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橄榄油成分对 C 反应蛋白的影响:计算机模拟证据。

Impact of Olive Oil Constituents on C-reactive Protein: In silico Evidence.

机构信息

Faculty of Medicine & Health Sciences, Universiti Malaysia Sarawak.

Department of Clinical Pharmacy, College of Pharmacy, Jouf University.

出版信息

J Oleo Sci. 2022;71(8):1199-1206. doi: 10.5650/jos.ess22008.

DOI:10.5650/jos.ess22008
PMID:35922932
Abstract

Pain is a sensation a humans sense as a protective mechanism against physical injury. This sensation is closely related to inflammation. It ranges from mild to highly obnoxious. It is well-known that the levels of the inflammatory biomarker, C-reactive protein (CRP), increase manifold in acute inflammation and pain. Olive oil, known to have many phytochemicals, has been traditionally used to alleviate pain. Amongst major phenolic compounds in olive oil are oleuropein (OLE), hydroxytyrosol (HT), tyrosol, and oleocanthal. Whether the analgesic and anti-inflammatory properties in olive oil are due to any specific interections is not known. Therefore, this study aimed to elucidate the possible anti-inflammatory and anti-nociceptive properties in those major phenolic compounds by using molecular docking software MOE 2015, comparing the energy value and binding site of phenolic compounds to that of well-known synthetic non-steroidal anti-inflammatory drugs (NSAIDs) and phosphocholine. The docking experiment showed that all compounds could directly interact with CRP. Oleuropein had the most potent interaction with CRP (-7.7580), followed by indomethacin (-6.0775), oleocanthal (-5.5734), ibuprofen (-5.3857), phosphocholine (-4.3876), HT (-4.2782), and tyrosol (-4.2329). Interestingly, the present study found other phytochemicals in olive oil that can be exploited as potential, safe, and cost-effective lead compound(s) for analgesic and anti-inflammatory activity, as supported by its molecular docking data.

摘要

疼痛是人类感知到的一种保护机制,用于防止身体受伤。这种感觉与炎症密切相关。疼痛的程度从轻微到非常强烈不等。众所周知,炎症生物标志物 C 反应蛋白 (CRP) 的水平在急性炎症和疼痛中会大幅增加。橄榄油含有许多植物化学物质,传统上被用于缓解疼痛。橄榄油中的主要酚类化合物包括橄榄苦苷 (OLE)、羟基酪醇 (HT)、酪醇和油橄榄苦苷。橄榄油中的镇痛和抗炎特性是否由于任何特定的相互作用尚不清楚。因此,本研究旨在使用分子对接软件 MOE 2015 阐明这些主要酚类化合物中可能具有的抗炎和镇痛特性,比较酚类化合物与已知的合成非甾体抗炎药 (NSAIDs) 和磷酸胆碱的能量值和结合位点。对接实验表明,所有化合物都可以直接与 CRP 相互作用。橄榄苦苷与 CRP 的相互作用最强 (-7.7580),其次是吲哚美辛 (-6.0775)、油橄榄苦苷 (-5.5734)、布洛芬 (-5.3857)、磷酸胆碱 (-4.3876)、HT (-4.2782) 和酪醇 (-4.2329)。有趣的是,本研究发现橄榄油中的其他植物化学物质也可以作为潜在的、安全的、具有成本效益的镇痛和抗炎活性的先导化合物,这得到了其分子对接数据的支持。

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