Antiangiogenic and Anticancer Potential of Supercritical Fluid Extracts from Nutmeg Seeds; In vitro, Ex vivo and In silico studies

Journal of Angiotherapy Pub Date : 2023-11-14 DOI:10.25163/angiotherapy.719371

Sawsan S. Al-Rawi, Ahmad Hamdy, Marthad A. Hamde, Dinesh Babu, Mansoureh Nazari, Mohd Omar, Ab Kadir, Aman Shah, Abdul Majid, Amin Malik Shah

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Abstract

Background: Angiogenesis is a vital process of forming new blood vessels that occurs during several normal physiological processes. It plays a substantial role in tumor growth and cancer by supplying oxygen and nutrients for the proliferating tumors. Nutmeg, the dried seed of Myristica fragrans, is known for its therapeutic properties. This study aimed to investigate the antiangiogenic and cytotoxic properties of nutmeg extracts derived by Soxhlet and supercritical fluid extraction (SFE) using in-vitro, ex-vivo, and in-silico studies. Method: Nutmeg anticancer property was evaluated against breast cancer cell MCF7 and colon cancer cell HCT116 using MTT in-vitro assay. The antiangiogenic property was investigated using 3D ex-vivo rat aorta assays. The chemical composition of nutmeg extract was characterized using GC/TOF-MS. Subsequently, the main compounds in the nutmeg extract were analyzed against the angiogenesis-associated molecules (COX-1, VEGFA, HIF, and EGF) by molecular docking and were compared with tamoxifen and 5-fluorouracil. Results: The SFE extracts exhibited higher antiangiogenic properties than the Soxhlet (IC50 31µg/mL). Nutmeg SFE extract exhibited higher cytotoxicity towards HCT116 than MCF7 cells. Several active compounds, including myristicin, eugenol, safrole, and α-asarone were identified in the nutmeg SFE extracts using GC/TOF-MS. Molecular docking revealed strong interactions between these compounds and angiogenesis molecular mediators. Particularly, myristicin blocked COX-1, VEGFA, HIF, and EGF enzymes, indicating possible binding interactions. Conclusion: This study highlights the limitless possibilities of nature's offerings in advancing human health. Nutmeg's potential compounds lie in their binding models, which have proven to be powerful tools against cancer and angiogenesis. Myristicin, α-asarone, safrole, and eugenol work synergistically to induce antiangiogenic effects, making nutmeg a promising natural source of angiogenesis inhibitors for future anticancer therapies. The Molecular docking result confirmed that the inhibition of COX-1, VEGF-A, HIF, and EGF by nutmeg compounds offers great potential in the treatment and prevention of various angiogenesis diseases.

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肉豆蔻籽超临界流体提取物的抗血管生成和抗癌潜力；体外、体内和硅学研究

背景：血管生成是在多个正常生理过程中形成新血管的重要过程。它通过为增殖的肿瘤提供氧气和营养物质，在肿瘤生长和癌症中发挥着重要作用。肉豆蔻是肉豆蔻的干燥种子，因其治疗特性而闻名。本研究旨在通过体内、体外和微观研究，探讨通过索氏提取法和超临界流体萃取法提取的肉豆蔻提取物的抗血管生成和细胞毒性特性。方法：使用 MTT 体外检测法评估肉豆蔻对乳腺癌细胞 MCF7 和结肠癌细胞 HCT116 的抗癌特性。使用三维体外大鼠主动脉试验研究了肉豆蔻的抗血管生成特性。使用 GC/TOF-MS 对肉豆蔻提取物的化学成分进行了表征。随后，通过分子对接分析了肉豆蔻提取物中的主要化合物与血管生成相关分子（COX-1、VEGFA、HIF 和 EGF）的关系，并与他莫昔芬和 5-氟尿嘧啶进行了比较。结果显示SFE提取物的抗血管生成特性高于索氏提取物（IC50为31微克/毫升）。肉豆蔻 SFE 提取物对 HCT116 细胞的细胞毒性高于 MCF7 细胞。利用 GC/TOF-MS 鉴定了肉豆蔻 SFE 提取物中的几种活性化合物，包括肉豆蔻苷、丁香酚、黄樟脑和 α-asarone。分子对接显示，这些化合物与血管生成分子介质之间存在很强的相互作用。尤其是肉豆蔻苷能阻断 COX-1、VEGFA、HIF 和 EGF 酶，表明可能存在结合相互作用。结论这项研究强调了大自然提供的促进人类健康的无限可能性。肉豆蔻的潜在化合物在于它们的结合模型，这些模型已被证明是对抗癌症和血管生成的有力工具。肉豆蔻苷、α-asarone、黄樟素和丁香酚协同作用，诱导抗血管生成效应，使肉豆蔻成为未来抗癌疗法中一种前景广阔的血管生成抑制剂天然来源。分子对接结果证实，肉豆蔻化合物对 COX-1、VEGF-A、HIF 和 EGF 的抑制作用为治疗和预防各种血管生成疾病提供了巨大的潜力。

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Journal of Angiotherapy

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