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顺铂与反式铂化合物联合应用于卵巢癌细胞系的协同作用。

Synergism from combination of cisplatin and a trans-platinum compound in ovarian cancer cell lines.

机构信息

Discipline of Biomedical Science, The University of Sydney, Lidcombe Campus C42, Lidcombe, NSW 1825, Australia.

出版信息

Anticancer Res. 2010 Nov;30(11):4547-53.

PMID:21115904
Abstract

Development of drug resistance and the presence of dose-limiting side-effects remain two major problems in cancer chemotherapy. Combination of drugs can offer a means of overcoming drug resistance and reducing side-effects. This study investigated synergism in activity from the combinations of cisplatin (Cis) and trans-planaramineplatinum(II) compound YH12 in the human ovarian A2780, A2780(cisR) and A2780(0473R) cancer cell lines. It was found that Cis and YH12 in combination produced both sequence- and concentration-dependent synergism. Addition of Cis first followed by YH12 4 h later produced least synergistic outcomes in all the three cell lines whereas the addition of YH12 first followed by Cis 4 h later and the bolus addition produced much greater synergism. It is believed that as Cis binds with a DNA strand forming intrastrand bifunctional 1,2-Pt(GG) and 1,2-Pt(AG) adducts, the DNA strand is bent. As a result, the subsequent interstrand bifunctional binding of YH12 to the bent DNA would be hampered due to a greater distance mismatch between the two trans-arms of YH12 and the distance between 1,2-interstrand N7(G) and N7(G) positions especially those close to the cisplatin-binding site. This may explain why the 0/4 h addition would be least synergistic in outcome. Conversely, although the interstrand GG binding of YH12 first (that would occur in the 4/0 h and 0/0 h additions), brings about global changes in DNA conformation, it will not significantly affect the subsequent intrastrand bifunctional binding of Cis, so that these modes of addition would result in greater synergistic outcomes. The results of the present study will have implications in the design of combination therapy if confirmed in vivo.

摘要

耐药性的发展和剂量限制副作用的存在仍然是癌症化疗的两个主要问题。药物联合可以提供克服耐药性和减少副作用的手段。本研究探讨了顺铂(Cis)和反式平面胺铂(II)化合物 YH12 在人卵巢 A2780、A2780(cisR)和 A2780(0473R)癌细胞系中的联合活性协同作用。结果发现 Cis 和 YH12 联合使用具有序列和浓度依赖性协同作用。在所有三种细胞系中,先加入 Cis 然后 4 小时后加入 YH12 产生的协同作用最小,而先加入 YH12 然后 4 小时后加入 Cis 和一次性加入产生的协同作用更大。据信,当 Cis 与 DNA 链结合形成内链双功能 1,2-Pt(GG)和 1,2-Pt(AG)加合物时,DNA 链会弯曲。结果,由于 YH12 的两个反式臂与 1,2-链间 N7(G)和 N7(G)位置之间的距离错配较大,尤其是靠近顺铂结合位点的位置,随后 YH12 与弯曲 DNA 的间链双功能结合会受到阻碍。这可以解释为什么 0/4 h 添加的协同作用最小。相反,尽管 YH12 的间链 GG 结合首先发生(在 4/0 h 和 0/0 h 添加中),会导致 DNA 构象的全局变化,但不会显著影响 Cis 的随后内链双功能结合,因此这些添加方式会产生更大的协同作用。如果在体内得到证实,本研究的结果将对联合治疗的设计产生影响。

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