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综合基因监测的应用:检测环境致癌物的最佳方法。

Application of integrated genetic monitoring: the optimal approach for detecting environmental carcinogens.

作者信息

Legator M S, Au W W

机构信息

Department of Preventive Medicine and Community Health, University of Texas Medical Branch, Galveston 77555-1010.

出版信息

Environ Health Perspect. 1994 Nov;102 Suppl 9(Suppl 9):125-32. doi: 10.1289/ehp.94102s9125.

Abstract

Short-term in vitro genetic toxicity assays have not fulfilled their anticipated role in predicting the carcinogenicity of environmental agents reliably and economically. A reduction in emphasis from nonanimal systems to relevant animal assays and population monitoring will help to reestablish the credibility of this field. An analysis of the various steps in the carcinogenic process indicates the biological responses occurring during these stages can be utilized for early detection of environmental carcinogens. Emphasis should be placed on using the earliest significant response that indicates genetic damage (e.g., gene mutations and chromosome alterations). Assays that detect pregenomic damage (e.g., adduct formation), without evidence of subsequent heritable genetic alterations, may produce misleading results for risk assessment and should not be considered as stand-alone monitoring procedures. Late biological responses may occur in tissues or organs where genetic damage may be difficult to measure, and the opportunity for intervention diminishes as we approach the clinical outcome. For example, analyzing localized cells that contain activated protooncogenes and inactivated tumor suppressor genes, although they further document adverse response from exposure to carcinogens, may be of greater value for indicating clinical outcome than for genetic monitoring. With few notable exceptions, the window of opportunity for genetic monitoring is the period after exposure where genetic damage is evident and where circulating lymphocytes can faithfully record this damage. An ongoing study of butadiene-exposed workers illustrates an optimum protocol, where multiple assays can be carried out and correlated with both external and internal measurements of exposure.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

短期体外遗传毒性试验未能在可靠且经济地预测环境因子致癌性方面发挥预期作用。从非动物系统向相关动物试验及人群监测的重点转移,将有助于重建该领域的可信度。对致癌过程中各个步骤的分析表明,这些阶段发生的生物学反应可用于早期检测环境致癌物。应着重利用表明遗传损伤(如基因突变和染色体改变)的最早显著反应。检测基因组前损伤(如加合物形成)但无后续可遗传基因改变证据的试验,可能会产生误导性的风险评估结果,不应被视为独立的监测程序。晚期生物学反应可能发生在难以测量遗传损伤的组织或器官中,且随着我们接近临床结果,干预的机会也会减少。例如,分析含有活化原癌基因和失活肿瘤抑制基因的局部细胞,尽管它们进一步证明了接触致癌物后的不良反应,但对于指示临床结果而言,可能比对遗传监测更有价值。除少数显著例外,遗传监测的机会窗口是暴露后遗传损伤明显且循环淋巴细胞能如实记录这种损伤的时期。一项针对接触丁二烯工人的正在进行的研究说明了一种最佳方案,即可以进行多种检测,并将其与外部和内部暴露测量结果相关联。(摘要截选至250字)

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