首页> 外文期刊>Oncology Research >The unique biological features of the marine product Yondelis (ET-743, trabectedin) are shared by its analog ET-637, which lacks the C ring.
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The unique biological features of the marine product Yondelis (ET-743, trabectedin) are shared by its analog ET-637, which lacks the C ring.

机译:海洋产品Yondelis(ET-743,trabectedin)的独特生物学特征与其类似物ET-637(缺乏C环)共有。

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It was previously suggested that the peculiar mechanism of action of the novel anticancer drug Yondelis (ET-743, trabectedin) was due to part of the molecule, units A and B, binding to DNA in the minor groove, causing an alkylation at the N2 of guanine, while unit C protrudes out of DNA, possibly interacting with transcription factors or other DNA binding proteins. To test this hypothesis, we have compared the biological activity and the mode of action of Yondelis with its analogue ET-637, which has the same chemical structure except for the lack of the C ring. Yondelis and ET-637 showed similar cytotoxic potency and cell cycle perturbations. As already reported for Yondelis, the UV-96 cell line, deficient in ERCC-1, was less sensitive to ET-637 than the parental cell line. The binding of Yondelis or ET-637 to DNA-oligonucleotides was demonstrated by gel shift assay and SDS did not reverse the binding. Both compounds blocked the temperature-induced activation of the HSP40 promoter in the range of 1-10 nM. This study indicates that ET-637 acts similarly to Yondelis and demonstrates that the C ring of Yondelis may not be required for its biological activity.
机译:以前有人认为,新型抗癌药Yondelis(ET-743,trabectedin)的独特作用机理是由于分子的一部分,即A和B单元与小沟中的DNA结合,导致N2处的烷基化鸟嘌呤的表达,而单元C从DNA突出,可能与转录因子或其他DNA结合蛋白相互作用。为了验证该假设,我们将Yondelis及其类似物ET-637的生物学活性和作用方式进行了比较,类似物ET-637具有相同的化学结构,但缺少C环。 Yondelis和ET-637表现出相似的细胞毒性效力和细胞周期扰动。如针对Yondelis的报道,缺少ERCC-1的UV-96细胞系对ET-637的敏感性低于亲代细胞系。通过凝胶位移测定法证实了Yondelis或ET-637与DNA-寡核苷酸的结合,并且SDS没有使结合逆转。两种化合物均在1-10 nM的范围内阻止了HSP40启动子的温度诱导活化。这项研究表明ET-637的作用与Yondelis类似,并证明Yondelis的C环可能不需要其生物活性。

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