Blood pressure-lowering and cardiovascular effects of plumbagin in rats: An insight into the underlying mechanisms

Q2 Agricultural and Biological Sciences

Current Research in Pharmacology and Drug Discovery Pub Date : 2022-01-01 DOI:10.1016/j.crphar.2022.100139

Maira Ahmad, Taseer Ahmad, Hafiz Muhammad Irfan, Nabeela Noor

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Abstract

Background

Plumbagin, a natural phenolic compound is investigated for response against blood pressure and vascular reactivity.

Methodology

Blood pressure lowering effects were observed by in-vivo invasive evaluation in normotensive rats, and in-vitro experimentation to measure changes of tension in isolated rat aorta and contractility in atria.

Results

The percentage decrease in mean arterial pressure (MAP) observed with plumbagin intravenously at doses of 0.1, 0.5, 1, 5, 10 μg/kg in normotensive rats was 7.16 ± 2.35, 15.5 ± 5.62, 19.5 ± 5.27, 26 ± 6.67, 34.33 ± 8.80, respectively. Plumbagin exerted vasorelaxant effects in rat aorta, unaffected by the removal of vascular endothelium, and _L-NAME and methylene blue pretreatment. Plumbagin completely inhibited phenylephrine (1 μM) and High K⁺ (80 mM) induced contractions. Similar to a Ca⁺² channel antagonist, plumbagin caused a rightward shift in the Ca⁺² concentration-response-curves (CRCs), resembling nifedipine. Pre-incubation with plumbagin, significantly suppressed contractions induced by phenylephrine in Ca⁺²-free medium via disrupting Ca⁺² release from intracellular stores. No change in vasorelaxant response was observed with the addition of potassium channel blockers, TEA and BaCl₂. In rat atrial strips, plumbagin exerted significant negative inotropic and chronotropic effects. No significant change was observed with atropine and atenolol pretreatment, so the effect appeared independent of muscarinic and beta-adrenergic receptors.

Conclusion

This study suggests the blood pressure lowering effects of plumbagin. That could be contributed by a decrease in vascular resistance via calcium antagonism, interferences in calcium efflux, and depressive effects on the rate and force of cardiac contraction. Further studies would be necessary to probe deeper into the underlying mechanisms.

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白桦素对大鼠的降血压和心血管作用:对潜在机制的洞察

作为一种天然酚类化合物，白桦素被研究用于降低血压和血管反应性。方法采用血压正常大鼠体内有创性降压实验和离体大鼠主动脉张力及心房收缩力变化的体外实验观察降压效果。结果0.1、0.5、1、5、10 μg/kg对正常大鼠平均动脉压(MAP)的降低率分别为7.16±2.35、15.5±5.62、19.5±5.27、26±6.67、34.33±8.80。白桦素对大鼠主动脉有血管松弛作用，不受血管内皮去除、L-NAME和亚甲基蓝预处理的影响。白桦素完全抑制1 μM的苯肾上腺素和80 mM的高K+诱导的收缩。与Ca+2通道拮抗剂类似，白杨苷引起Ca+2浓度-反应曲线(CRCs)向右移动，类似硝苯地平。在无Ca+2的培养基中，用白桦素预先孵育，通过破坏细胞内Ca+2的释放，显著抑制苯肾上腺素引起的收缩。在加入钾通道阻滞剂、TEA和BaCl2后，血管松弛反应没有变化。在大鼠心房条带中，白桦素具有显著的负性肌力和变时作用。阿托品和阿替洛尔预处理未见明显变化，因此其作用与毒蕈碱受体和β -肾上腺素能受体无关。结论白桦素具有明显的降血压作用。这可能是由于钙拮抗作用降低血管阻力，干扰钙外排，抑制心脏收缩的速度和力量。有必要进行进一步的研究，以更深入地探讨其潜在机制。

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