首页> 外文期刊>Journal of Inorganic Biochemistry: An Interdisciplinary Journal >Evaluation of in vitro cytotoxicity and hepatotoxicity of platinum(II) and palladium(II) oxalato complexes with adenine derivatives as carrier ligands
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Evaluation of in vitro cytotoxicity and hepatotoxicity of platinum(II) and palladium(II) oxalato complexes with adenine derivatives as carrier ligands

机译:以腺嘌呤衍生物为载体配体的草酸铂(II)和草酸钯(II)配合物的体外细胞毒性和肝毒性的评估

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摘要

In vitro antitumour activity of the [Pt(ox)(L_n)_2] (1-7) and [Pd(ox)(L_n)_2] (8-14) oxalato (ox) complexes involving N6-benzyl-9-isopropyladenine-based N-donor carrier ligands (L_n) against ovarian carcinoma (A2780), cisplatin resistant ovarian carcinoma (A2780cis), malignant melanoma (G-361), lung carcinoma (A549), cervix epitheloid carcinoma (HeLa), breast adenocarcinoma (MCF7) and osteosarcoma (HOS) human cancer cell lines was studied. Some of the tested complexes were even several times more cytotoxic as compared with cisplatin employed as a positive control. The improved cytotoxic effect was demonstrated for the platinum(II) complexes 3 (IC_(50)=3.2±1.0μM and 3.2±0.6μM) and 5 (IC_(50)=4.0±1.0μM and 4.1±1.4μM) against A2780 and A2780cis, as compared with 11.5±1.6μM, and 30.3±6.1μM determined for cisplatin, respectively. The significant in vitro cytotoxicity against MCF7 (IC_(50)=8.2±3.8μM for 12) and A2780 (IC_(50)=5.4±1.2μM for 14) was evaluated for the palladium(II) oxalato complexes, which again exceeded cisplatin, whose IC_(50) equalled 19.6±4.3μM against the MCF7 cells. Selected complexes were also screened for their in vitro cytotoxic effect in primary cultures of human hepatocytes and they were found to be non-hepatotoxic.
机译:涉及N6-苄基-9-异丙基腺嘌呤的[Pt(ox)(L_n)_2](1-7)和[Pd(ox)(L_n)_2](8-14)草酸(ox)复合物的体外抗肿瘤活性卵巢癌(A2780),顺铂耐药性卵巢癌(A2780cis),恶性黑素瘤(G-361),肺癌(A549),子宫颈上皮癌(HeLa),乳腺腺癌(MCF7)的基于N的供体载体配体(L_n) )和骨肉瘤(HOS)人类癌细胞系的研究。与顺铂用作阳性对照相比,某些测试的复合物的细胞毒性甚至更高。铂(II)配合物3(IC_(50)= 3.2±1.0μM和3.2±0.6μM)和5(IC_(50)= 4.0±1.0μM和4.1±1.4μM)对A2780的细胞毒性作用得到改善和A2780cis,分别为11.5±1.6μM和30.3±6.1μM。对于草酸钯(II)复合物,评估了其对MCF7(对于12的IC_(50)= 8.2±3.8μM)和对A2780(对于14的IC_(50)= 5.4±1.2μM)的显着体外细胞毒性,该复合物再次超过顺铂,其针对MCF7细胞的IC_(50)等于19.6±4.3μM。还筛选了选定的复合物在人肝细胞的原代培养物中的体外细胞毒性作用,发现它们是非肝毒性的。

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