Antihypertensive effect of carvacrol is improved after incorporation in β‐cyclodextrin as a drug delivery system

硝普钠 药理学 苯肾上腺素 环糊精 化学 血压 抗高血压药 医学 一氧化氮 内科学 色谱法
作者
Liliane Barreto da Silva,Samuel Barbosa Camargo,Raiana dos Anjos Moraes,Carla Fiama de Azevedo Medeiros,Anderson de Melo Jesus,Afrânio Ferreira Evangelista,Cristiane Flora Villarreal,Lucindo José Quintans‐Júnior,Darízy Flávia Silva
出处
期刊:Clinical and Experimental Pharmacology and Physiology [Wiley]
卷期号:47 (11): 1798-1807 被引量:17
标识
DOI:10.1111/1440-1681.13364
摘要

Abstract Carvacrol (CARV), has been shown to possess various pharmacological properties, especially in the treatment of cardiovascular diseases. We evaluated the antihypertensive effect of the CARV free and encapsulation of CARV in β‐cyclodextrin (CARV/β‐CD), and whether CARV/β‐CD is able to improve the antihypertensive effects of CARV free in spontaneously hypertensive rats (SHR). The rats were randomly divided into four groups, each treated daily for 21 days and the mean arterial pressure and heart rate was measured every 5 days: group 1, Wistar‐vehicle solution; group 2, SHR‐vehicle; group 3, SHR‐CARV 50 mg/kg/d; and group 4, CARV/β‐CD 50 mg/kg/d. After 21 days of treatment, the mesenteric artery from treated animals was tested for phenylephrine (Phe) and sodium nitroprusside (SNP) sensitivity. In addition, administration of CARV/β‐CD induced important antihypertensive activity when compared with the uncomplexed form, reducing the progression of arterial hypertension in SHR. Moreover, pharmacological potency to Phe in the SHR‐CARV and CARV/β‐CD groups was increased, approaching values expressed in the Wistar‐vehicle. Furthermore, CARV/β‐CD reduced the production of the pro‐inflammatory mediator, IL‐1β, and increased anti‐inflammatory cytokine, IL‐10. Together, these results produced evidence that the encapsulation of CARV in β‐CD can improve cardiovascular activity, showing potential anti‐inflammatory and antihypertensive effects.

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