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Genistein Derivatives Regioisomerically Substituted at 7-O- and 4′-O- Have Different Effect on the Cell Cycle

机译:Genistein衍生物在7-O-和4'-O-对细胞周期产生不同的效果

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Our previous studies on antiproliferative properties of genistein derivatives substituted at C7 hydroxyl group of the ring A revealed some compounds with antimitotic properties. The aim of this work was to synthesize their analogues substituted at the 4′-position of the ring B in genistein and to define their antiproliferative mechanism of action in selected cancer cell lines in vitro. C4′-substituted glycoconjugates were obtained in a three-step procedure (1) alkylation with an ω-bromoester; (2) deacylation; (3) Ferrier-type rearrangement glycosylation with acylated glycals. Biological effects including antiproliferative effects of the compounds, cell cycle, DNA lesions (ATM activation, H2A.X phosphorylation, and micronuclei formation), and autophagy were studied in human cancer cell lines. Some of the tested derivatives potently inhibited cell proliferation. The presence of a substituent at the 4′-position of the ring B in genistein correlated to a p53-independent G1 cell-cycle arrest. The derivatives substituted at C4′ did not induce DNA lesions and appeared to be nongenotoxic. The tested compounds induced autophagy and caused remarkable decrease of cell volume.
机译:我们以前关于在环A的C7羟基中取代的Genistein衍生物的抗增殖性质的研究显示了一些具有抗催化性质的化合物。这项工作的目的是将它们的类似物综合在Genistein中的环B的4'位置取代,并在体外在选定的癌细胞系中定义它们的抗增殖作用机制。在用ω-溴酯的三步骤(1)烷基化中获得C4'-取代的糖缀合物; (2)脱乙酰化; (3)具有酰化族化族化合物的特定型重新排列糖基化。在人类癌细胞系中研究了生物学效应,包括化合物,细胞周期,DNA病变(ATM激活,H2A.x磷酸化和微核)和自噬的抗增殖作用。一些测试的衍生物有效地抑制细胞增殖。在Genistein的环B的4'-位置处存在取代基与p53无关的G1细胞循环骤停。在C4'被取代的衍生物没有诱导DNA病变并似乎是NongEnotoxic。测试的化合物诱导自噬并引起细胞体积的显着降低。

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