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首页> 美国卫生研究院文献>Integrated Blood Pressure Control >Chronic resveratrol reverses a mild angiotensin II-induced pressor effect in a rat model
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Chronic resveratrol reverses a mild angiotensin II-induced pressor effect in a rat model

机译:慢性白藜芦醇逆转大鼠模型中轻度血管紧张素II诱导的升压作用

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Resveratrol is reported to reduce blood pressure in animal models of hypertension, but the mechanisms are unknown. We have shown that resveratrol infusion increases sodium excretion. We hypothesized that chronic ingestion of resveratrol would reduce angiotensin II (Ang II)-induced increases in blood pressure by decreasing oxidative stress and by also decreasing sodium reabsorption through a nitric oxide-dependent mechanism. We infused rats with vehicle or 80 μg Ang II/d over 4 weeks. Vehicle or Ang II-infused rats were individually housed, pair fed, and placed on a diet of normal chow or normal chow plus 146 mg resveratrol/d. Groups included 1) control, 2) resveratrol-fed, 3) Ang II-treated, and 4) Ang II plus resveratrol. Systolic blood pressure was measured by tail cuff. During the 4th week, rats were placed in metabolic caging for urine collection. NO2/NO3 and 8-isoprostane excretion were measured. Ang II increased systolic blood pressure in the 1st week by +14±5 mmHg (P<0.05) in Group 3 and +10±3 mmHg (P<0.05) in Group 4, respectively. Blood pressure was unchanged in Groups 1 and 2. After 4 weeks, blood pressure remained elevated in Group 3 rats with Ang II (+9±3 mmHg, P<0.05), but in Group 4, blood pressure was no longer elevated (+2±2 mmHg). We found no significant differences between the groups in sodium excretion or cumulative sodium balance (18.49±0.12, 17.75±0.16, 17.97±0.17, 18.46±0.18 μEq Na+/7 d in Groups 1–4, respectively). Urinary excretion of NO2/NO3 in the four groups was 1) 1631±207 μmol/24 h, 2) 1045±236 μmol/24 h, 3) 1490±161 μmol/24 h, and 4) 609±17 μmol/24 h. 8-Isoprostane excretion was 1) 63.85±19.39 nmol/24 h, 2) 73.57±22.02 nmol/24 h, 3) 100.69±37.62 nmol/24 h, and 4) 103.00±38.88 nmol/24 h. We conclude that chronic resveratrol supplementation does not blunt Ang II-increased blood pressure, and while resveratrol has mild depressor effects, these do not seem to be due to natriuresis or enhanced renal nitric oxide synthesis.
机译:据报道,在高血压动物模型中,白藜芦醇可以降低血压,但其机制尚不清楚。我们已经证明白藜芦醇输注会增加钠排泄。我们假设长期摄入白藜芦醇可通过减少氧化应激并通过一氧化氮依赖性机制减少钠的重吸收来减少血管紧张素II(Ang II)引起的血压升高。我们在4周内给大鼠注入了媒介物或80μgAng II / d。将单独注入媒介物或Ang II的大鼠圈养,成对喂食并置于正常食物或正常食物加146 mg白藜芦醇/ d的饮食中。组包括1)对照组,2)白藜芦醇-喂养,3)Ang II-治疗的和4)Ang II加白藜芦醇。通过尾袖测量收缩压。在第4周,将大鼠置于代谢笼中以收集尿液。测量了NO2 / NO3和8-异前列腺素的排泄量。第3组的Ang II在第1周的收缩压分别增加+ 14±5 mmHg(P <0.05)和第4组的+ 10±3 mmHg(P <0.05)。第1组和第2组的血压没有变化。4周后,Ang II组的Ang II大鼠的血压仍然升高(+ 9±3 mmHg,P <0.05),而第4组的血压不再升高(+ 2±2毫米汞柱)。我们发现两组之间的钠排泄或累积钠平衡无显着差异(第1-4组中分别为18.49±0.12、17.75±0.16、17.97±0.17、18.46±0.18μEqNa + / 7 d)。四组中NO2 / NO3的尿排泄分别为1)1631±207μmol/ 24 h,2)1045±236μmol/ 24 h,3)1490±161μmol/ 24 h和4)609±17μmol/ 24 H。 8-异前列腺素排泄为1)63.85±19.39 nmol / 24 h,2)73.57±22.02 nmol / 24 h,3)100.69±37.62 nmol / 24 h,和4)103.00±38.88 nmol / 24 h。我们得出的结论是,长期补充白藜芦醇不会抑制Ang II升高的血压,尽管白藜芦醇具有轻度的降压作用,但这些似乎不是由于利钠或肾脏一氧化氮合成增强。

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