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新型染料木黄酮衍生物通过不同机制诱导细胞死亡和细胞周期停滞。

Novel genistein derivatives induce cell death and cell cycle arrest through different mechanisms.

机构信息

Ludwik Hirszfeld Institute of Immunology and Experimental Therapy, Wrocław, Poland.

出版信息

Nutr Cancer. 2013;65(6):874-84. doi: 10.1080/01635581.2013.804938.

Abstract

Genistein is a natural compound belonging to isoflavone family of secondary plant metabolites, characterized by pleiotropic biological activity. Here we present the results of a study on new analogs and polysaccharide complexes of genistein as potent antiproliferative and cell death-inducing agents. Most potent were 2 analogs (i.e., IFG-027 and IFG-043) and 2 complexes (i.e., SPG-G and XG-G), which had higher or similar antiproliferative activity in comparison to genistein. However, these 2 analogs decreased the number of cells in G2/M phase in contrast to genistein and SPG-G complex. Genistein analogs, IFG-027 and IFG-043, and also SPG-G complex decreased mitochondrial membrane potential and induced the externalization of phosphatidylserine to the extracellular membrane site, which indicates the induction of apoptosis. Interestingly, genistein and its analogs induced caspase 3-activation supporting apoptotic mechanism of cell death but SPG-G supported caspase 3-independent apoptosis. XG-G complex probably did not induce cell death through the apoptotic pathway, as we did not find the externalization of phosphatidylserine and activation of caspase-3. After the treatment of HL-60 cells with genistein, SPG-G and XG-G formation of acidic vesicular organelle (AVO) was detected. In contrast, in the cells that were treated with genistein analogs IFG-027 and IFG-043, AVO formation was not observed.

摘要

染料木黄酮是一种天然化合物,属于植物次生代谢产物异黄酮家族,具有多种生物学活性。在这里,我们介绍了染料木黄酮新类似物和多糖复合物作为强效抗增殖和诱导细胞死亡剂的研究结果。最有效的是 2 种类似物(即 IFG-027 和 IFG-043)和 2 种复合物(即 SPG-G 和 XG-G),它们的抗增殖活性与染料木黄酮相比更高或相似。然而,与染料木黄酮和 SPG-G 复合物相比,这 2 种类似物减少了 G2/M 期的细胞数量。染料木黄酮类似物 IFG-027 和 IFG-043 以及 SPG-G 复合物降低了线粒体膜电位并诱导了磷脂酰丝氨酸向细胞外膜位点的外化,这表明诱导了细胞凋亡。有趣的是,染料木黄酮及其类似物诱导了 caspase 3 的激活,支持细胞死亡的凋亡机制,但 SPG-G 支持 caspase 3 非依赖性凋亡。XG-G 复合物可能不会通过凋亡途径诱导细胞死亡,因为我们没有发现磷脂酰丝氨酸的外化和 caspase-3 的激活。在用染料木黄酮、SPG-G 和 XG-G 处理 HL-60 细胞后,检测到酸性囊泡细胞器 (AVO) 的形成。相比之下,在用染料木黄酮类似物 IFG-027 和 IFG-043 处理的细胞中,未观察到 AVO 的形成。

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