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利用转基因小鼠模型在短期生物测定中识别化学致癌物并评估潜在风险。

Identifying chemical carcinogens and assessing potential risk in short-term bioassays using transgenic mouse models.

作者信息

Tennant R W, French J E, Spalding J W

机构信息

Laboratory of Environmental Carcinogenesis and Mutagenesis, National Institute of Environmental Health Sciences, Research Triangle Park, NC 27709, USA.

出版信息

Environ Health Perspect. 1995 Oct;103(10):942-50. doi: 10.1289/ehp.95103942.

Abstract

Cancer is a worldwide public health concern. Identifying carcinogens and limiting their exposure is one approach to the problem of reducing risk. Currently, epidemiology and rodent bioassays are the means by which putative human carcinogens are identified. Both methods have intrinsic limitations: they are slow and expensive processes with many uncertainties. The development of methods to modify specific genes in the mammalian genome has provided promising new tools for identifying carcinogens and characterizing risk. Transgenic mice may provide advantages in shortening the time required for bioassays and improving the accuracy of carcinogen identification; transgenic mice might now be included in the testing armamentarium without abandoning the two-year bioassay, the current standard. We show that mutagenic carcinogens can be identified with increased sensitivity and specificity using hemizygous p53 mice in which one allele of the p53 gene has been inactivated. Furthermore, the TG.AC transgenic model, carrying a v-Ha-ras construct, has developed papillomas and malignant tumors in response to a number of mutagenic and nonmutagenic carcinogens and tumor promoters, but not to noncarcinogens. We present a decision-tree approach that permits, at modest extra cost, the testing of more chemicals with improved ability to extrapolate from rodents to humans.

摘要

癌症是一个全球性的公共卫生问题。识别致癌物并限制对其接触是降低风险问题的一种解决方法。目前,流行病学和啮齿动物生物测定法是识别潜在人类致癌物的手段。这两种方法都有内在局限性:它们是缓慢且昂贵的过程,存在许多不确定性。在哺乳动物基因组中修饰特定基因的方法的发展为识别致癌物和表征风险提供了有前景的新工具。转基因小鼠在缩短生物测定所需时间和提高致癌物识别准确性方面可能具有优势;现在可以将转基因小鼠纳入测试手段,而不摒弃当前标准的两年生物测定法。我们表明,使用p53基因一个等位基因已失活的半合子p53小鼠,可以更高的灵敏度和特异性识别诱变致癌物。此外,携带v-Ha-ras构建体的TG.AC转基因模型,已针对多种诱变和非诱变致癌物及肿瘤启动剂产生了乳头状瘤和恶性肿瘤,但对非致癌物无反应。我们提出了一种决策树方法,该方法只需适度增加成本,就能以更高的从啮齿动物外推至人类的能力测试更多化学品。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/076c/1519166/4a1cb43204eb/envhper00358-0071-a.jpg

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