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Comparison of Harvey ras and Kirstenras activity in rat mammary carcinogenesis.

机译:Harvey ras和Kirstenras活性在大鼠乳腺癌变中的比较。

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摘要

In cancers where mutations in the closely related Harvey ras, Kirsten ras, or N-ras genes are observed, one ras gene family member is often found mutated to the exclusion of other ras gene family members. Yet, the mechanism(s) responsible for tissue-selective ras gene mutations are not known. The overall goal of this thesis was to further characterize and evaluate the selective activation of the Harvey ras gene in the rat mammary carcinogenesis model. Three studies were performed in this thesis. The first study investigated ras gene activation in rats exposed to the carcinogen N-nitroso-N-methylurea (NMU) at different ages. A significant number of mammary carcinomas developed in rats exposed during both sexual development and senescence. Mutations in the Harvey ras gene were found in carcinomas from rats exposed to NMU during sexual development, but not those resulting from NMU exposure to senescent rats. No Kirsten ras gene mutations were found in mammary carcinomas from rats exposed to NMU at any age. In a second study, replication-defective retroviral vectors were used to express activated forms of the Harvey ras and Kirsten ras genes in rat mammary parenchyma. Although infection with the activated form of Kirsten ras led to the efficient development of rat mammary carcinomas, ten-fold higher numbers of mammary carcinomas were observed with the Harvey ras gene expressing vectors. In a third study, transgenic rats were produced that express the Harvey ras gene or the Kirsten ras gene controlled by the regulatory elements of the rat Harvey ras gene. Transgenic rats overexpressing Harvey Ras developed half as many tumors after NMU exposure as their non-transgenic littermates, whereas mammary carcinoma development was not significantly different in transgenic rats expressing the Kirsten ras gene driven by Harvey ras gene regulatory elements compared to their non-transgenic littermates. The collective results from these studies support a dominant role for Harvey ras in rat mammary carcinogenesis that is dependent on ras activity at the protein level.
机译:在观察到密切相关的Harvey ras,Kirsten ras或N-ras基因突变的癌症中,经常发现一个ras基因家族成员发生了突变,从而排除了其他ras基因家族成员。然而,负责组织选择性ras基因突变的机制尚不清楚。本论文的总体目标是进一步表征和评估大鼠乳腺癌变模型中Harvey ras基因的选择性激活。本论文进行了三项研究。第一项研究调查了暴露于不同年龄致癌物N-亚硝基-N-甲基脲(NMU)的大鼠中的ras基因激活。在性发育和衰老期间暴露的大鼠中发展出大量的乳癌。在性发育过程中暴露于NMU的大鼠的癌中发现了Harvey ras基因的突变,但在衰老大鼠中暴露于NMU的癌却未发现这些突变。在任何年龄的暴露于NMU的大鼠的乳癌中均未发现Kirsten ras基因突变。在第二项研究中,复制缺陷型逆转录病毒载体用于在大鼠乳腺实质中表达Harvey ras和Kirsten ras基因的活化形式。尽管用活化形式的Kirsten ras感染导致大鼠乳腺癌的有效发展,但使用Harvey ras基因表达载体观察到的乳腺癌数目高出十倍。在第三项研究中,产生了转基因大鼠,它们表达受大鼠Harvey ras基因调控元件控制的Harvey ras基因或Kirsten ras基因。过度表达Harvey Ras的转基因大鼠在NMU暴露后发生的肿瘤数量是其非转基因同窝仔的一半,而在表达由Harvey ras基因调控元件驱动的Kirsten ras基因的转基因大鼠中,其乳癌的发展与非转基因同窝仔相比没有显着差异。 。这些研究的总体结果支持了Harvey ras在大鼠乳癌中的主要作用,该作用取决于蛋白水平上的ras活性。

著录项

  • 作者

    Thompson, Todd Anthony.;

  • 作者单位

    The University of Wisconsin - Madison.;

  • 授予单位 The University of Wisconsin - Madison.;
  • 学科 Oncology.;Toxicology.
  • 学位 Ph.D.
  • 年度 1997
  • 页码 234 p.
  • 总页数 234
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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