Shenyang Pharmaceutical University, Shenyang 110016, China.
Guangxi University of Chinese Medicine, Nanning 530200, China.
Bioorg Chem. 2019 Jul;88:102961. doi: 10.1016/j.bioorg.2019.102961. Epub 2019 Apr 29.
20(R)-25-methoxyl-dammarane-3β,12β,20-triol (AD-1, CN Patent: 201010107476.7) is a novel derivative of dammarane-type ginsenoside. AD-1 has been shown to inhibit cancer cell proliferation without significant host toxicity in vivo, and has excellent development potential as a new anti-cancer agent. This study was designed systematically to explore the metabolic pathway of ginseng sapogenins. The metabolism of drugs in the body is a complex biotransformation process where drugs are structurally modified to different molecules (metabolites) through various metabolizing enzymes. The compounds responsible for the effects of orally administered ginseng are believed to be metabolites produced in the gastrointestinal tract, so understanding the metabolism of the drug candidate can help to optimize its pharmacokinetics. In this study, faeces samples were collected and extracted after oral administration of AD-1. The 16 metabolites of AD-1 were isolated and identified for the first time with various chromatographic techniques, including semi-preparative high performance liquid chromatography, nuclear magnetic resonance spectroscopy, and mass spectrometry; of these 16 metabolites, 10 were novel compounds. We first discovered the biotransformation of dammarane-type sapogenins into oleanane-type sapogenins in rats and found a series of metabolites that changed, mainly at C-25 and C-29. This study provides new ideas for the metabolic pathway of ginseng sapogenins. The isolated compounds were screened for their effect on the viability and proliferation against cancer cell lines (Human A549, MCF-7, HELA, HO-8901 and U87). The discovery of novel active metabolites 3β,12β,21α,22β-Hydroxy-24-norolean-12-ene (M6) may lead to a new or improved drug candidate. For one, M6 could inhibit the growth of all the tested cancer cells. Among the tested cell lines, M6 exhibited the most remarkable inhibitory effect on ovarian cancer HO-8901 cells, with IC value of 2.086 μM. On this basis, we studied the anticancer mechanisms of M6. The results indicated that the pro-apoptotic feature of M6 acts via a mitochondrial pathway. Our results indicated that M6 exhibited a higher inhibitory effect on cancer-cell proliferation than AD-1 by inducing cell apoptosis. Our work provides data for future investigations on the metabolic mechanism of AD-1 in vivo and the potential for future research on developing a new drug.
20(R)-25-甲氧基达玛烷-3β,12β,20-三醇(AD-1,中国专利:201010107476.7)是一种新型达玛烷型人参皂苷衍生物。AD-1 在体内显示出抑制癌细胞增殖而没有明显的宿主毒性,作为一种新型抗癌药物具有极好的开发潜力。本研究系统地探索了人参皂甙的代谢途径。药物在体内的代谢是一个复杂的生物转化过程,药物通过各种代谢酶结构修饰为不同的分子(代谢物)。口服人参产生作用的化合物被认为是在胃肠道中产生的代谢物,因此了解候选药物的代谢情况有助于优化其药代动力学。在这项研究中,口服 AD-1 后收集并提取粪便样本。首次使用各种色谱技术,包括半制备高效液相色谱、核磁共振波谱和质谱,分离和鉴定了 AD-1 的 16 种代谢物;其中 10 种是新化合物。我们首次在大鼠中发现了达玛烷型皂甙转化为齐墩果烷型皂甙的生物转化,并发现了一系列发生变化的代谢物,主要在 C-25 和 C-29 位。这项研究为人参皂甙的代谢途径提供了新的思路。分离得到的化合物进行了活性筛选,以评估它们对癌细胞系(人 A549、MCF-7、HELA、HO-8901 和 U87)的活力和增殖的影响。新型活性代谢物 3β,12β,21α,22β-羟基-24-去甲齐墩烷-12-烯(M6)的发现可能导致新的或改进的候选药物。M6 可以抑制所有测试的癌细胞的生长。在测试的细胞系中,M6 对卵巢癌 HO-8901 细胞的抑制作用最为显著,IC 值为 2.086 μM。在此基础上,我们研究了 M6 的抗癌机制。结果表明,M6 通过线粒体途径发挥促凋亡作用。我们的结果表明,M6 通过诱导细胞凋亡对癌细胞增殖的抑制作用高于 AD-1。我们的工作为 AD-1 在体内的代谢机制和开发新药的潜在未来研究提供了数据。
