甜罗勒(Ocimum basilicum L.)提取物中6种主要化合物抗高血压作用的分子对接分析

Bayu Cakra Buana, I. Iksen, K. Gurning
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摘要

高血压是一种异常高的血压状况,是可预防的心血管疾病、慢性肾脏疾病和认知障碍的主要原因。在高血压的情况下,抑制血管紧张素转换酶(ACE)的表达已被证明是通过抑制血管紧张素I向血管紧张素II的转化来控制高血压的有效方法。卡托普利是最常用的ACE抑制剂。它同时抑制血管紧张素I向强效血管收缩剂血管紧张素II和血管舒张肽缓激肽的转化。另一方面,甜罗勒(Ocimum basilicum L.)在传统的印度和中国医学中用于治疗多种疾病,包括高血压。该研究旨在调查甜罗勒(Ocimum basilicum L.)提取物中发现的6种主要化合物的效力,作为抗高血压疗法。分析表明,罗勒提取物含有多种可与ACE相互作用并抑制其活性的化合物,是一种有效的抗高血压药物。分子对接分析和药物相似性预测表明,樟脑不违反Lipinski规则,具有高胃肠道吸收,与ACE具有高亲和力,与ACE-卡托普利相互作用的相互作用位点相似,可能是潜在的候选药物。
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Molecular docking analysis of six major compounds from sweet basil (Ocimum basilicum L.) extract as potential anti-hypertension therapy
Hypertension is an abnormally high blood pressure condition that is the leading cause of preventable cardiovascular disease, chronic kidney disease, and cognitive impairment. In the case of hypertension, repressing the Angiotensin-Converting Enzyme (ACE) expression has been shown to be an effective method of controlling hypertension by inhibiting the conversion of angiotensin I to angiotensin II. Captopril is the most commonly used ACE inhibitor. It simultaneously inhibits the conversion of angiotensin I to the potent vasoconstrictor angiotensin II and the vasodilator peptide bradykinin. Sweet basil (Ocimum basilicum L.) on the other hand, is used in traditional Indian and Chinese medicine to treat a variety of diseases, including hypertension. The study aimed attempts to investigate the potency of 6 major compounds found in sweet basil (Ocimum basilicum L.) extract, as an anti-hypertension therapy. The analysis demonstrates that Ocimum basilicum L., extract is effective as an anti-hypertension therapy because it contains several compounds that may interact with ACE and inhibit its activity. The molecular docking analysis and drug-likeness prediction indicate that camphor could be a potential drug candidate because it does not violate the Lipinski rule, has a high Gastrointestinal (GI) absorption, a high affinity to interact with ACE, and a similar interaction site to the ACE-Captopril interaction.
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