首页> 外国专利> DI- AND TRI-CATIONIC GLYCOSYLATED ANTITUMOR ETHER LIPIDS, L-GUCOSYLATED GAELS AND RHAMNOSE-LINKED GAELS AS CYTOTOXIC AGENTS AGAINST EPITHELIAL CANCER CELLS AND CANCER STEM CELLS

DI- AND TRI-CATIONIC GLYCOSYLATED ANTITUMOR ETHER LIPIDS, L-GUCOSYLATED GAELS AND RHAMNOSE-LINKED GAELS AS CYTOTOXIC AGENTS AGAINST EPITHELIAL CANCER CELLS AND CANCER STEM CELLS

机译:二和三阳离子糖基化的抗胆固醇脂质,L-糖基化的凝胶和鼠李糖连接的凝胶作为抗上皮性癌细胞和癌干细胞的细胞毒剂

摘要

Glycosylated Antitumor Ether Lipids (GAELs) kill cancer cells by a nonapoptotic pathway which is an attractive strategy to avoid resistance. To further optimize the antitumor effect, we prepared various analogs of di-, and tri-cationic GAEL analogs differing in the nature of the sugar (D-giucose or L-glucose), the anomeric linkage as well as position of the glycerolipid moiety. The di- and tri-cationic GAELs were synthesized and their in vitro anticancer properties were evaluated against drug resistant and aggressively growing cancer cell lines derived from human breast, prostate, pancreatic and ovarian cancers. The most potent dicationic GAEL analogs were also studied against cancer stem cells obtained from breast BT 474, prostate DU145 and ovarian A2780cp cell lines. Our results indicate that the number of positive charges, the position of the amino substituents and the nature of the sugar have significant effects on the anticancer activities of these compounds. The most active analog kill 50% of the cells at concentration range of 0.5-5μΜ and 90% of the cells at the concentration of 1-10μΜ depending on type of cancer cells.
机译:糖基化的抗肿瘤醚脂质(GAEL)通过非凋亡途径杀死癌细胞,这是避免耐药性的一种有吸引力的策略。为了进一步优化抗肿瘤作用,我们制备了二阳离子和三阳离子GAEL类似物的各种类似物,这些类似物在糖的性质(D-葡糖或L-葡萄糖),端基异构键以及甘油脂部分的位置上有所不同。合成了双阳离子和三阳离子GAEL,并评估了其体外抗癌特性对源自人乳腺癌,前列腺癌,胰腺癌和卵巢癌的耐药性和侵袭性增长的癌细胞系的作用。还研究了最有效的药用GAEL类似物针对从乳腺BT 474,前列腺DU145和卵巢A2780cp细胞系获得的癌症干细胞。我们的结果表明,正电荷的数量,氨基取代基的位置和糖的性质对这些化合物的抗癌活性具有重要影响。取决于癌细胞的类型,最活跃的类似物在0.5-5μM的浓度范围内杀死50%的细胞,在1-10μM的浓度下杀死90%的细胞。

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