首页> 外文期刊>Peptides: An International Journal >Cytoskeleton alterations induced by Geodia corticostylifera depsipeptides in breast cancer cells.
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Cytoskeleton alterations induced by Geodia corticostylifera depsipeptides in breast cancer cells.

机译:Geodia corticostylifera depsipeptides在乳腺癌细胞中诱导的细胞骨架改变。

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Crude extracts of the marine sponge Geodia corticostylifera from Brazilian Coast have previously shown antibacterial, antifungal, cytotoxic, haemolytic and neurotoxic activities. The present work describes the isolation of the cyclic peptides geodiamolides A, B, H and I (1-4) from G. corticostylifera and their anti-proliferative effects against sea urchin eggs and human breast cancer cell lineages. Its structure-activity relationship is discussed as well. In an initial series of experiments these peptides inhibited the first cleavage of sea urchin eggs (Lytechinus variegatus). Duplication of nuclei without complete egg cell division indicated the mechanism of action might be related to microfilament disruption. Further studies showed that the geodiamolides have anti-proliferative activity against human breast cancer cell lines (T47D and MCF7). Using fluorescence techniques and confocal microscopy, we found evidence that the geodiamolides A, B, H and I act by disorganizing actin filaments of T47D and MCF7 cancer cells, in a way similar to other depsipeptides (such as jaspamide 5 and dolastatins), keeping the normal microtubule organization. Normal cells lines (primary culture human fibroblasts and BRL3A rat liver epithelial cells) were not affected by the treatment as tumor cells were, thus indicating the biomedical potential of these compounds.
机译:来自巴西海岸的海洋海绵Geodia corticostylifera的粗提物先前已显示出抗菌,抗真菌,细胞毒性,溶血和神经毒性活性。本工作描述了从皮质糖皮质激素中分离出环缩二糖胺分子A,B,H和I(1-4)的环肽及其对海胆卵和人乳腺癌细胞谱系的抗增殖作用。还讨论了其结构-活性关系。在最初的一系列实验中,这些肽抑制了海胆卵(Lytechinus variegatus)的首次切割。没有完整卵细胞分裂的细胞核重复表明其作用机制可能与微丝破坏有关。进一步的研究表明,地二糖醇对人乳腺癌细胞系(T47D和MCF7)具有抗增殖活性。使用荧光技术和共聚焦显微镜,我们发现证据表明,地二糖苷A,B,H和I通过破坏T47D和MCF7癌细胞的肌动蛋白丝而起作用,其方式类似于其他大肽肽(如jaspamide 5和dolastatins),正常的微管组织。正常细胞系(原代培养人成纤维细胞和BRL3A大鼠肝上皮细胞)不受治疗的影响,因为肿瘤细胞受到了治疗,因此表明了这些化合物的生物医学潜力。

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