从森林洋葱中鉴定新型功能化合物及其对乳腺癌的生物活性

IF 4.8 Q1 AGRICULTURE, MULTIDISCIPLINARY Journal of Agriculture and Food Research Pub Date : 2024-08-20 DOI:10.1016/j.jafr.2024.101362
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引用次数: 0

摘要

从天然资源中发现治疗肿瘤(如乳腺癌)的新分子,对功能食品的开发和制药业都具有重要意义。森林洋葱(Eleutherine bulbosa (Mill.) Urb.)是一种具有潜在抗乳腺癌活性的天然资源,但其活性成分的特性及其作用机制仍有待探索。因此,本研究的重点是代谢物分析、硅学或药理作用活性和机制,以及体外细胞系的高级验证。通过网络药理学和分子对接模拟,从鳞茎叶乙醇提取物(EBE)中鉴定出了 10 种化合物,这些化合物具有抑制癌症受体和自由基的活性。最有希望的化合物是阿芬甾醇,其与 PARP-1、HER2 和 iNOS 受体的结合值分别为 -11.26、-8.34 和 -9.17 μg/mL。在 ABTS 和 DPPH 自由基清除试验中,EBE 和阿伐那司醇的 EC50 值比对照抗氧化剂 Trolox 的 EC50 值更小,效力更高。EBE和venasterol对人类乳腺癌MCF-7细胞具有抗增殖活性(LD50为217.8 μg/mL),对正常MCF-10A细胞的细胞毒性相对较低(LD50为1000 μg/mL)。EBE 对 MCF-7 的抗增殖机制与 TGF-β、HER2、PI3K 和 AKT 的下调有关,而 TGF-β、HER2、PI3K 和 AKT 是已知的肿瘤激活因子。经 EBE 处理后,MCF-7 中的抑癌基因 miR-29a-3p 呈剂量依赖性显著上调(p < 0.05)。
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Identification of novel functional compounds from forest onion and its biological activities against breast cancer

The discovery of new molecules from natural sources for the treatment of tumors such as breast cancers is of importance for the development of functional foods and to the pharmaceutical industry. A natural resource with potential activity against breast cancer is forest onion, Eleutherine bulbosa (Mill.) Urb., but the identity of its active constituents and their mechanisms of action remain unexplored. Therefore, this study focuses on metabolite profiling, in silico or pharmacoinformatic activity and mechanisms, as well as advanced validation on in vitro cell lines. Ten compounds identified in E. bulbosa bulb ethanolic extract (EBE) showed cancer receptor and radical inhibitory activity via network pharmacology and molecular docking simulation. The most promising compound was avenasterol binding PARP-1, HER2, iNOS receptors with values of −11.26, −8.34, and −9.17 μg/mL, respectively. EBE and avenasterol had a smaller EC50 value, or higher potency, than the control antioxidant Trolox in radical scavenging tests with ABTS and DPPH. In line with the in silico study, EBE and avenasterol showed antiproliferative activity against human breast cancer MCF-7 with LD50 217.8 μg/mL, with relatively low cytotoxicity to normal MCF-10A cells (LD50 > 1000 μg/mL). The antiproliferative mechanism of EBE on MCF-7 was associated with downregulation of TGF-β, HER2, PI3K, and AKT which are known tumor activators. Significant (p < 0.05) upregulation of tumor suppressor gene miR-29a-3p in MCF-7 was observed after treatment with EBE in a dose-dependent manner.

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来源期刊
CiteScore
5.40
自引率
2.60%
发文量
193
审稿时长
69 days
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