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对在哺乳动物细胞培养中测试的951种化学物质的致断裂性数据进行的比较分析。

A comparative analysis of data on the clastogenicity of 951 chemical substances tested in mammalian cell cultures.

作者信息

Ishidate M, Harnois M C, Sofuni T

机构信息

Division of Mutagenesis, National Institute of Hygienic Sciences, Tokyo, Japan.

出版信息

Mutat Res. 1988 Mar;195(2):151-213. doi: 10.1016/0165-1110(88)90023-1.

Abstract

A literature review was conducted using original papers published during 1964-1985 on the in vitro clastogenicity of chemical substances. Results of tests on 951 chemical substances were abstracted from over 240 reports to form the database. The evaluation of these data relied on each author's original conclusion on a positive or negative outcome. Of these 951 substances, 447 (47%) were consistently positive either with or without activation; 417 (44%) were negative in the direct test but not tested with metabolic activation systems; 4 were negative but tested only with activation; and 30 (3%) were clearly negative both with and without activation. The remaining 53 substances gave variable results when tested under different experimental protocols or in different cell types, but were positive in at least one test. Although discrepant results were found associated with some cell types, the addition of metabolic activation systems tended to eliminate such variability. No one cell appeared to be superior in response to all clastogens. For screening purposes, the choice of cell may thus depend more on the general usefulness and reliability of a cell type than on a strong response to a particular chemical. However, the use of a suitable metabolic activation system does appear to be of critical importance. The concentration at which clastogenic effects were detected varied extensively for different test substances, ranging from a minimum of 4.3 X 10(-8) to 6.9 X 10(2) mM. Possible mechanisms of action for substances active at only high levels are discussed, but no satisfactory explanation is available at this time. The relevance of tests conducted at concentrations high enough to alter significantly the osmolarity and other culture conditions is considered, and caution urged in the interpretation of test results obtained under physiologically stressful conditions. The clastogenic potential was compared quantitatively using an index of effective concentration (D20) and one which estimates the number of cells with exchange aberrations expected per mg/ml (TR) for data obtained by using a uniform protocol and cultures of Chinese hamster lung (CHL) cells. Both values were distributed over a wide range, demonstrating the variety of genotoxic potential in chemicals. In general, a substance which was active at only high concentrations produced fewer exchange-type aberrations. In vivo activity, as measured by tumourigenic effect and formation of micronuclei in bone marrow, tended to be greater for substances with a D20 below 10(-2) mg/ml and a TR value over 10(3).(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

我们检索了1964年至1985年间发表的关于化学物质体外致断裂性的原始论文,进行了文献综述。从240多篇报告中提取了951种化学物质的测试结果,形成了数据库。对这些数据的评估依赖于每位作者对阳性或阴性结果的原始结论。在这951种物质中,447种(47%)无论有无激活都始终呈阳性;417种(44%)在直接测试中呈阴性,但未用代谢激活系统进行测试;4种呈阴性,但仅用激活进行了测试;30种(3%)无论有无激活均明显呈阴性。其余53种物质在不同实验方案或不同细胞类型下测试时结果不一,但至少在一项测试中呈阳性。尽管在某些细胞类型中发现了不一致的结果,但添加代谢激活系统往往会消除这种变异性。没有一种细胞对所有致断裂剂的反应都表现出优势。因此,出于筛选目的,细胞的选择可能更多地取决于细胞类型的一般实用性和可靠性,而不是对特定化学物质的强烈反应。然而,使用合适的代谢激活系统似乎至关重要。不同测试物质检测到致断裂效应的浓度差异很大,范围从最低的4.3×10⁻⁸到6.9×10² mM。讨论了仅在高浓度下有活性的物质的可能作用机制,但目前尚无令人满意的解释。考虑了在足以显著改变渗透压和其他培养条件的高浓度下进行测试的相关性,并敦促在解释在生理应激条件下获得的测试结果时要谨慎。使用有效浓度指数(D20)和估计每毫克/毫升预期有交换畸变细胞数的指数(TR),对使用统一方案和中国仓鼠肺(CHL)细胞培养物获得的数据进行定量比较致断裂潜力。这两个值分布范围很广,表明化学物质的遗传毒性潜力各不相同。一般来说,仅在高浓度下有活性的物质产生的交换型畸变较少。通过致瘤效应和骨髓微核形成来衡量的体内活性,对于D20低于10⁻²毫克/毫升且TR值超过10³的物质往往更大。(摘要截选至400字)

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