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正缬氨酸可降低遗传性应激性高血压大鼠的血压并诱导利尿。

Norvaline Reduces Blood Pressure and Induces Diuresis in Rats with Inherited Stress-Induced Arterial Hypertension.

机构信息

Scientific Research Institute of Physiology and Basic Medicine, 4 Timakova Street, Novosibirsk 630117, Russia.

Federal Scientific Center Institute of Cytology and Genetics, 6, Prosp. M. A. Lavrent'eva, Novosibirsk, Russia.

出版信息

Biomed Res Int. 2020 Feb 12;2020:4935386. doi: 10.1155/2020/4935386. eCollection 2020.

Abstract

Growing evidence suggests that increased arginase activity affects vital bioprocesses in various systems and universally mediates the pathogenesis of numerous metabolic diseases. The adverse effects of arginase are associated with a severe decline in L-arginine bioavailability, which leads to nitric oxide synthase substrate insufficiency, uncoupling, and, eventually, superoxide anion generation and substantial reduction of nitric oxide (NO) synthesis. In cooperation, it contributes to chronic oxidative stress and endothelial dysfunction, which might lead to hypertension and atherosclerosis. Recent preclinical investigations point arginase as a promising therapeutic target in ameliorating metabolic and vascular dysfunctions. In the present study, adult rats with inherited stress-induced arterial hypertension (ISIAH) were used as a model of hypertension. Wistar rats served as normotensive controls. Experimental animals were intraperitoneally administered for seven days with nonproteinogenic amino acid L-norvaline (30 mg/kg/day), which is a potent arginase inhibitor, or with the vehicle. Blood pressure (BP), body weight, and diuresis were monitored. The changes in blood and urine levels of creatinine, urea, and NO metabolites were analyzed. We observed a significant decline in BP and induced diuresis in ISIAH rats following the treatment. The same procedure did not affect the BP of control animals. Remarkably, the treatment had no influence upon glomerular filtration rate in two experimental groups, just like the daily excretion of creatinine and urea. Conversely, NO metabolite levels were amplified in normotonic but not in hypertensive rats following the treatment. The data indicate that L-norvaline is a potential antihypertensive agent and deserves to be clinically investigated. Moreover, we suggest that changes in blood and urine are causally related to the effect of L-norvaline upon BP regulation.

摘要

越来越多的证据表明,精氨酸酶活性的增加会影响各种系统中的重要生物过程,并普遍介导许多代谢疾病的发病机制。精氨酸酶的不良影响与 L-精氨酸生物利用度的严重下降有关,这导致一氧化氮合酶底物不足、解偶联,最终导致超氧阴离子生成和一氧化氮 (NO) 合成的大量减少。共同作用下,导致慢性氧化应激和内皮功能障碍,可能导致高血压和动脉粥样硬化。最近的临床前研究表明,精氨酸酶是改善代谢和血管功能障碍的有前途的治疗靶点。在本研究中,遗传性应激诱导动脉高血压(ISIAH)成年大鼠被用作高血压模型。Wistar 大鼠作为正常血压对照。实验动物连续七天腹腔内给予非蛋白氨基酸 L-正缬氨酸(30mg/kg/天),这是一种有效的精氨酸酶抑制剂,或给予载体。监测血压 (BP)、体重和尿量。分析血液和尿液中肌酐、尿素和 NO 代谢物水平的变化。我们观察到 ISIAH 大鼠在治疗后血压显著下降并诱导利尿。相同的程序对对照动物的血压没有影响。值得注意的是,该治疗对两组实验动物的肾小球滤过率没有影响,就像肌酐和尿素的日常排泄一样。相反,在治疗后,正常血压大鼠的 NO 代谢物水平升高,但高血压大鼠则不然。数据表明 L-正缬氨酸是一种潜在的抗高血压药物,值得临床研究。此外,我们认为血液和尿液中的变化与 L-正缬氨酸对血压调节的影响有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4fe8/7042509/3dcd4331f71e/BMRI2020-4935386.001.jpg

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