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首页> 外文期刊>Journal of Medicinal Chemistry >Synthesis and biological activity of chimeric structures derived from the cytotoxic natural compounds dolastatin 10 and dolastatin 15.
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Synthesis and biological activity of chimeric structures derived from the cytotoxic natural compounds dolastatin 10 and dolastatin 15.

机译:源自细胞毒性天然化合物dolastatin 10和dolastatin 15的嵌合结构的合成和生物活性。

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摘要

The natural cytotoxic compounds dolastatins 10 and 15 exhibit great similarities in structure and in their biological activity profiles. Two compounds (1 and 2) formed by interchanging the dolaisoleuine residue of dolastatin 10 and the MeVal-Pro dipeptide of dolastatin 15 were synthesized in order to evaluate the possible equivalence of these units. These compounds can be considered as chimeras of dolastatins 10 and 15 formed by the N-terminal part of the former and the C-terminal part of the latter and vice versa. Both analogues exhibited a marked decrease in their cytotoxic activity but showed similar differential cytotoxicity with regard to the cell lines assayed compared with the parent compounds. HT-29 cell line was the least sensitive one. However, this activity was in the nanomolar level and close to that of vincristine. The differences in their effect on tubulin polymerization were less pronounced. We confirmed the already known crucial role of the Dil residue in this assay. The nonequivalence of the Dil unit and the MeVal-Pro dipeptide probably reflects modification in the relative positions of the N-dimethylamino and the phenyl moieties.
机译:天然细胞毒性化合物dolastatins 10和15在结构和生物学活性方面显示出极大的相似性。合成了通过互换dolastatin 10的dolaso​​leuine残基和dolastatin 15的MeVal-Pro二肽而形成的两种化合物(1和2),以评估这些单元的可能等效性。这些化合物可以被认为是由前者的N末端部分和后者的C末端部分形成的Dolastatin 10和15的嵌合体,反之亦然。两种类似物均表现出明显的细胞毒性活性降低,但与所检测的细胞系相比,其母体化合物显示出相似的差异性细胞毒性。 HT-29细胞系是最不敏感的一种。但是,该活性处于纳摩尔水平,接近长春新碱。它们对微管蛋白聚合作用的差异不太明显。我们确认了Dil残留物在此测定法中的已知关键作用。 Dil单元和MeVal-Pro二肽的不等价可能反映了N-二甲基氨基和苯基部分的相对位置的改变。

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