消旋草对 MDA-MB 231 三阴性乳腺癌的细胞毒性特性、糖酵解效应和高分辨率呼吸测定线粒体活性。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Francis Adu-Amankwaah, Candice Februarie, Kudakwashe Nyambo, Gerald Maarman, Ndivhuwo Tshililo, Lawrence Mabasa, Vuyo Mavumengwana, Lucinda Baatjies
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引用次数: 0

摘要

导言:由于三阴性乳腺癌(TNBC)对传统疗法具有抗药性,而且缺乏特异性分子靶点,因此它代表着一个重大的全球健康危机。本研究探索了外消旋草(E. racemosus)作为 TNBC 替代疗法的潜力。方法:对E. racemosus进行正己烷溶剂萃取和生物活性馏分萃取,并使用基于质谱的代谢物分析鉴定萃取物中的植物化学成分。提取物还针对 MDA-MB 231 TNBC 细胞进行了测试,以确定其细胞毒性。细胞死亡的模式是通过流式细胞术确定的。使用多重活性检测试剂盒评估了 Caspases 3、8 和 9 的活性。使用 Seahorse XFp 和 Oroboros O2K 对 MDA-MB 231 细胞系的糖酵解活性和线粒体功能进行了高分辨率呼吸测量:结果:对E. racemosus植物粗提取物进行的代谢物分析确定了香豆素、黄酮类、倍半萜类、三萜类和未知化合物的存在。提取物显示出良好的细胞毒性活性,粗己烷提取物的半最大抑制浓度(IC50)为 12.84 µg/mL,生物活性部分为 15.49 µg/mL。此外,与未经处理的细胞相比,粗己烷提取物和生物活性馏分提取物与参考药物顺铂一样能诱导 MDA-MB-231 TNBC 细胞凋亡(分别为 17.44%、17.26% 和 20.25%)。Caspase 3 活性证实了顺铂和植物粗提取物都能诱导细胞凋亡,而 Caspase 8 和 9 活性则证实了内源性和外源性细胞凋亡途径都被激活。在正己烷粗萃取物中观察到糖酵解活性水平升高。高分辨率呼吸测量显示,除复合体-IV 活性外,所有线粒体状态下的线粒体活性都升高:这些研究结果支持进一步探索外消旋山豆根作为 TNBC 潜在治疗药物的可能性,为开发不良反应最小的靶向治疗方法提供了前景广阔的途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cytotoxic properties, glycolytic effects and high-resolution respirometry mitochondrial activities of Eriocephalus racemosus against MDA-MB 231 triple-negative breast cancer.

Introduction: Triple-negative breast cancer (TNBC) represents a significant global health crisis due to its resistance to conventional therapies and lack of specific molecular targets. This study explored the potential of Eriocephalus racemosus (E. racemosus) as an alternative treatment for TNBC. The cytotoxic properties and high-resolution respirometry mitochondrial activities of E. racemosus against the MDA-MB 231 TNBC cell line were evaluated.

Methods: Hexane solvent and bioactive fraction extractions of E. racemosus were performed, while mass spectrometry-based metabolite profiling was used to identify the phytochemical constituents of the extracts. The extracts were further tested against MDA-MB 231 TNBC cells to determine their cytotoxicity. The mode of cell death was determined using flow cytometry. The activities of caspases 3, 8, and 9 were assessed using a multiplex activity assay kit. Glycolytic activity and High-resolution respirometry measurements of mitochondrial function in the MDA-MB 231 cell line were conducted using the Seahorse XFp and Oroboros O2K.

Results: Metabolite profiling of E. racemosus plant crude extracts identified the presence of coumarins, flavonoids, sesquiterpenoids, triterpenoids, and unknown compounds. The extracts demonstrated promising cytotoxic activities, with a half maximal inhibitory concentration (IC50) of 12.84 µg/mL for the crude hexane extract and 15.49 µg/mL for the bioactive fraction. Further, the crude hexane and bioactive fraction extracts induced apoptosis in the MDA-MB-231 TNBC cells, like the reference drug cisplatin (17.44%, 17.26% and 20.25%, respectively) compared to untreated cells. Caspase 3 activities confirmed the induction of apoptosis in both cisplatin and the plant crude extracts, while caspase 8 and 9 activities confirmed the activation of both the intrinsic and extrinsic apoptosis pathways. Increased levels of glycolytic activity were observed in the hexane crude extract. High-resolution respiratory measurements showed elevated mitochondrial activities in all mitochondrial states except for complex-IV activity.

Conclusion: These findings support further exploration of E. racemosus as a potential therapeutic agent for TNBC, offering a promising avenue for the development of targeted treatments with minimal adverse effects.

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CiteScore
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