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生物分子对诱变剂和致癌物的直接拦截。

Direct interception of mutagens and carcinogens by biomolecules.

作者信息

Hartman P E, Hartman Z

机构信息

Department of Biology, Johns Hopkins University, Baltimore, Maryland 21218.

出版信息

Basic Life Sci. 1993;61:351-66. doi: 10.1007/978-1-4615-2984-2_33.

Abstract

Five points are emphasized: 1. Chemical interception and mere physical exclusion of mutagens and carcinogens constitute the major means by which mutations in cellular DNA are prevented. DNA repair processes comprise critical, but relatively minor, modes of genetic protection. 2. Disruption of a mutagen-interception defense mechanism can lead to substantial increases in mutagenesis and can preordain sites to eventual tumor formation. 3. Quantitation of the relative contributions of various blocking molecules is often simplified by the fact that protection can be calculated merely through knowledge of the measured concentration of the antimutagen and its rate of reaction with specific mutagens as measured in straightforward in vitro tests. 4. Two recently recognized defensive molecules, carnosine and ergothioneine, are put ++forward as examples of interesting chemical interceptor molecules. 5. Essentially all antimutagens are in fact "double-edged swords." Situations can be artificially constructed that can lead to generation of toxic species from molecules that are normally antimutagens; in isolated cases some of these interactions can be pictured as having deleterious consequences in vivo. This may be one reason why a number of important antimutagens are often sequestered, either in different tissues or by binding to dispensable macromolecules.

摘要

强调了五点

  1. 对诱变剂和致癌物的化学拦截以及单纯的物理排除是预防细胞DNA突变的主要手段。DNA修复过程是重要但相对次要的遗传保护模式。2. 诱变剂拦截防御机制的破坏会导致诱变作用大幅增加,并可能预先确定最终形成肿瘤的部位。3. 各种阻断分子相对贡献的定量通常因以下事实而简化:仅通过了解抗诱变剂的测量浓度及其与特定诱变剂的反应速率(如在简单的体外试验中测量)就可以计算保护作用。4. 最近发现的两种防御分子,肌肽和麦角硫因,被作为有趣的化学拦截分子的例子提出。5. 实际上,所有抗诱变剂都是“双刃剑”。可以人为构建一些情况,导致通常作为抗诱变剂的分子产生有毒物质;在个别情况下,其中一些相互作用在体内可能会产生有害后果。这可能是一些重要抗诱变剂经常被隔离的原因之一,要么在不同组织中,要么通过与可消耗的大分子结合。

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