首页> 美国卫生研究院文献>International Journal of Molecular Sciences >The Product of Matrix Metalloproteinase Cleavage of Doxorubicin Conjugate for Anticancer Drug Delivery: Calorimetric Spectroscopic and Molecular Dynamics Studies on Peptide–Doxorubicin Binding to DNA
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The Product of Matrix Metalloproteinase Cleavage of Doxorubicin Conjugate for Anticancer Drug Delivery: Calorimetric Spectroscopic and Molecular Dynamics Studies on Peptide–Doxorubicin Binding to DNA

机译:用于抗癌药物缀合物的多柔比星缀合物的基质金属蛋白酶裂解产物:热量光谱和分子动力学研究肽 - 多柔比星与DNA的结合

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摘要

Matrix metalloproteinases (MMPs) are extracellular matrix degradation factors, promoting cancer progression. Hence, they could provide an enzyme-assisted delivery of doxorubicin (DOX) in cancer treatment. In the current study, the intercalation process of DOX and tetrapeptide–DOX, the product of the MMPs’ cleavage of carrier-linked DOX, into dsDNA was investigated using stationary and time-resolved fluorescence spectroscopy, UV-Vis spectrophotometry and isothermal titration calorimetry (ITC). The molecular dynamics (MD) simulations on the same tetrapeptide–DOX…DNA and DOX…DNA systems were also performed. The undertaken studies indicate that DOX and tetrapeptide–DOX can effectively bond with dsDNA through the intercalation mode; however, tetrapeptide–DOX forms less stable complexes than free DOX. Moreover, the obtained results demonstrate that the differences in DNA affinity of both forms of DOX can be attributed to different intercalation modes. Tetrapeptide–DOX shows a preference to intercalate into DNA through the major groove, whereas DOX does it through the minor one. In summary, we can conclude that the tetrapeptide–DOX intercalation to DNA is significant and that even the lack of non-specific proteases releasing DOX from the tetrapeptide conjugate, the presence of which is suggested by the literature for the efficient release of DOX, should not prevent the cytostatic action of the anthracycline.
机译:基质金属蛋白酶(MMP)是细胞外基质降解因子,促进癌症进展。因此,它们可以在癌症治疗中提供多柔比星(DOX)的酶辅助递送。在目前的研究中,使用静止和时间分辨荧光光谱,UV-Vis分光光度法和等温滴定热量研究,研究了DOX和四肽-DOX的嵌入过程,将载体连接DOX的MMPS连接的DOX的产物分解为DSDNA( ITC)。还进行了相同四肽-DOX ... DNA和DOX的分子动力学(MD)模拟。进行的研究表明,DOX和四肽-DOX可以通过插入模式有效地与DSDNA键合;然而,四肽-DOX形成比自由DOX更稳定的络合物。此外,所得结果表明,两种形式的DOX的DNA亲和力的差异可归因于不同的插层模式。 Tetrapeptide-Dox显示偏好通过主要凹槽嵌入DNA,而DOX通过次要的凹槽。总之,我们可以得出结论,Tetrapeptipe-Dox嵌入对DNA的显着性,即使缺乏来自四肽缀合物的非特异性蛋白酶释放DOX,其存在应该有效地提出了DOX的有效释放的情况。不防止蒽环素的细胞抑制作用作用。

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