Synthesis and antiproliferative activity of cisplatin-3-chloropiperidine conjugates

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-09-20 DOI:10.1002/cbic.202400519
Richard Göttlich, Mats Georg, Anton A. Legin, Michaela Hejl, Michael A. Jakupec, Jonathan Becker
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Abstract

We report the synthesis and characterization of two novel cisplatin- alkylating agents conjugates. Combining a platinum based cytostatic agent with a sterically demanding alkylating agent could potentially induce further DNA damage, block cell repair mechanisms and keep the substrate active against resistant tumor cell lines. The 3-chloropiperidines utilized as ligands in this work are cyclic representatives of the N-mustard family and were not able to coordinate platinum on their own. The introduction of a second coordination site, in form of a pyridine moiety, led to the isolation of the desired conjugates. They were characterized with HRMS, CHN-analyses and XRD. We concluded this work by examining the cytotoxicity of the ligands and the obtained complexes with MTT assays in human cancer cell lines. While the ligands showed hardly any activity, the novel conjugates both displayed a high antiproliferative and cytotoxic potency in a panel of three cell lines. Moreover, both complexes were able to largely circumvent the acquired cisplatin resistance of A2780cisR ovarian cancer cells, both in the MTT assay and a flow-cytometric apoptosis assay.
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顺铂-3-氯哌啶共轭物的合成与抗增殖活性
我们报告了两种新型顺铂-烷化剂共轭物的合成和表征。将铂类细胞抑制剂与立体要求较高的烷化剂结合使用,有可能诱发进一步的 DNA 损伤,阻断细胞修复机制,并使底物对抗药性肿瘤细胞株保持活性。这项研究中用作配体的 3-氯哌啶是 N-芥末家族的环状代表,本身无法与铂配位。通过引入吡啶分子形式的第二个配位位点,分离出了所需的共轭物。我们利用 HRMS、CHN 分析和 XRD 对它们进行了表征。最后,我们用 MTT 法检测了配体和所获复合物在人类癌细胞系中的细胞毒性。虽然配体几乎没有显示出任何活性,但新型共轭物在三种细胞系中都显示出了很高的抗增殖性和细胞毒性。此外,在 MTT 试验和流式细胞凋亡试验中,这两种复合物都能在很大程度上规避 A2780cisR 卵巢癌细胞的顺铂耐药性。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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