Departamento de Química Farmacéutica y Orgánica, Facultad de Farmacia, Universidad de Granada c/Campus de Cartuja s/n, 18071 Granada, Spain.
ChemMedChem. 2011 Oct 4;6(10):1854-9. doi: 10.1002/cmdc.201100276. Epub 2011 Jul 27.
Herein we report the design, synthesis, and anticancer activity of a series of substituted (R,S)-9-[2- or 3-(3,4-dihydro-2H-1,5-benzoxathiepine-3-yloxy)alkyl]-9H-purines. Derivatives with propylenoxy-linked 2',6'-dichloro- and 6'-bromopurines are more active than their respective ethylenoxy-linked purine conjugates. On the other hand, the compound with a propylenoxy-linked 6'-chloropurine is nearly equipotent to the corresponding ethylenoxy-linked conjugate. Our results show that bromo- and chloropurine-conjugated benzoxathiepines containing a propylenoxy linker are able to inhibit PI3 kinase (PI3K) phosphorylation in MCF-7 breast cancer cells, indicating that the activation of eIF2α, together with inhibition of the PI3K pathway, is the mechanism of action by which these compounds effect their antitumor activity in the MCF-7 cell line; apoptosis was induced in a p53-independent manner.
在这里,我们报告了一系列取代的(R,S)-9-[2-或 3-(3,4-二氢-2H-1,5-苯并硫杂环庚烷-3-氧基)烷基]-9H-嘌呤的设计、合成和抗癌活性。带有丙烯氧基连接的 2',6'-二氯和 6'-溴嘌呤衍生物比其相应的乙撑氧基连接的嘌呤缀合物更具活性。另一方面,带有丙烯氧基连接的 6'-氯嘌呤的化合物几乎与相应的乙撑氧基连接的缀合物具有相同的效力。我们的结果表明,含有丙烯氧基连接体的溴代和氯代嘌呤苯并硫杂环庚烷能够抑制 MCF-7 乳腺癌细胞中 PI3 激酶(PI3K)的磷酸化,表明 eIF2α 的激活以及 PI3K 途径的抑制是这些化合物在 MCF-7 细胞系中发挥其抗肿瘤活性的作用机制;凋亡是一种不依赖 p53 的方式诱导的。
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