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硫酸二乙酯和硫酸二甲酯处理DNA后的大分子复合物形成及其他效应:物理化学和电子显微镜研究

Formation of macromolecular complexes and other effects of DNA treatment with diethyl and dimethyl sulfate: physico-chemical and electron microscopic studies.

作者信息

Kubinski H, Kubinski Z O, Fiandt M, Konopa G

出版信息

Carcinogenesis. 1981;2(10):981-90. doi: 10.1093/carcin/2.10.981.

Abstract

In vitro exposures of isolated DNA to one of the two carcinogenic and mutagenic chemicals, diethylsulfate or dimethylsulfate, induces several kinds of physicochemical and morphological alterations. These changes are detectable by a variety of independent techniques. A fraction of DNA treated briefly with either of these two chemicals moves during velocity centrifugation experiments less rapidly than the bulk of control DNA and more rapidly through gels during electrophoresis. This apparent decrease in size is paralleled by the formation of large DNA aggregates with mobilities indicating molecular weights several times that of the untreated, control DNA. The presence of a basic protein in the incubation mixture increases the rate of formation of such complexes. the tendency of the alkylated DNA to bind to both biological and non-biological materials is reflected in the increased attachment of DNA to columns built with methyl-esterified serum albumin and in its quantitative retention on nitrocellulose filters. DNA exposed to dimethylsulfate decreases its density in CsCl gradients. A mixture of two or more DNAs of different densities exposed to this chemical produces an u.v.-absorbing band which is found in such gradients at an intermediate density. If the alkylation reaction is carried out in the presence of a protein, a portion of DNA bands at a density intermediate between the density of DNA and that of the protein, even in the presence of an ionic detergent in the gradient. Under the electron microscope the alkylated DNA shows multiple single-strand breaks and peeling-off whiskers of denatured DNA. Aggregates of DNA molecules become visible upon further incubation of DNA with the alkylating agent. We suggest that the DNA-DNA and DNA- protein complexes play an important role in the process of carcinogenesis and mutagenesis.

摘要

将分离出的DNA在体外暴露于两种致癌和致突变化学物质之一,即硫酸二乙酯或硫酸二甲酯,会引发多种物理化学和形态学改变。这些变化可用多种独立技术检测到。用这两种化学物质中的任何一种短暂处理过的一部分DNA,在速度离心实验中移动速度比大部分对照DNA慢,而在电泳过程中通过凝胶的速度更快。这种明显的尺寸减小伴随着大的DNA聚集体的形成,其迁移率表明分子量是未处理的对照DNA的几倍。孵育混合物中碱性蛋白质的存在会增加此类复合物的形成速率。烷基化DNA与生物和非生物材料结合的倾向体现在DNA与用甲基酯化血清白蛋白构建的柱的结合增加以及其在硝酸纤维素滤膜上的定量保留。暴露于硫酸二甲酯的DNA在CsCl梯度中密度降低。暴露于这种化学物质的两种或更多种不同密度的DNA混合物会产生一个紫外吸收带,在这样的梯度中可以在中间密度处找到。如果烷基化反应在蛋白质存在下进行,即使在梯度中有离子去污剂,一部分DNA条带的密度也介于DNA和蛋白质的密度之间。在电子显微镜下,烷基化的DNA显示出多个单链断裂和变性DNA的剥离须状物。将DNA与烷基化剂进一步孵育后,DNA分子聚集体变得可见。我们认为DNA-DNA和DNA-蛋白质复合物在致癌和致突变过程中起重要作用。

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