RSS-Feed abonnieren
DOI: 10.1055/s-0034-1372647
Ethanol Extract and Isolated Constituents from Artemisia Dracunculus Inhibit Esophageal Squamous Cell Carcinoma and Induce Apoptotic Cell Death
Publikationsverlauf
received 13. Februar 2014
accepted 26. März 2014
Publikationsdatum:
30. Juli 2014 (online)
Abstract
The objective of the present study was to examine the antitumor efficacy of the ethanol extract from Artemisia dracunculus as well as the compounds isolated from it on cultured EC‑109 esophageal squamous cell carcinoma (ESCC) cells. Apoptotic activities of the compounds were also studied using flow cytometry. EC‑109 esophageal cancer cells were treated with varying concentrations of compounds 1–7 isolated from the plant as well as the ethanol extract of Artemisia dracunculus. The cytotoxicity was evaluated by MTT assay and the apoptotic studies of the compounds were determined using flow-cytometry. Effect on mitochondrial membrane potential loss ΛΨ m induced by compounds 2 and 4 was also studied in these cells. Bioassay-guided fractionation of the ethanol extract from the shoot and root parts of Artemisia dracunculus led to the isolation of 7-methoxycoumarin (1), scopoletin (2), dracumerin (3), sakuranetin (4), elimicin (5), davidigenin (6) and 6-methoxycapillarisin (7). All the compounds as well as the extract showed mild to potent cell proliferation inhibitory activities against the esophageal cell line. Sakuranetin and 6-methoxycapillarisin were found to have the most potent effects in inhibiting the cell proliferation. The 2 potent compounds, sakuranetin and 6-methoxycapillarisin were evaluated for their effects on cell cycle phase distribution (DNA damage) as well as their effects on mitochondrial membrane potential loss ΛΨ m. Both compounds induced DNA damage as well as mitochondrial membrane potential loss in esophageal cancer cells. The study suggests that compounds, Sakuranetin and 6-methoxycapillarisin isolated from Artemisia dracunculus possess potent anticancer effects by inducing DNA damage in these cells.
-
References
- 1 Ma X, Wang Z. Anticancer drug discovery in the future: an evolutionary perspective. Drug Discov Today 2009; 14: 1136-1142
- 2 Gordaliza M. Natural products as leads to anticancer drugs. Clin Transl Oncol 2007; 9: 767-776
- 3 Madhuri S, Pandey G. Some anticancer medicinal plants of foreign origin. Curr Sci 2009; 96
- 4 Harvey AL. Medicines from nature: are natural products still relevant to drug discovery. Trends Pharmacol Sci 1999; 20: 196-198
- 5 Newman DJ, Cragg GM, Snader KM. The influence of natural products upon drug discovery. Nat Prod Rep 2000; 17: 215-234
- 6 Mann J. Natural products in cancer chemotherapy: past, present and future. Nat Rev Cancer 2002; 2: 143-148
- 7 Reichert JM, Wenger JB. Development trends for new cancer therapeutics and vaccines. Drug Discov Today 2008; 13: 7-30
- 8 Carnesecchi S, Schneider Y, Ceraline J et al. Geraniol, a component of plant essential oils inhibits growth and polyamine biosynthesis in human colon cancer cells. J Pharmacol Exp Ther 2001; 298: 197-200
- 9 Jemal A, Bray F, Center MM et al. Global cancer statistics. CA Cancer J Clin 2011; 61: 69-90
- 10 Gibbs JB. Mechanism-based target identification and drug discovery in cancer research. Science 2000; 287: 1969-1973
- 11 Debatin KM. Apoptosis pathways in cancer and cancer therapy. Cancer Immunol Immunother 2004; 53: 153-159
- 12 Obolskiy D, Pischel I, Feistel B et al. Artemisia dracunculus L. (tarragon): a critical review of its traditional use, chemical composition, pharmacology, and safety. J Agric Food Chem 2011; 59: 11367-11384
- 13 Herz W, Bhat SV, Santhanam PS. Coumarins of Artemisia dracunculoides and 3΄,6 dimethoxy-4΄,5,7-trihydroxyflavone from A. Arctica. Phytochemistry 1970; 9: 891-894
- 14 Jalmakhanbetova RI, Adekenov SM. Chemical Study of Artemisia filatovae. Chem Nat Comp 2007; 43: 347-348
- 15 Efferth T. Antiplasmodial and antitumor activity of artemisinin from bench to beside. Planta Med 2007; 73: 299-309
- 16 Wons H, Brown GD. Germacranolides from Artemisia myriantha and their conformation. Phytochemistry 2002; 59: 529-536
- 17 Kim JH, Kim HK, Jeon SB et al. New sesquiterpene- monoterpene lactone, artemisolide, isolated from Artemisia argyi. Tetrahedron lett 2002; 43: 6205-6208
- 18 Shimizu T, Lin F, Hasegawa M et al. The potential bioproduction of the pharmaceutical agent sakuranetin, a flavonoid phytoalexin in rice. Bioengineered 2012; 3: 352-357
- 19 Lu M, Sun L, Zhou J et al. Dihydroartemisinin induces apoptosis in colorectal cancer cells through the mitochondria-dependent pathway. Tumour Biol 2014; (In press PMID: 24519064)
- 20 Chan HW, Singh NP, Lai HC. Cytotoxicity of dihydroartemisinin toward Molt-4 cells attenuated by N-tert-butyl-alpha-phenylnitrone and deferoxamine. Anticancer Res 2013; 33: 4389-4393
- 21 Jin M, Shen X, Zhao C et al. In vivo study of effects of artesunate nanoliposomes on human hepatocellular carcinoma xenografts in nude mice. Drug Deliv 2013; 20: 127-133
- 22 Tin AS, Sundar SN, Tran KQ et al. Antiproliferative effects of artemisinin on human breast cancer cells requires the downregulated expression of the E2F1 transcription factor and loss of E2F1-target cell cycle genes. Anticancer Drugs 2012; 23: 370-379