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首页> 外文期刊>Journal of biological inorganic chemistry: JBIC: a publication of the Society of Biological Inorganic Chemistry >Synthesis, antiproliferative activity in cancer cells and DNA interaction studies of [Pt(cis-1,3-diaminocycloalkane)Cl-2] analogs
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Synthesis, antiproliferative activity in cancer cells and DNA interaction studies of [Pt(cis-1,3-diaminocycloalkane)Cl-2] analogs

机译:癌细胞中的合成,抗增殖活性和[Pt(CIS-1,3-二烷基烷烃)CL-2]类似物的DNA相互作用研究

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The search for more effective platinum anticancer drugs has led to the design, synthesis, and preclinical testing of hundreds of new platinum complexes. This search resulted in the recognition and subsequent FDA approval of the third-generation Pt(II) anticancer drug, [Pt(1,2-diaminocyclohexane)(oxalate)], oxaliplatin, as an effective agent in treating colorectal and gastrointestinal cancers. Another promising example of the class of anticancer platinum(II) complexes incorporating the Pt(1,n-diaminocycloalkane) moiety is kiteplatin ([Pt(cis-1,4-DACH)Cl-2], DACH = diaminocyclohexane). We report here our progress in evaluating the role of the cycloalkyl moiety in these complexes focusing on the synthesis, characterization, evaluation of the antiproliferative activity in tumor cells and studies of the mechanism of action of new [Pt(cis-1,3-diaminocycloalkane)Cl-2] complexes wherein thecis-1,3-diaminocycloalkane group contains the cyclobutyl, cyclopentyl, and cyclohexyl moieties. We demonstrate that [Pt(cis-1,3-DACH)Cl-2] destroys cancer cells with greater efficacy than the other two investigated 1,3-diamminocycloalkane derivatives, or cisplatin. Moreover, the investigated [Pt(cis-1,3-diaminocycloalkane)Cl-2] complexes show selectivity toward tumor cells relative to non-tumorigenic normal cells. We also performed several mechanistic studies in cell-free media focused on understanding some early steps in the mechanism of antitumor activity of bifunctional platinum(II) complexes. Our data indicate that reactivities of the investigated [Pt(cis-1,3-diaminocycloalkane)Cl-2] complexes and cisplatin with glutathione and DNA binding do not correlate with antiproliferative activity of these platinum(II) complexes in cancer cells. In contrast, we show that the higher antiproliferative activity in cancer cells of [Pt(cis-1,3-DACH)Cl-2] originates from its highest hydrophobicity and most efficient cellular uptake. Graphic abstract
机译:寻求更有效的铂抗癌药物导致了数百种铂复合物的设计,合成和临床前测试。该搜索导致第三代Pt(II)抗癌药物[Pt(1,2-二氨基环己烷),奥沙利铂作为治疗结直肠癌和胃肠癌的有效试剂的识别和随后的FDA批准。掺入Pt(1,N-二氨基环烷烃)部分的抗癌铂(II)复合物的另一个有希望的例子是KITEPLATIN([PT(CIS-1,4-DACT)CL-2],达抗=二氨基环己烷)。我们在此报告我们在评估这些复合物中的环烷基部分在这些复合物中的作用的进展,其专注于合成,表征,评价肿瘤细胞中的抗增殖活性以及新的[Pt(CIS-1,3-二烷基烷烃的作用机制的研究)Cl-2]复合物,其中Thecis-1,3-二氨基环烷基组含有环丁基,环戊基和环己基部分。我们证明[Pt(CIS-1,3-DACH)CL-2]破坏具有比其他两种研究的1,3-氨基环烷烃或顺铂的更高效率的癌细胞。此外,研究的[Pt(CIS-1,3-二氨基环烷烃)CL-2]复合物相对于非致瘤正常细胞显示对肿瘤细胞的选择性。我们还专注于理解双官能铂(II)复合物的抗肿瘤活性机理的一些早期步骤的无细胞培养基中的几项机制研究。我们的数据表明,研究的[Pt(CIS-1,3-二氨基环烷烃)Cl-2]复合物和顺铂与谷胱甘肽和DNA结合的反应性与癌细胞中这些铂(II)复合物的抗增殖活性不相关。相反,我们表明[Pt(CIS-1,3-DACH)CL-2]的癌细胞中较高的抗增殖活性起源于其最高疏水性和最有效的细胞摄取。图形摘要

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