顺势疗法母酊剂:代谢组学和抗肿瘤活性

M. N. O. Melo, A. P. Oliveira, R. Garrett, P. Zancan, A. C. Ochioni, Mirio Grazi, H. Ramm, T. Jaeger, S. Baumgartner, C. Holandino
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摘要

背景:粘属植物是一种具有抗肿瘤活性的半寄生植物。然而,欧洲野牡丹乙醇提取物(VAE)在肿瘤模型中也显示出体外活性。目的:通过二维和三维模型评价50种夏冬季节收获的VAE的代谢特征及其抗肿瘤活性。方法:采用浸渍法制备VAE。在家槐、栎属和榆属上生长;V.相册子;源自西尔维斯特松的奥地利松;V.相册子;冷杉病源自白冷杉。化学分析采用液相色谱-高分辨率质谱联用,偏最小二乘判别分析(PLS-DA)在Metaboanalyst 4.0中进行。通过MTT、结晶紫和糖酵解途径分析,在二维和三维模型(MDA-MB-231癌细胞)中评价所选VAE的抗肿瘤潜力。结果与讨论:PLS-DA的前3个主成分分别解释了正、负模式下数据变化的60%和40%。不同亚种间形成了3个类群,并表现出化学相似性。初步鉴定为:pinobankasin或柚皮苷己糖;异鼠李素-3-己糖苷,葡萄糖醇和不同的氨基酸。夏用0.5% v/v的VAE诱导的细胞毒损伤高于冬用0.5% v/v的VAE,在3D模型(72h)中,冷杉和栎树的肿瘤存活率分别降低49%和42%。2D模型的MDA-MB-231糖酵解途径显示葡萄糖消耗和细胞外乳酸生成减少。在孵育48h时,冷杉和栎树可抑制6-磷酸果糖激酶(PFK)和丙酮酸激酶(PK)活性。结论:VAE提取物具有不同的代谢组,糖酵解途径可能是其抑制肿瘤生长的重要靶点。
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Viscum album L. homeopathic mother tinctures: Metabolome and antitumor activity
Background: Viscum album L. is a semi-parasitic plant with antitumor activity attributed to the aqueous extracts. However, European V. album ethanolic extracts (VAE) have also demonstrated in vitro activity in tumor models. Aims: Evaluate the metabolic profiles of fifty VAE harvested during summer and winter seasons and their antitumor activity through 2D and 3D models. Methodology: VAE were prepared by maceration from: V. album subsp. album growing on Malus domestica, Quercus sp.     and Ulmus sp.; V. album subsp. austriacum from Pinus sylvestris; V. album subsp. abietis from Abies alba. Chemical analyses were performed through liquid chromatography coupled with high resolution mass spectrometry and Partial Least Squares Discriminant Analysis (PLS-DA) was performed in the Metaboanalyst 4.0. The antitumor potential of the selected VAE was evaluated in 2D and 3D models (MDA-MB-231 cancer cells) by MTT, crystal violet and glycolytic pathway analysis. Results and discussion: The first 3 principal components in PLS-DA explained 60% and 40% of data variation in positive and negative modes respectively. Three groups were formed and showed chemical similarity among V. album subspecies. The compounds responsible for group separation were tentatively identified as: pinobankasin or naringenin hexoside; isorhamnetin-3-hexoside, meglutol and different amino acids. The summer VAE at 0.5% v/v induced higher cytotoxic damage than the winter preparations, and Abies alba and Quercus sp. VAE promoted 49% and 42% reduction of tumor viability in 3D model (72h incubation), respectively. MDA-MB-231 glycolytic pathway in 2D model showed a decrease in the glucose consumption and extracellular lactate production. Also, PFK (6- phosphofructo-1-kinase) and PK (Pyruvate kinase) activities were inhibited by Abies alba and Quercus sp. VAE at 48h of incubation. Conclusion: VAE extracts showed different metabolomes and the glycolytic pathway should be an important target involved in the inhibition of tumor growth by these extracts.
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