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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Structural and mechanistic bases for the induction of mitotic chromosomal loss and duplication ('malsegregation') in the yeast Saccharomyces cerevisiae: relevance to human carcinogenesis and developmental toxicology.
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Structural and mechanistic bases for the induction of mitotic chromosomal loss and duplication ('malsegregation') in the yeast Saccharomyces cerevisiae: relevance to human carcinogenesis and developmental toxicology.

机译:酿酒酵母中诱导有丝分裂染色体丢失和复制(“分离不良”)的结构和机制基础:与人类致癌作用和发育毒理学有关。

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MultiCASE has the ability to automatically determine the structural features responsible for the biological activity of chemicals. In the present study, 93 chemicals tested for their ability to induce chromosomal 'malsegregation' in the yeast Saccharomyces cerevisiae were analyzed. This 'malsegregation' mimics molecular events that occur during human development and carcinogenesis resulting in an effective loss of one chromosome of an autosomal pair and duplication of the homologue. Structural features associated with the ability to induce such chromosome loss and duplication were identified and compared with those obtained from examination of other toxicological data bases. The most significant structural similarities were identified between the induction of chromosomal malsegregation and several toxicological phenomena such as cellular toxicity, induction of sister chromatid exchanges in vitro and rodent developmental toxicity. Very significant structural similarities were also found with systemic toxicity, induction of micronuclei in vivo and human developmental toxicity. Less significant structural overlaps were found between yeast malsegregation and rodent carcinogenicity, DNA reactivity and mutagenicity, and the induction of chromosome aberrations in vitro and sister chromatid exchanges in vivo. These overlaps may indicate mechanistic similarities between the induction of chromosomal malsegregation and other toxicological phenomena. The predictivity of the SAR model derived from the present data base is relatively low, however. This may be merely a reflection of the small size and composition of the data base, however, further analyses suggest that it reflects primarily the multiple mechanisms responsible for the induction of chromosomal malsegregation in yeast and the complexity of the phenomenon.
机译:MultiCASE具有自动确定负责化学物质生物活性的结构特征的能力。在本研究中,对93种化学物质进行了测试,这些化学物质诱导了酿酒酵母中的染色体“异常分离”。这种“不正确的分离”模仿了人类发育和致癌过程中发生的分子事件,从而导致常染色体对中一条染色体的有效缺失和同源物的重复。鉴定了与诱导这种染色体丢失和复制的能力有关的结构特征,并将其与从其他毒理学数据库中获得的结构特征进行了比较。在诱导染色体错误分离和几种毒理学现象(如细胞毒性,体外诱导的姐妹染色单体交换和啮齿类动物发育毒性)之间发现了最重要的结构相似性。在全身毒性,体内微核诱导和人类发育毒性方面也发现了非常显着的结构相似性。在酵母菌的偏分离和啮齿动物的致癌性,DNA反应性和诱变性之间以及在体外诱导染色体畸变和体内姊妹染色单体交换之间,发现的结构重叠不太明显。这些重叠可能表明在染色体错误分离和其他毒理学现象之间的机理相似性。但是,从当前数据库得出的SAR模型的可预测性相对较低。这可能只是数据库的小规模和组成的反映,但是,进一步的分析表明,它主要反映了导致酵母中染色体错误分离和现象复杂性的多种机制。

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