摘要
目的 综述呫吨酮类化合物的抗肿瘤研究进展。方法 查阅国内外文献,归纳呫吨酮类化合物的来源及其抗肿瘤研究现状。结果 呫吨酮(xanthone,氧杂蒽酮)类化合物是以呫吨酮为母体的一类化合物,主要存在于龙胆科和藤黄科植物中,是近代天然产物中的一类重要活性成分。现代药理学研究表明,呫吨酮类化合物可通过作用拓扑异构酶Ⅱ、DNA烷基化、嵌入DNA、交联DNA、KDR/Flk-1磷酸化、细胞凋亡、α-糖苷酶和芳香酶等耙点而产生抗肿瘤作用。结论 呫吨酮类化合物的数量众多,结构各异,其抗肿瘤作用靶点多,为天然产物抗肿瘤的研究和开发提供了线索。
关键词
呫吨酮类化合物 /
天然产物 /
合成产物 /
抗肿瘤作用
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戴支凯 程训佳.
呫吨酮类化合物的抗肿瘤研究进展[J]. 中国药学杂志, 2010, 45(22): 1701-1703
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参考文献
[1] YIN H F, QIAN X P. Advance on antitumor effect of Gamboge[J]. Mod J Integr Tradit Chin West Med(现代中西医结合杂志),2008,17(14): 2264-2267.
[2] FOTIE J, BOHLE D S. Pharmacological and biological activities of xanthones[J]. Anti-infect Agents Med Chem, 2006, 5(1): 15-31.
[3] POULI N,MARAKOS P. Fused xanthone derivatives as antiproliferative agents[J]. Anti-Cancer Agents Med Chem, 2009, 9(1): 77-98.
[4] YU J, WU X Q, SUN H F, et al. Advance of biological activity of rhein and its derivatives[J]. Pharm Clin Res, 2008, 16(2): 125-128.
[5] ANTAL N, FIEDLER H P, STACKEBRANDT E, et al. Retymicin, galtamycin B, saquayamycin Z and ribofuranosyllumichrome, novel secondary metabolites from Micromonospora sp. Tü 6368 Ⅰ. Taxonomy, fermentation, isolation and biological activities[J]. J Antibiot, 2005, 58(2): 95-102.
[6] YANG R Y, HUANG Z J, SHAO C L, et al. Metabolites of mangrove endophytic fungus No. ZZF71 from the South China Sea[J]. Chem Res Appl, 2008, 20(7): 893-895.
[7] WANG H D, TAN C Y, ZHAO J M, et al. HPLC analysis of two active constitutes in Gentianopsis paludosa Ma from Tibet[J]. Chin J Pharm Anal(药物分析杂志), 2007, 27(3): 421-423.
[8] WOO S, KANG D H, KIM J, et al. Synthesis, cytotoxicity and topoisomerase II inhibition study of new thioxanthone analogues[J]. Bull Korean Chem Soc, 2008, 29(2): 471-474.
[9] SOUSA E, PAIVA A, NAZARETH N, et al. Bromoalkoxyxanthones as promising antitumor agents: synthesis, crystal structure and effect on human tumor cell lines[J]. Eur J Med Chem, 2009, 44(9): 3830-3835.
[10] KRICK A, KEHRAUS S, GERHUSER C, et al. Potential cancer chemopreventive in vitro activities of monomeric xanthone derivatives from the marine algicolous fungus Monodictys putredinis[J]. J Nat Prod, 2007, 70(3): 353-360.
[11] YU L M, ZHAO M M, YANG B, et al. Immunomodulatory and anticancer activities of phenolics from Garcinia mangostana fruit pericarp[J]. Food Chemistry, 2009, 116(4):969-973.
[12] YUKIHIRO A, YOSHIHITO N, MUNEKAZU I, et al. Anti-cancer effects of xanthones from pericarps of mangosteen[J]. Int J Mol Sci, 2008, 9(3): 355-370.
[13] NAKAGAWA Y, IINUMA M, NAOE T, et al. Characterized mechanism of alpha-mangostin-induced cell death: caspase-independent apoptosis with release of endonuclease-G from mitochondria and increased miR-143 expression in human colorectal cancer DLD-1 cells[J]. Bioorg Med Chem, 2007, 15(16): 5620-5628.
[14] BALUNAS M J, SU B, BRUEGGEMEIER R W, et al. Xanthones from the botanical dietary supplement mangosteen (Garcinia mangostana) with aromatase inhibitory activity[J]. J Nat Prod, 2008, 71(7): 1161-1166.
[15] KUHAJDA F P. Fatty acid synthase and cancer: new application of an old pathway [J]. Cancer Res, 2006, 66(12): 5977-5980.
[16] HAO J, MA X F. In fruit, vegetables, seasoning falty acid synthase inhibitor screening [J]. Life Sci Instruments(生命科学仪器), 2008, 6(11): 22-30.
[17] HAN Q B, WANG Y L, YANG L, et al. Cytotoxic polyprenylated xanthones from the resin of Garcinia hanburyi [J]. Chem Pharm Bull, 2006, 54 (2): 265-267.
[18] HAN Q B, YANG L, WANG Y L, et al. A pair of novel cytotoxic polyprenylated xanthone epimers from gamboges [J]. Chem Biodivers, 2006, 3 (1): 101-105.
[19] PANDEY M K, SUNG B, AHN K S, et al. Gambogic acid, a novel ligand for transferrin receptor, potentiates TNF-induced apoptosis through modulation of the nuclear factor-kappa B signaling pathway[J]. Blood, 2007, 110(10):3517-3525.
[20] LU N, YANG Y, YOU Q D, et al. Gambogic acid inhibits angiogenesis through suppressing vascular endothelial growth factor induced tyrosine phosphorylation of KDR/Flk-1[J]. Cancer Lett, 2007, 258(1): 80-89.
[21] QIN Y, MENG L, HU C, et al. Gambogic acid inhibits the catalytic activity of human topoisomerase II {alpha} by binding to its ATPase domain[J]. Mol Cancer Ther, 2007, 6(9): 2429-2440.
[22] WANG T, WEI J, QIAN X, et al. Gambogic acid, a potent inhibitor of survivin, reverses docetaxel resistance in gastric cancer cells[J]. Cancer Lett, 2008, 262(2): 214-222.
[23] REUTRAKUL V, AMANTACHOKE N, POHMAKOTR M, et al. Cytotoxic and anti-H IV-1 caged xanthones from the resin and fruits of Garcinia hanburyi[J]. Planta Med, 2007, 73 (1): 33-40.
[24] DING L, LIU B, QI L L, et al. Anti-proliferation, cell cycle arrest and apoptosis induced by a natural xanthone from Gentianopsis paludosa Ma, in human promyelocytic leukemia cell line HL-60 cells[J]. Toxicol In Vitro, 2009, 23(3): 408-417.
[25] LEE B W, LEE J H, LEE S T, et al. Antioxidant and cytotoxic activities of xanthones from Cudrania tricuspidata[J]. Bioorganic and Medicinal Chemistry Letters, 2005, 15(24): 5548-5552.
[26] WIJERATNE E M K, TURBYVILLE T J, FRITZ A, et al. A new dihydroxanthenone from a plantassociated strain of the fungus Chaetomium globosum demonstrates anticancer activity[J]. Bioorg Med Chem, 2006, 14(23): 7917-7923.
[27] WANG T C, CHEN I L, LU C M, et al. Synthesis, and cytotoxic and antiplatelet activities of oxime- and methyloxime-containing flavone, isoflavone, and xanthone derivatives[J]. Chem Biodivers, 2005, 2(2): 253-263.
[28] SUN H L, TSAI A C, PAN S L, et al. EPOX inhibits angiogenesis by degradation of Mcl-1 through ERK inactivation[J]. Clin Cancer Res, 2009, 15(15): 4904-4914.
[29] GOODELL J R, MADHOK A A, HIASA H, et al. Synthesis and evaluation of acridone- and acridone-based anti-herpes agents with topoisomerase activity[J]. Bioorg Med Chem, 2006, 14(16): 5467-5480.
[30] LIU Y, KE Z, CUI J, et al. Synthesis, inhibitory activities, and QSAR study of xanthone derivatives as alpha-glucosidase inhibitors[J]. Bioorg Med Chem, 2008, 16(15):7185-7192.
[31] SKALLI S, ZAID A, SOULAYMANI R. Drug interactions with herbal medicines[J]. Ther Drug Monit, 2007, 29(6): 679-686.
[32] FOTI R S, WAHLSTROM J L. The role of dietary supplements in cytochrome P450-mediated drug interactions[J]. Lat Am Bull Carib Med Arom Plants,2008,7(2): 66-84.
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