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维生素 D(2)类似物作为潜在白血病分化诱导剂和前列腺癌增殖抑制剂的结构-功能分析。

Structure-function analysis of vitamin D(2) analogs as potential inducers of leukemia differentiation and inhibitors of prostate cancer proliferation.

机构信息

Department of Biotechnology, University of Wroclaw, Tamka, Poland.

出版信息

J Steroid Biochem Mol Biol. 2011 Aug;126(1-2):46-54. doi: 10.1016/j.jsbmb.2011.04.006. Epub 2011 Apr 29.

Abstract

We characterized a structure-function relationships of four analogs of vitamin D(2) with extended and branched side-chains. We tested their ability to induce differentiation of human acute myeloid leukemia (AML) cells both in vitro and ex vivo. Our experiments on five human cell lines revealed substantial differences among tested analogs. Analogs with side-chains extended by one (PRI-1906) or two carbon units (PRI-1907) displayed similar or elevated cell-differentiating activity in comparison to 1,25-dihydroxyvitamin D(3) (1,25D), whereas further extending side-chain resulted in substantially lower biological activity (PRI-1908 and PRI-1909). Similar pattern of cell-differentiating activities to that observed in human cell lines has also been shown in blast cells isolated from patients diagnosed with AML. The ability of the analogs to activate expression of CYP24A1 gene has been studied in HL60 cell line. The analog PRI-1906 activated expression of CYP24A1 similarly to 1,25D, while PRI-1907 weaker than 1,25D. In addition, the analogs PRI-1906 and PRI-1907 were able to moderately inhibit proliferation and significantly activate expression of CYP24A1 mRNA in prostate cancer cells PC-3. Finally, we examined the molecular actions triggered by these analogs and found that their biological activity was related to their ability to induce expression and nuclear translocation of VDR and C/EBPβ.

摘要

我们描述了四个具有延伸和支链侧链的维生素 D(2)类似物的结构-功能关系。我们测试了它们在体外和体内诱导人急性髓细胞白血病 (AML) 细胞分化的能力。我们在五个人类细胞系上的实验揭示了测试类似物之间存在实质性差异。具有一个(PRI-1906)或两个碳原子侧链延伸的类似物(PRI-1907)与 1,25-二羟基维生素 D(3)(1,25D)相比显示出相似或更高的细胞分化活性,而进一步延伸侧链导致生物活性显著降低(PRI-1908 和 PRI-1909)。在从诊断为 AML 的患者中分离的原始细胞中也观察到与在人细胞系中观察到的类似的细胞分化活性模式。在 HL60 细胞系中研究了类似物激活 CYP24A1 基因表达的能力。类似物 PRI-1906 激活 CYP24A1 表达的能力与 1,25D 相似,而 PRI-1907 则弱于 1,25D。此外,类似物 PRI-1906 和 PRI-1907 能够适度抑制前列腺癌细胞 PC-3 的增殖并显著激活 CYP24A1 mRNA 的表达。最后,我们检查了这些类似物触发的分子作用,发现它们的生物活性与其诱导 VDR 和 C/EBPβ 表达和核转位的能力有关。

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