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1. Janus face of sepsis: a viewpoint

2. Towards an ecological definition of sepsis: a viewpoint

3. Fever and hypothermia represent two populations of sepsis patients and are associated with outside temperature

4. Targeted delivery of a phosphoinositide 3‐kinase γ inhibitor to restore organ function in sepsis

5. Impact of ambient temperature on inflammation-induced encephalopathy in endotoxemic mice—role of phosphoinositide 3-kinase gamma

6. Hormesis Meetings at the Royal Palace

8. Memory-Like Responses of Brain Microglia Are Controlled by Developmental State and Pathogen Dose

9. PI3Kγ Mediates Microglial Proliferation and Cell Viability via ROS

10. Memory-Like Inflammatory Responses of Microglia to Rising Doses of LPS: Key Role of PI3Kγ

11. Trained Circulating Monocytes in Atherosclerosis: Ex Vivo Model Approach

12. The Role of the Pathogen Dose and PI3Kγ in Immunometabolic Reprogramming of Microglia for Innate Immune Memory

13. NLPR3 Inflammasomes and Their Significance for Atherosclerosis

14. Signaling Pathways and Key Genes Involved in Regulation of foam Cell Formation in Atherosclerosis

15. In Search for Genes Related to Atherosclerosis and Dyslipidemia Using Animal Models

16. Role of Phagocytosis in the Pro-Inflammatory Response in LDL-Induced Foam Cell Formation; a Transcriptome Analysis

17. Enhancing and Extending Biological Performance and Resilience

18. Deterioration of Organ Function As a Hallmark in Sepsis: The Cellular Perspective

19. Liver dysfunction and phosphatidylinositol-3-kinase signalling in early sepsis: experimental studies in rodent models of peritonitis.

20. Hormetic Signaling Patterns

23. Prostaglandin EP3 receptor activation is antinociceptive in sensory neurons via PI3Kγ, AMPK and GRK2

24. Targeting Complement C5a Receptor 1 for the Treatment of Immunosuppression in Sepsis

25. The cellular basis of organ failure in sepsis—signaling during damage and repair processes

26. Targeted delivery of a phosphoinositide 3-kinase γ inhibitor to restore organ function in sepsis through dye-functionalized lipid nanocarriers

27. NLPR3 Inflammasomes and Their Significance for Atherosclerosis

28. A brief overview of currently used atherosclerosis treatment approaches targeting lipid metabolism alterations

29. In Search for Genes Related to Atherosclerosis and Dyslipidemia Using Animal Models

30. Role of Phagocytosis in the Pro-Inflammatory Response in LDL-Induced Foam Cell Formation; a Transcriptome Analysis

31. Role of adipose tissue in facial aging

32. Phosphoinositide 3-kinase γ ties chemoattractant- and adrenergic control of microglial motility

33. Phagocytosis of bone marrow derived macrophages is controlled by phosphoinositide 3-kinase γ

34. Pathogen-Induced Hormetic Responses

35. List of Contributors

36. The protein-tyrosine phosphatase DEP-1 promotes migration and phagocytic activity of microglial cells in part through negative regulation of fyn tyrosine kinase

37. Impact of Connexins on Atherogenesis: A Brief Review

38. Signaling Pathways and Key Genes Involved in Regulation of foam Cell Formation in Atherosclerosis

39. Enhancing and Extending Biological Performance and Resilience

40. Toxin-induced hormesis may restrain aging

41. Reduced ambient temperature exacerbates SIRS-induced cardiac autonomic dysregulation and myocardial dysfunction in mice

42. Remembering Pathogen Dose: Long-Term Adaptation in Innate Immunity

43. The fifth dimension of innate immunity

44. PI3Kγ integrates cAMP and Akt signalling of the μ-opioid receptor

45. Trügerische Etiketten für Signalproteine

46. Phosphoinositide 3-kinase ? mediates microglial phagocytosis via lipid kinase-independent control of cAMP

47. Phosphoinositide 3-Kinase γ Restrains Neurotoxic Effects of Microglia After Focal Brain Ischemia

48. The p101 subunit of PI3Kγ restores activation by Gβ mutants deficient in stimulating p110γ

49. PI3Kγ controls oxidative bursts in neutrophils via interactions with PKCα and p47phox

50. Overlapping and distinct roles for PI3Kβ and γ isoforms in S1P-induced migration of human and mouse endothelial cells

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