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顺式和反式铂(II)及铂(IV)化合物对小牛胸腺脱氧核糖核酸的复性作用。

Renaturation effects of cis and trans platinum II and IV compounds on calf thymus deoxyribonucleic acid.

作者信息

Harder H C

出版信息

Chem Biol Interact. 1975 Jan;10(1):27-39. doi: 10.1016/0009-2797(75)90044-7.

Abstract

The effects of cis dichlorodiammine platinum [cis Pt(II)], trans dichlorodiammine platinum (trans Pt(II)], cis tetrachlorodiammine platinum [cis Pt(IV)], trans tetrachlorodiammine platinum [trans Pt(IV)], and ethylenediaminedichloride platinum [Pt(II)en] on the absorption spectra, and thermal hyper- and hypochromicity of calf thymus DNA were investigated. Platinum-induced renaturation was studied as one parameter of interstrand cross-linking. Based on a DNA cross-linking hypothesis, the tumor-inhibitory platinum compounds cis Pt(II), cis Pt(IV) and Pt(II)en would be expected to induce renaturation following thermal denaturation, whereas the ineffective drugs, trans Pt(II) and trans Pt(IV) would not. All five bind to DNA in such a way as to induce renaturation. However, cis Pt(IV) requires at least a 3- to 4-fold longer incubation time than is required by the other compounds to form the coordination bonds necessary for renaturation. Maximum renaturation with all compounds was observed at a molar Pt/base ratio of 0.05 except cis Pt(IV), with which it was 0.25. The rate of the formation of the platinum-coordinated cross-links by fresh cis Pt(II) suggests two reactions or types of reactions occur. The first is rapid and destabilizes the DNA helix, whereas the second is slow and responsible for renaturation following thermal denaturation. These results suggest that cis Pt(IV) may be activated cellularly and that cross-linking is not the primary mechanism of action of the tumor-inhibitory platinum compounds.

摘要

研究了顺二氯二氨合铂[顺式Pt(II)]、反二氯二氨合铂(反式Pt(II))、顺四氯二氨合铂[顺式Pt(IV)]、反四氯二氨合铂[反式Pt(IV)]以及乙二胺二氯化铂[Pt(II)en]对小牛胸腺DNA吸收光谱和热增色性及减色性的影响。研究了铂诱导的复性作为链间交联的一个参数。基于DNA交联假说,预计具有肿瘤抑制作用的铂化合物顺式Pt(II)、顺式Pt(IV)和Pt(II)en在热变性后会诱导复性,而无效药物反式Pt(II)和反式Pt(IV)则不会。所有这五种化合物均以诱导复性的方式与DNA结合。然而,顺式Pt(IV)形成复性所需的配位键所需的孵育时间比其他化合物至少长3至4倍。除顺式Pt(IV)的摩尔Pt/碱基比为0.25外,所有化合物在摩尔Pt/碱基比为0.05时观察到最大复性。新鲜顺式Pt(II)形成铂配位交联的速率表明发生了两种反应或两类反应。第一种反应迅速,会使DNA螺旋不稳定,而第二种反应缓慢,是热变性后复性的原因。这些结果表明顺式Pt(IV)可能在细胞内被激活,并且交联不是具有肿瘤抑制作用的铂化合物的主要作用机制。

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