Mahmoud Ali M, Aboul-Soud Mourad A M, Han Junkyu, Al-Sheikh Yazeed A, Al-Abd Ahmed M, El-Shemy Hany A
Department of Biochemistry, Faculty of Agriculture, Cairo University, Giza 12613, Egypt.
Graduate School of Life and Environmental Sciences, University of Tsukuba, Tsukuba, Ibaraki 305‑8572, Japan.
Int J Oncol. 2016 May;48(5):1886-94. doi: 10.3892/ijo.2016.3418. Epub 2016 Mar 4.
The merging of high-throughput gene expression techniques, such as microarray, in the screening of natural products as anticancer agents, is considered the optimal solution for gaining a better understanding of the intervention mechanism. Red yeast rice (RYR), a Chinese dietary product, contains a mixture of hypocholesterolemia agents such as statins. Typically, statins have this effect via the inhibition of HMG‑CoA reductase, the key enzyme in the biosynthesis of cholesterol. Recently, statins have been shown to exhibit various beneficial antineoplastic properties through the disruption of tumor angiogenesis and metastatic processes. Mevinolin (MVN) is a member of statins and is abundantly present in RYR. Early experimental trials suggested that the mixed apoptotic/necrotic cell death pathway is activated in response to MVN exposure. In the current study, the cytotoxic profile of MVN was evaluated against MCF‑7, a breast cancer‑derived cell line. The obtained results indicated that MVN‑induced cytotoxicity is multi‑factorial involving several regulatory pathways in the cytotoxic effects of MVN on breast cancer cell lines. In addition, MVN‑induced transcript abundance profiles inferred from microarrays showed significant changes in some key cell processes. The changes were predicted to induce cell cycle arrest and reactive oxygen species generation but inhibit DNA repair and cell proliferation. This MVN‑mediated multi‑factorial stress triggered specific programmed cell death (apoptosis) and DNA degradation responses in breast cancer cells. Taken together, the observed MVN‑induced effects underscore the potential of this ubiquitous natural compound as a selective anticancer activity, with broad safety margins and low cost compared to benchmarked traditional synthetic chemotherapeutic agents. Additionally, the data support further pre‑clinical and clinical evaluations of MVN as a novel strategy to combat breast cancer and overcome drug resistance.
将高通量基因表达技术(如微阵列)应用于天然产物作为抗癌剂的筛选中,被认为是更好地理解干预机制的最佳解决方案。红曲米(RYR)是一种中国膳食产品,含有他汀类等降胆固醇药物的混合物。通常,他汀类药物通过抑制HMG-CoA还原酶(胆固醇生物合成中的关键酶)来发挥这种作用。最近,他汀类药物已被证明通过破坏肿瘤血管生成和转移过程而表现出各种有益的抗肿瘤特性。美伐他汀(MVN)是他汀类药物的一种,大量存在于红曲米中。早期实验表明,暴露于MVN会激活混合的凋亡/坏死细胞死亡途径。在本研究中,评估了MVN对MCF-7(一种乳腺癌衍生细胞系)的细胞毒性特征。所得结果表明,MVN诱导的细胞毒性是多因素的,涉及MVN对乳腺癌细胞系细胞毒性作用中的几个调节途径。此外,从微阵列推断出的MVN诱导的转录本丰度谱显示,一些关键细胞过程发生了显著变化。这些变化预计会诱导细胞周期停滞和活性氧生成,但会抑制DNA修复和细胞增殖。这种MVN介导的多因素应激在乳腺癌细胞中引发了特定的程序性细胞死亡(凋亡)和DNA降解反应。综上所述,观察到的MVN诱导的效应强调了这种普遍存在的天然化合物作为一种具有选择性抗癌活性的潜力,与基准传统合成化疗药物相比,具有广泛的安全范围和低成本。此外,这些数据支持对MVN进行进一步的临床前和临床评估,作为对抗乳腺癌和克服耐药性的新策略。
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