Acmella caulirhiza 的叶和花的水提取物通过降低某些基因的表达和激活 Caspase-3 来减少癌细胞的增殖

IF 3.4 Q2 BIOCHEMICAL RESEARCH METHODS Biochemistry Research International Pub Date : 2024-02-10 DOI:10.1155/2024/3293305
Huiny Miriane Tienoue Fotso, Mary-Ann Mbong Angie, F. Ntentie, Inelle Makamwe, Ferdinand Lanvin Edoun Ebouel, Emmerencia Kenjing Ndansack, Enyong Julius Oben
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引用次数: 0

摘要

癌症发病率的上升和癌症治疗的多种副作用促使研究人员不断寻找含有具有细胞死亡特性的生物活性化合物的植物。这项研究旨在评估 Acmella caulirhiza 提取物的抗增殖作用。通过清除 DPPH● 和 NO● 自由基,评估了三种 Acmella caulirhiza 提取物(水提取物 (AE-Ac)、水乙醇提取物 (HEE-Ac) 和乙醇提取物 (EE-Ac))的体外抗氧化潜力。随后,采用 MTT 法对乳腺癌(MCF-7)、脑癌(CT2A、SB-28 和 GL-261)、结肠癌(MC-38)和皮肤癌(YUMM 1.7 和 B16-F1)的细胞毒活性进行了评估。然后,选择提取物活性最强的癌株,通过 RT-PCR 法评估与癌症发生有关的某些基因的表达,并通过 Western 印迹法评估与细胞死亡机制有关的裂解 Caspase-3 的表达。AE-Ac 的清除活性最好,对 DPPH● 和 NO● 的 IC50 分别为 0.52 和 0.02。这种 AE-Ac 含有生物碱、黄酮类化合物和单宁酸,对 YUMM 1.7 细胞的活性更高(24 小时和 48 小时的 IC50 分别为 149.42 和 31.99 μg/mL)。结果还显示,AE-Ac能下调炎症基因(IL-1b p=0.017和IL-6 p=0.028)、生长因子(PDGF p=0.039、IGF p=0.034、E2F1p=0.038和E2F2p=0.016)和抗凋亡蛋白基因(Bcl-2 p=0.028和Bcl-6 p=0.039)的表达。AE-Ac能正向调节已裂解的caspase-3,从而诱导细胞凋亡。AE-Ac 对癌症进展相关基因的表达有抑制作用,因此是一种潜在的健康干预剂,可用于癌症治疗方案。
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Aqueous Extract of Leaves and Flowers of Acmella caulirhiza Reduces the Proliferation of Cancer Cells by Underexpressing Some Genes and Activating Caspase-3
The increasing prevalence of cancers and the multiple side effects of cancer treatments have led researchers to constantly search for plants containing bioactive compounds with cell death properties. This work aimed at evaluating the antiproliferative effect of an Acmella caulirhiza extract. After evaluation of the in vitro antioxidant potential of the three extracts of Acmella caulirhiza (aqueous (AE-Ac), hydroethanolic (HEE-Ac), and ethanolic (EE-Ac)) through the scavenging of DPPH● and NO● radicals, the extract with the best antioxidant activity was selected for bioactive compound assessment and antiproliferative tests. Subsequently, the cytotoxic activity was evaluated on the viability of breast (MCF-7), brain (CT2A, SB-28, and GL-261), colon (MC-38), and skin (YUMM 1.7 and B16-F1) cancer lines using the MTT method. Then, the line where the extract was the most active was selected to evaluate the expression of certain genes involved in cancerogenesis by RT-PCR and the expression of cleaved caspase-3 involved in cell death mechanism by western blot. The AE-Ac showed the best scavenging activity with IC50s of 0.52 and 0.02 for DPPH● and NO●, respectively. This AE-Ac was found to contain alkaloids, flavonoids, and tannins and was more active on YUMM 1.7 cells (IC50 = 149.42 and 31.99 μg/mL for 24 and 48 h, respectively). Results also showed that AE-Ac downregulated the expression of inflammation (IL-1b p=0.017 and IL-6 p=0.028), growth factors (PDGF p=0.039, IGF p=0.034, E2F1p=0.038, and E2F2p=0.016), and antiapoptotic protein genes (Bcl-2 p=0.028 and Bcl-6 p=0.039). The cleaved caspase-3 was positively modulated by the AE-Ac inducing thus cell death by apoptosis. AE-Ac showed inhibitory effects on the expression of genes involved in cancer progression making it a potential health intervention agent that can be exploited in cancer therapy protocols.
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来源期刊
Biochemistry Research International
Biochemistry Research International BIOCHEMICAL RESEARCH METHODS-
CiteScore
6.30
自引率
0.00%
发文量
27
审稿时长
14 weeks
期刊最新文献
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