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机构地区:[1]解放军第188医院药学部,广东广州510052 [2]中南民族大学药学院,湖北武汉430073
出 处:《广东药学院学报》2015年第6期727-732,共6页Academic Journal of Guangdong College of Pharmacy
摘 要:目的设计、合成具有抗乳腺癌包括荷尔蒙依赖型(ER+)和非荷尔蒙依赖型(ER-)活性的二茂铁-组蛋白去乙酰化酶抑制剂(HDACi)缀合物。方法将二茂铁取代伏立诺他(SAHA)的一个苯环得到二茂铁-HDACi缀合物,测试这些化合物对HDAC1、6、8的抑制活性,并通过MTT法测试化合物的抗乳腺癌活性。结果合成了9个二茂铁-SAHA缀合物,结构均通过~1H NMR和^(13)C NMR进行了表征。初步的生物活性结果表明,这些二茂铁-HDACi缀合物对HDAC1、6、8均有较强的抑制作用,其中肟酸化合物(5a^5c)对HDAC1、6、8的抑制活性强于羧酸(4a^4c)和噻吩肟酸化合物(6a^6c)。在细胞抑制试验中,大部分二茂铁-HDACi缀合物对乳腺癌MCF-7和MDA-MB-231细胞具有较强的抑制活性,而对前列腺癌PC-3细胞的抑制活性较弱。此外,这些二茂铁-HDACi缀合物对正常VERO细胞没有毒性,而SAHA和他莫昔芬却有毒性。结论本研究为开发具有抗乳腺癌包括荷尔蒙依赖型(ER+)和非荷尔蒙依赖型(ER-)活性的药物提供了参考。Objective To synthetize the ferrocene-HDACi conjugates with inhibitory activity in hormonedependent( ER+) and hormone-independent( ER-) breast cancer cell lines. Methods One of the phenol ring in SAHA scaffold was substituted with ferrocenyl group to get ferrocene-HDACi conjugates,which were evaluated on HDAC1,6,8 inhibition activity,and the anti-breast cancer activity was assessed by MTT.Results Nine ferrocene-HDACi conjugates were synthesized,and these compounds had been confirmed by^1 H NMR and^(13) C NMR spectra. The preliminary biological results showed that these conjugates strongly inhibited HDAC1,HDAC6,HDAC8,and hydroxamic acid derivatives( 5a- 5c) demonstrated high activity for HDAC1,HDAC6,HDAC8 over carboxylic acid( 4a-4c) and thiohydroxamic acid( 6a-6c) analogues.In cell proliferation assays,it was found that ferrocene-HDACi conjugates showed not only inhibition effect in hormone-dependent breast cancer MCF-7 cells but also in hormone-independent MDA-MB-231 cells,which had weak inhibitory activity on PC-3 cells. All conjugates were nontoxic to health VERO cells,while SAHA and tamoxifen showed essential toxicity. Conclusion This study provides information for development of drugs with inhibitory activity in hormone-dependent and hormone-independent breast cancer.
关 键 词:二茂铁-SAHA缀合物 合成 抗乳腺癌活性
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