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1. المستوى الدلالي في رسائل الزرزوريات

3. Prospects for Urinary Proteomics

6. Calpastatin controls polymicrobial sepsis by limiting procoagulant microparticle release.

8. AP214, an analogue of alpha-melanocyte-stimulating hormone, ameliorates sepsis-induced acute kidney injury and mortality.

9. Macrophage depletion protects against cisplatin-induced ototoxicity and nephrotoxicity.

10. Macrophage Depletion Protects Against Cisplatin-Induced Ototoxicity and Nephrotoxicity.

11. Readmission and Mortality After Hospitalization With Acute Kidney Injury.

12. BAM15 treats mouse sepsis and kidney injury, linking mortality, mitochondrial DNA, tubule damage, and neutrophils.

13. The Application of Guanidinium to Improve Biomolecule Quality in Fixed, Paraffin-embedded Tissue.

15. The effect of continuous intravenous norepinephrine infusion on systemic hemodynamics in a telemetrically-monitored mouse model of sepsis.

16. Class B Scavenger Receptors BI and BII Protect against LPS-Induced Acute Lung Injury in Mice by Mediating LPS.

17. Cell-free DNA maps COVID-19 tissue injury and risk of death and can cause tissue injury.

19. Improving Care for Patients after Hospitalization with AKI.

21. A Furosemide Excretion Stress Test Predicts Mortality in Mice After Sepsis and Outperforms the Furosemide Stress Test During Vasopressin Administration.

22. Sex and the kidneys: current understanding and research opportunities.

23. Circadian variation in the release of small extracellular vesicles can be normalized by vesicle number or TSG101.

24. Chronic kidney diseases in agricultural communities: report from a workshop.

25. Enlightening kidney pathophysiology.

26. Gut Leakage of Fungal-Derived Inflammatory Mediators: Part of a Gut-Liver-Kidney Axis in Bacterial Sepsis.

27. Statistical methods for building better biomarkers of chronic kidney disease.

28. How Community Engagement Is Enhancing NIDDK Research.

29. Mesenchymal stromal cell potency to treat acute kidney injury increased by ultrasound-activated interferon-γ/interleukin-10 axis.

31. Overcoming Translational Barriers in Acute Kidney Injury: A Report from an NIDDK Workshop.

32. Research Needs to Understand Self-Management of Lower Urinary Tract Symptoms: Summary of NIDDK Workshop.

33. The role of adenosine 1a receptor signaling on GFR early after the induction of sepsis.

34. Developing a neonatal acute kidney injury research definition: a report from the NIDDK neonatal AKI workshop.

35. Complementary Initiatives from the NIDDK to Advance Kidney Health.

36. Nonbiologic factors that impact management in women with urinary incontinence: review of the literature and findings from a National Institute of Diabetes and Digestive and Kidney Diseases workshop.

37. Mitochondrial DNA-enriched microparticles promote acute-on-chronic alcoholic neutrophilia and hepatotoxicity.

38. Future Directions of Research and Care for Urinary Incontinence: Findings from the National Institute of Diabetes and Digestive and Kidney Diseases Summit on Urinary Incontinence Clinical Research in Women.

39. Quantification of Exosomes.

40. Research Needs for Effective Transition in Lifelong Care of Congenital Genitourinary Conditions: A Workshop Sponsored by the National Institute of Diabetes and Digestive and Kidney Diseases.

41. Human SR-BII mediates SAA uptake and contributes to SAA pro-inflammatory signaling in vitro and in vivo.

42. Urine Exosomes: An Emerging Trove of Biomarkers.

43. Advancing a Comprehensive Approach to the Study of Lower Urinary Tract Symptoms.

45. Social Determinants of Racial Disparities in CKD.

46. Urinary Stone Disease: Advancing Knowledge, Patient Care, and Population Health.

47. Antagonism of scavenger receptor CD36 by 5A peptide prevents chronic kidney disease progression in mice independent of blood pressure regulation.

48. Human SR-BI and SR-BII Potentiate Lipopolysaccharide-Induced Inflammation and Acute Liver and Kidney Injury in Mice.

49. Strategies to improve the understanding of long-term renal consequences after neonatal acute kidney injury.

50. The Authors Reply.

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