389 results on '"Cornelius, Denise C."'
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2. Preeclampsia and COVID-19: the Role of Inflammasome Activation
3. Tumor Necrosis Factor-alpha Blockade Improves Uterine Artery Resistance, Maternal Blood Pressure, and Fetal Growth in Placental Ischemic Rats
4. The role of tumor necrosis factor in triggering activation of natural killer cell, multi-organ mitochondrial dysfunction and hypertension during pregnancy
5. Vascular endothelial mitochondrial oxidative stress in response to preeclampsia: a role for angiotension II type 1 autoantibodies
6. IL‐33 Signaling Inhibition Leads to a Preeclampsia‐Like Phenotype in Pregnant Rats.
7. Abatacept Decreases Renal T-cell Infiltration and Renal Inflammation and Ameliorates Progressive Renal Injury in Obese Dahl Salt-sensitive Rats Before Puberty.
8. 17-Hydroxyprogesterone caproate improves T cells and NK cells in response to placental ischemia; new mechanisms of action for an old drug
9. AT1‐AA Is Produced in Offspring in Response to Placental Ischemia and Is Lowered by B‐Cell Depletion Without Compromising Overall Offspring Health
10. Inhibition of Caspase 1 Reduces Blood Pressure, Cytotoxic NK Cells, and Inflammatory T-Helper 17 Cells in Placental Ischemic Rats
11. Investigation of interleukin-2-mediated changes in blood pressure, fetal growth restriction, and innate immune activation in normal pregnant rats and in a preclinical rat model of preeclampsia
12. Renal natural killer cell activation and mitochondrial oxidative stress; new mechanisms in AT1-AA mediated hypertensive pregnancy
13. Placental CD4+ T cells isolated from preeclamptic women cause preeclampsia-like symptoms in pregnant nude-athymic rats
14. IL-33 supplementation improves uterine artery resistance and maternal hypertension in response to placental ischemia.
15. Metformin reduces insulin resistance and attenuates progressive renal injury in prepubertal obese Dahl salt-sensitive rats
16. Abstract 022: Il-33 Supplementation Improves Vascular Function And Maternal Hypertension In Response To Placental Ischemia
17. Contributors
18. The Role of Sex Differences in Inflammation and Autoimmune Diseases
19. Plasma syndecan-1 levels identify a cohort of patients with severe sepsis at high risk for intubation after large-volume intravenous fluid resuscitation
20. Chronic treatment with IL-25 increases renal M2 macrophages and reduces renal injury in obese Dahl salt-sensitive rats during the prepubescent stage
21. VASCULAR AND RENAL MECHANISMS OF PREECLAMPSIA
22. Role of Mitochondrial Dysfunction and Reactive Oxygen Species in Mediating Hypertension in the Reduced Uterine Perfusion Pressure Rat Model of Preeclampsia
23. Metformin reduces insulin resistance and attenuates progressive renal injury in prepubertal obese Dahl salt-sensitive rats.
24. NLRP3 inhibition improves maternal hypertension, inflammation, and vascular dysfunction in response to placental ischemia
25. Inhibiting B cell activating factor attenuates preeclamptic symptoms in placental ischemic rats
26. B2 cells contribute to hypertension and natural killer cell activation possibly via AT1-AA in response to placental ischemia
27. Sex differences in cardiovasculasr response to sepsis
28. Neutralizing MIP3a reduces renal immune cell infiltration and progressive renal injury in young obese Dahl salt-sensitive rats
29. RUPP Th17s cause Hypertension and Mitochondrial Dysfunction in the Kidney and Placenta during Pregnancy
30. Abstract 103: Il-33 Supplementation Improves Vascular Function And Maternal Hypertension In Response To Placental Ischemia
31. Proliferation of endogenous regulatory T cells improve the pathophysiology associated with placental ischaemia of pregnancy
32. Interleukin-4 supplementation improves the pathophysiology of preeclampsia in response to placental ischemia: 23
33. Continued Investigation Into 17-OHPC: Results From the Preclinical RUPP Rat Model of Preeclampsia
34. Chronic treatment with IL-25 increases renal M2 macrophages and reduces renal injury in obese Dahl salt-sensitive rats during the prepubescent stage.
35. Treatment with rapamycin reduces progressive proteinuria while inducing hyperglycemia in obese Dahl salt‐sensitive leptin‐receptor mutant rats prior to puberty
36. IL‐25 Supplementation Induces M2 Macrophage Polarization, Reduces Blood Pressure, and Improves Fetal Weight in Placental Ischemic Rats
37. NLRP3 Inhibition Improves Maternal Blood Pressure, Inflammation, and Vascular Function During Placental Ischemia
38. Decreasing Insulin Resistance Reduces Early Progressive Proteinuria by Decreasing Renal Hyperfiltration and Inflammation in Obese Dahl Salt‐Sensitive Rats
39. The SSLepR mutant rat represents a novel model to study obesity-induced renal injury before puberty
40. Placental CD4+ T cells from preeclamptic patients cause autoantibodies to the angiotensin II type I receptor and hypertension in a pregnant rat model of preeclampsia
41. Treatment With Lisinopril Prevents the Early Progression of Glomerular Injury in Obese Dahl Salt-Sensitive Rats Independent of Lowering Arterial Pressure
42. Sex differences in cardiovascular response to sepsis.
43. B2 cells contribute to hypertension and natural killer cell activation possibly via AT1-AA in response to placental ischemia.
44. Progesterone supplementation attenuates hypertension and the autoantibody to the angiotensin II type I receptor in response to elevated interleukin-6 during pregnancy
45. Characterization of Mitochondrial Bioenergetics in Preeclampsia
46. Progesterone Induced Blocking Factor Reduces Hypertension and Placental Mitochondrial Dysfunction in Response to sFlt-1 during Pregnancy
47. Platelet Inhibition Prevents NLRP3 Inflammasome Activation and Sepsis-Induced Kidney Injury
48. Abstract 42: Inhibiting Stimulatory Dendritic Cells Reduces Early Progressive Proteinuria In Obese Dahl Salt-sensitive Rats.
49. Abstract 31: Esomeprazole Improves Blood Pressure, Intrauterine Growth, Inflammation, And Vascular Function During Placental Ischemia Through Inhibition Of NLRP3
50. Abstract 26: IL-17 Causes Hypertension, Reduced Fetal Weight And Natural Killer Cell Activation In The Absence Of T Cells
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