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甘薯叶提取物中的极地生物酚类化合物协同抑制前列腺癌细胞增殖和体内肿瘤生长。

Polar biophenolics in sweet potato greens extract synergize to inhibit prostate cancer cell proliferation and in vivo tumor growth.

机构信息

Department of Biology and.

出版信息

Carcinogenesis. 2013 Sep;34(9):2039-49. doi: 10.1093/carcin/bgt141. Epub 2013 Apr 29.

DOI:10.1093/carcin/bgt141
PMID:23629419
Abstract

Polyphenolic phytochemicals present in fruits and vegetables indisputably confer anticancer benefits upon regular consumption. Recently, we demonstrated the growth-inhibitory and apoptosis-inducing properties of polyphenol-rich sweet potato greens extract (SPGE) in cell culture and in vivo prostate cancer xenograft models. However, the bioactive constituents remain elusive. Here, we report a bioactivity-guided fractionation of SPGE based upon differential solvent polarity using chromatographic techniques that led to the identification of a remarkably active polyphenol-enriched fraction, F5, which was ~100-fold more potent than the parent extract as shown by IC50 measurements in human prostate cancer cells. High-performance liquid chromatography-ultraviolet and mass spectrometric analyses of the seven SPGE fractions suggested varying abundance of the major phenols, quinic acid (QA), caffeic acid, its ester chlorogenic acid, and isochlorogenic acids, 4,5-di-CQA, 3,5-di-CQA and 3,4-di-CQA, with a distinct composition of the most active fraction, F5. Subfractionation of F5 resulted in loss of bioactivity, suggesting synergistic interactions among the constituent phytochemicals. Quantitative analyses revealed a ~2.6- and ~3.6-fold enrichment of QA and chlorogenic acid, respectively, in F5 and a definitive ratiometric relationship between the isochlorogenic acids. Daily oral administration of 400mg/kg body wt of F5 inhibited growth and progression of prostate tumor xenografts by ~75% in nude mice, as evidenced by tumor volume measurements and non-invasive real-time bioluminescence imaging. These data generate compelling grounds to further examine the chemopreventive efficacy of the most active fraction of SPGE and suggest its potential usefulness as a dietary supplement for prostate cancer management.

摘要

水果和蔬菜中存在的多酚类植物化学成分无疑能通过经常食用为人体带来抗癌益处。最近,我们在细胞培养和体内前列腺癌异种移植模型中证明了富含多酚的甘薯叶提取物(SPGE)的生长抑制和诱导细胞凋亡特性。然而,其生物活性成分仍不明确。在这里,我们报告了一种基于使用色谱技术的不同溶剂极性的 SPGE 生物活性导向分离,该技术导致了一个非常活跃的多酚富集部分 F5 的鉴定,F5 的效力比亲本提取物高约 100 倍,这通过在人前列腺癌细胞中的 IC50 测量来证明。对 SPGE 的七个部分的高效液相色谱-紫外和质谱分析表明,主要酚类物质、奎尼酸(QA)、咖啡酸、其酯绿原酸和异绿原酸、4,5-二-CQA、3,5-二-CQA 和 3,4-二-CQA 的丰度不同,最活跃的部分 F5 的组成也不同。F5 的亚部分分离导致生物活性丧失,表明组成植物化学成分之间存在协同相互作用。定量分析显示,F5 中 QA 和绿原酸的分别富集了约 2.6 倍和 3.6 倍,异绿原酸之间存在明确的比例关系。每日口服 400mg/kg 体重的 F5,通过肿瘤体积测量和非侵入性实时生物发光成像,在裸鼠中抑制了前列腺肿瘤异种移植物的生长和进展,抑制率约为 75%。这些数据为进一步研究 SPGE 最活跃部分的化学预防功效提供了令人信服的依据,并表明其作为前列腺癌管理膳食补充剂的潜在用途。

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