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二甲基苯并蒽(DMBA)及其K区域硫代类似物的致癌效力与小鼠皮肤32P后标记及突变-R小鼠乳糖Z基因突变数据的相关性:与标准遗传毒性试验中观察到的活性比较

Correlation of carcinogenic potency with mouse-skin 32P-postlabeling and muta-Rmouse lac Z- mutation data for DMBA and its K-region sulphur isostere: comparison with activities observed in standard genotoxicity assays.

作者信息

Ashby J, Brusick D, Myhr B C, Jones N J, Parry J M, Nesnow S, Paton D, Tinwell H, Rosenkranz H S, Curti S

机构信息

ZENECA Central Toxicology Laboratory, Alderley Park, Macclesfield, UK.

出版信息

Mutat Res. 1993 Aug;292(1):25-40. doi: 10.1016/0165-1161(93)90005-k.

Abstract

The genotoxicities in vitro and in vivo of the mouse-skin carcinogen 7,12-dimethylbenz[a]anthracene (DMBA) have been compared with those of its weakly carcinogenic 4,5-sulphur analogue, 6,11-dimethylbenzo[b]naphtho-[2,3-d]thiophene (S-DMBA). The only datasets that correlated with the relative carcinogenicity of these agents to the skin were those conducted using topically exposed mouse skin. Thus, both chemicals induced lacZ- mutations in the skin of lacZ+ transgenic mice, and both produced DNA adducts on mouse-skin DNA as assessed using the 32P-postlabeling technique. In each case, DMBA gave a stronger response than did S-DMBA. In contrast to these responses, only DMBA was active in the mouse bone-marrow micronucleus assay and in the C3H10T1/2 in vitro cell transformation assay. Both chemicals were mutagenic to Salmonella and of approximately equal potency. The molecular geometry of DMBA and S-DMBA are compared, and divergent CASE predictions of activity in the Salmonella assay and skin-painting bioassay are discussed. The importance of conducting predictive genotoxicity assays in systems close to those in which carcinogenicity is to be assessed is emphasized by these data.

摘要

已将小鼠皮肤致癌物7,12-二甲基苯并[a]蒽(DMBA)与其弱致癌性的4,5-硫类似物6,11-二甲基苯并[b]萘并[2,3-d]噻吩(S-DMBA)的体外和体内遗传毒性进行了比较。唯一与这些试剂对皮肤的相对致癌性相关的数据集是使用局部暴露的小鼠皮肤进行的那些。因此,两种化学物质均在lacZ +转基因小鼠的皮肤中诱导lacZ突变,并且如使用32P后标记技术所评估的那样,两者均在小鼠皮肤DNA上产生DNA加合物。在每种情况下,DMBA的反应均比S-DMBA更强。与这些反应相反,只有DMBA在小鼠骨髓微核试验和C3H10T1 / 2体外细胞转化试验中具有活性。两种化学物质对沙门氏菌均具有致突变性,且效力大致相同。比较了DMBA和S-DMBA的分子几何结构,并讨论了沙门氏菌试验和皮肤涂抹生物试验中活性的不同CASE预测。这些数据强调了在接近要评估致癌性的系统中进行预测性遗传毒性试验的重要性。

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