses Elicited by Type I and Type III Interferons

26. Interpreting heterogeneity in intestinal tuft cell structure and function

27. Detection of succinate by intestinal tuft cells triggers a type 2 innate immune circuit

28. Tuft-cell-derived IL-25 regulates an intestinal ILC2–epithelial response circuit

29. Contributors

30. Intestinal Tuft Cells

31. Tuft-Cell-Derived Leukotrienes Drive Rapid Anti-helminth Immunity in the Small Intestine but Are Dispensable for Anti-protist Immunity

32. NAIP-NLRC4 Inflammasomes Coordinate Intestinal Epithelial Cell Expulsion with Eicosanoid and IL-18 Release via Activation of Caspase-1 and -8

33. Leukotrienes provide an NFAT-dependent signal that synergizes with IL-33 to activate ILC2s

34. The N -Ethyl- N -Nitrosourea-Induced Goldenticket Mouse Mutant Reveals an Essential Function of Sting in the In Vivo Interferon Response to Listeria monocytogenes and Cyclic Dinucleotides

35. Detection of Succinate by Intestinal Tuft Cells Triggers a Type 2 Innate Immune Circuit

36. ILC2 activation by leukotrienes: NFAT joins the team

37. Respiratory chain dysfunction and oxidative stress correlate with severity of primary CoQ 10 deficiency

38. I-L-C-2 it: type 2 immunity and group 2 innate lymphoid cells in homeostasis

39. Type 2 innate lymphoid cells control eosinophil homeostasis

40. Rapid induction of inflammatory lipid mediators by the inflammasome in vivo

41. The N-ethyl-N-nitrosourea-induced Goldenticket mouse mutant reveals an essential function of Sting in the in vivo interferon response to Listeria monocytogenes and cyclic dinucleotides

42. Critical function for Naip5 in inflammasome activation by a conserved carboxy-terminal domain of flagellin

43. Cell-type specific control of immune responses mediated by inflammasomes in vivo (INM6P.333)

44. Rapid induction of lipid mediators is a novel effector function of the inflammasome in vivo (117.24)

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