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黄花蒿次生代谢产物对癌细胞的细胞毒性活性与其指定活性成分青蒿素的比较。

Cytotoxic activity of secondary metabolites derived from Artemisia annua L. towards cancer cells in comparison to its designated active constituent artemisinin.

机构信息

Department of Pharmaceutical Biology, Institute of Pharmacy and Biochemistry, University of Mainz, Mainz, Germany.

出版信息

Phytomedicine. 2011 Aug 15;18(11):959-69. doi: 10.1016/j.phymed.2011.06.008. Epub 2011 Aug 9.

DOI:10.1016/j.phymed.2011.06.008
PMID:21831619
Abstract

Artemisia annua L. (sweet wormwood, qinhao) has traditionally been used in Chinese medicine. The isolation of artemisinin from Artemisia annua and its worldwide accepted application in malaria therapy is one of the showcase success stories of phytomedicine during the past decades. Artemisinin-type compounds are also active towards other protozoal or viral diseases as well as cancer cells in vitro and in vivo. Nowadays, Artemisia annua tea is used as a self-reliant treatment in developing countries. The unsupervised use of Artemisia annua tea has been criticized to foster the development of artemisinin resistance in malaria and cancer due to insufficient artemisinin amounts in the plant as compared to standardized tablets with isolated artemisinin or semisynthetic artemisinin derivatives. However, artemisinin is not the only bioactive compound in Artemisia annua. In the present investigation, we analyzed different Artemisia annua extracts. Dichloromethane extracts were more cytotoxic (range of IC₅₀: 1.8-14.4 μg/ml) than methanol extracts towards Trypanosoma b. brucei (TC221 cells). The range of IC₅₀ values for HeLa cancer cells was 54.1-275.5 μg/ml for dichloromethane extracts and 276.3-1540.8 μg/ml for methanol extracts. Cancer and trypanosomal cells did not reveal cross-resistance among other compounds of Artemisia annua, namely the artemisinin-related artemisitene and arteanuine B as well as the unrelated compounds, scopoletin and 1,8-cineole. This indicates that cells resistant to one compound retained sensitivity to another one. These results were also supported by microarray-based mRNA expression profiling showing that molecular determinants of sensitivity and resistance were different between artemisinin and the other phytochemicals investigated.

摘要

黄花蒿 (青蒿、qinhao) 历来在中医药中使用。青蒿素从黄花蒿中分离出来,并在全世界范围内用于疟疾治疗,这是过去几十年植物药的一个成功案例。青蒿素类化合物对其他原生动物或病毒性疾病以及体外和体内的癌细胞也有活性。如今,黄花蒿茶在发展中国家被用作一种自主治疗方法。由于植物中青蒿素的含量与标准化的青蒿素片剂或半合成青蒿素衍生物相比不足,因此未经监督使用黄花蒿茶被批评会助长疟疾和癌症中青蒿素耐药性的发展。然而,青蒿素并不是黄花蒿中唯一的生物活性化合物。在本研究中,我们分析了不同的黄花蒿提取物。与甲醇提取物相比,二氯甲烷提取物对锥虫 (TC221 细胞) 的细胞毒性更强 (IC₅₀ 范围:1.8-14.4 μg/ml)。二氯甲烷提取物对宫颈癌 HeLa 细胞的 IC₅₀ 值范围为 54.1-275.5 μg/ml,甲醇提取物的 IC₅₀ 值范围为 276.3-1540.8 μg/ml。癌症和锥虫细胞之间没有显示出黄花蒿其他化合物之间的交叉耐药性,即与青蒿素相关的青蒿烯和 arteanuine B 以及与青蒿素无关的化合物,即东莨菪素和 1,8-桉树脑。这表明对一种化合物耐药的细胞对另一种化合物保持敏感。基于微阵列的 mRNA 表达谱分析也支持了这些结果,该分析表明青蒿素和研究的其他植物化学物质之间的敏感性和耐药性的分子决定因素不同。

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