Journal of experimental nephrology最新文献

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Toll-like receptor 3 signaling and human glomerular endothelial cells toll样受体3信号传导与人肾小球内皮细胞的关系

Journal of experimental nephrology

Pub Date : 2020-12-31 DOI: 10.46439/nephrology.1.002

引用次数: 0

In vitro analysis and cadaver feasibility study of a peritoneal dialysis catheter tungsten weighted anchor 腹膜透析置管钨重锚的体外分析及尸体可行性研究

Journal of experimental nephrology

Pub Date : 2020-12-31 DOI: 10.46439/nephrology.1.005

引用次数: 0

Usefulness to assess the disease progression and mortality risk profiles, in a population of chronic kidney disease patients followed by general practitioners and nephrologists 在全科医生和肾病学家随访的慢性肾病患者人群中评估疾病进展和死亡风险概况的有效性

Journal of experimental nephrology

Pub Date : 2020-12-31 DOI: 10.46439/nephrology.1.003

引用次数: 0

Beneficial effects of nicotinamide on hypertensive mice with impaired endothelial nitric oxide function 烟酰胺对内皮细胞一氧化氮功能受损的高血压小鼠的有益作用

Journal of experimental nephrology

Pub Date : 2020-08-26 DOI: 10.46439/nephrology.1.001

Phillip K Huynh, Jennifer C. Wilder, S. Hiller, J. Hagaman, N. Takahashi, Nobuyo Maeda-Smithies, Feng Li

Nicotinamide (Nam, amide form of niacin acid or nicotinate), a precursor for nicotinamide adenine dinucleotide (NAD+), is important for normal physiological function of organisms. Nam also suppresses mobilization of Ca2+ from sarcoplasmic reticulum into cytoplasm through inhibiting ADP-ribose cyclase. Previously, we have demonstrated that a pharmacological dose of Nam normalizes maternal blood pressure in mouse models of preeclampsia, a pregnancy related hypertensive disorder. We hypothesized that Nam could decrease blood pressure in hypertensive conditions unrelated to pregnancy. Nam at a dose of 500 mg/kg/day was given to wild type (WT) mice treated with L-NAME, endothelial nitric oxide synthase (eNOS)-null and renin transgenic (Renin-Tg) mice via drinking water. Blood pressure was measured by tail-cuff at different stages of treatment. The function and structure of kidneys of WT mice with L-NAME were determined at the end of the study. The gene expression of markers of inflammation and fibrosis in the kidneys of WT mice with L-NAME was also measured. Nam effectively prevented increase in blood pressure in L-NAME treated mice and decreased elevated blood pressure in eNOS-null mice. However, it did not alter high blood pressure in Renin-Tg mice. Nam prevented increase in urinary albumin excretion and collagen deposit in kidneys of WT mice treated with L-NAME. In addition, Nam significantly decreased the mRNA levels of the markers of inflammation and fibrosis in the kidneys of WT mice treated with L-NAME. Nam may execute beneficial effects on hypertensive conditions associated with eNOS dysfunction via suppressing inflammation. Because Nam is generally regarded as safe in humans, it merits further evaluation for the tailored treatment for the subgroup of hypertensive cases associated with impaired eNOS system.

烟酰胺(Nam，烟酸或烟酸的酰胺形式)是烟酰胺腺嘌呤二核苷酸(NAD+)的前体，对生物体的正常生理功能至关重要。Nam还通过抑制adp核糖环化酶抑制Ca2+从肌浆网进入细胞质的动员。在此之前，我们已经证明，在子痫前期(一种与妊娠相关的高血压疾病)的小鼠模型中，药物剂量的Nam可以使母体血压正常。我们假设Nam可以降低与妊娠无关的高血压患者的血压。以500 mg/kg/天的剂量，通过饮水给药给L-NAME处理的野生型(WT)小鼠、内皮型一氧化氮合酶(eNOS)缺失小鼠和肾素转基因(renin - tg)小鼠。在治疗的不同阶段用尾袖测量血压。研究结束时，对L-NAME小鼠肾脏的功能和结构进行了测定。同时检测L-NAME小鼠肾脏炎症和纤维化标志物的基因表达。Nam有效防止L-NAME处理小鼠血压升高，降低enos缺失小鼠血压升高。然而，它并没有改变肾素- tg小鼠的高血压。Nam阻止L-NAME处理的WT小鼠尿白蛋白排泄和肾脏胶原沉积的增加。此外，Nam显著降低了L-NAME处理的WT小鼠肾脏炎症和纤维化标志物的mRNA水平。Nam可能通过抑制炎症对eNOS功能障碍相关的高血压疾病产生有益作用。由于Nam通常被认为对人类是安全的，因此值得进一步评估其对与eNOS系统受损相关的高血压病例亚组的量身定制治疗。

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引用次数: 9

Beneficial effects of nicotinamide on hypertensive mice with impaired endothelial nitric oxide function. 烟酰胺对内皮细胞一氧化氮功能受损的高血压小鼠的有益作用。

Journal of experimental nephrology

Pub Date : 2020-01-01

Phillip K Huynh, Jen Wilder, Sylvia Hiller, John Hagaman, Nobuyuki Takahashi, Nobuyo Maeda-Smithies, Feng Li

Nicotinamide (Nam, amide form of niacin acid or nicotinate), a precursor for nicotinamide adenine dinucleotide (NAD+), is important for normal physiological function of organisms. Nam also suppresses mobilization of Ca²⁺ from sarcoplasmic reticulum into cytoplasm through inhibiting ADP-ribose cyclase. Previously, we have demonstrated that a pharmacological dose of Nam normalizes maternal blood pressure in mouse models of preeclampsia, a pregnancy related hypertensive disorder. We hypothesized that Nam could decrease blood pressure in hypertensive conditions unrelated to pregnancy. Nam at a dose of 500 mg/kg/day was given to wild type (WT) mice treated with L-NAME, endothelial nitric oxide synthase (eNOS)-null and renin transgenic (Renin-Tg) mice via drinking water. Blood pressure was measured by tail-cuff at different stages of treatment. The function and structure of kidneys of WT mice with L-NAME were determined at the end of the study. The gene expression of markers of inflammation and fibrosis in the kidneys of WT mice with L-NAME was also measured. Nam effectively prevented increase in blood pressure in L-NAME treated mice and decreased elevated blood pressure in eNOS-null mice. However, it did not alter high blood pressure in Renin-Tg mice. Nam prevented increase in urinary albumin excretion and collagen deposit in kidneys of WT mice treated with L-NAME. In addition, Nam significantly decreased the mRNA levels of the markers of inflammation and fibrosis in the kidneys of WT mice treated with L-NAME. Nam may execute beneficial effects on hypertensive conditions associated with eNOS dysfunction via suppressing inflammation. Because Nam is generally regarded as safe in humans, it merits further evaluation for the tailored treatment for the subgroup of hypertensive cases associated with impaired eNOS system.

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引用次数: 0

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