首页> 外文期刊>Teratogenesis, carcinogenesis, and mutagenesis >Cyclophosphamide: Interstrain differences in the production of mutagenic metabolites by S9‐fractions from liver and kidney in different mutagenicity test systems in vitro and in the teratogenic response in vivo between CBA and C 57 BL mice
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Cyclophosphamide: Interstrain differences in the production of mutagenic metabolites by S9‐fractions from liver and kidney in different mutagenicity test systems in vitro and in the teratogenic response in vivo between CBA and C 57 BL mice

机译:环磷酰胺:在体外不同致突变性测试系统中,肝脏和肾脏的S9级分产生诱变代谢物的菌株间差异以及CBA和C 57 BL小鼠体内致畸反应的差异

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AbstractThe formation of mutagenic compounds from cyclophosphamide (CPA) by S9‐fractions from liver (S9L) or kidney (S9K) of pregnant CBA and C 57 BL mice was investigated, using point mutations inSalmonella typhimurium(TA 1535) and the induction of sister chromatid exchanges (SCE) in human peripheral lymphocytes (HPL) or Chinese hamster ovary (CHO) cells as end points. In addition, the teratological response of CBA and C 57 BL mice to CPA on day 11 of pregnancy was analysed in vivo.The results are as follows: (1) S9L from CBA mice was more effective than S9L from C 57 BL mice in metabolizing CPA to products inducing mutations inSalmonellaand SCEs in HPL and CHO cells. (2) S9L was more effective than S9K from both strains of mice. (3) In vivo pretreatment of mice with a single dose of CPA (20 mg/kg) reduced the in vitro metabolizing capacity of S9L and S9K significantly and led to the disappearance of the interstrain difference. (4) The embryolethal and teratogenic effects of CPA were stronger in C 57 BL than in CBA mice; the types of teratological effects were partially different in the two strain
机译:摘要以鼠伤寒沙门氏菌(TA 1535)的点突变和诱导人外周淋巴细胞(HPL)或中国仓鼠卵巢(CHO)细胞中姐妹染色单体交换(SCE)为终点,研究了妊娠CBA和C57 BL小鼠肝脏(S9L)或肾脏(S9K)S9组分形成环磷酰胺(CPA)诱变化合物。此外,还分析了CBA和C 57 BL小鼠在妊娠第11天对CPA的畸形反应。结果如下:(1)CBA小鼠的S9L比C 57 BL小鼠的S9L在将CPA代谢为HPL和CHO细胞中沙门氏菌和SCEs突变的产物更有效。(2)两种小鼠品系的S9L均比S9K更有效。(3)单剂量CPA(20 mg/kg)小鼠体内预处理显著降低S9L和S9K的体外代谢能力,导致菌株间差异消失。(4)CPA在C 57 BL中的胚胎致死和致畸作用强于CBA小鼠;两种菌株的致畸效应类型部分不同

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