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培养的小鼠胚胎在妊娠早期代谢苯并[a]芘:可通过姐妹染色单体交换检测到的遗传差异。

Cultured mouse embryos metabolize benzo[a]pyrene during early gestation: genetic differences detectable by sister chromatid exchange.

作者信息

Galloway S M, Perry P E, Meneses J, Nebert D W, Pedersen R A

出版信息

Proc Natl Acad Sci U S A. 1980 Jun;77(6):3524-8. doi: 10.1073/pnas.77.6.3524.

Abstract

Mouse embryos explanted at 7 1/2 or 8 1/2 days of gestation were cultured in medium containing benzo[a]pyrene and supplemented with 5-bromodeoxyuridine to allow detection of sister chromatid exchanges. The murine Ah locus regulates the inducible metabolism of polycyclic hydrocarbons such as benzo[a]pyrene. A high frequency of sister chromatid exchange was induced by benzo[a]pyrene in embryos from three Ah-"responsive" inbred strains (BALB/cDub, C3H/AnfCum, and C57BL/6N); there was little or no increase in two Ah-"nonresponsive" inbred strains (AKR/J and DBA/2J). Benzo[a]pyrene also induced sister chromatid exchanges in the Ah-responsive recombinant inbred line B6NXAKN-12 but not in the Ah-nonresponsive recombinant inbred line B6NXAKN-3. Sister chromatid exchange in cultured Ah-responsive mouse embryos was thus shown to be a sensitive assay. These data provide direct evidence that genetically responsive mouse embryos (early postimplantation stage) possess the subcellular processes necessary for induction of enzymes that metabolize benzo[a]pyrene to its chemically active forms(s). Both the Ah regulatory gene product (a cytoslic receptor) and the structural gene product (inducible cytochrome P1-450) therefore appear to be functional at an early embryonic age. Furthermore, this metabolic capacity may play an important role in the damage to embryonic cells by polycyclic hydracarbons.

摘要

将妊娠7.5天或8.5天的小鼠胚胎植入含有苯并[a]芘的培养基中培养,并添加5-溴脱氧尿苷以检测姐妹染色单体交换。小鼠的Ah基因座调节多环烃如苯并[a]芘的诱导代谢。苯并[a]芘在三种Ah“反应性”近交系(BALB/cDub、C3H/AnfCum和C57BL/6N)的胚胎中诱导了高频率的姐妹染色单体交换;在两种Ah“无反应性”近交系(AKR/J和DBA/2J)中几乎没有增加或没有增加。苯并[a]芘在Ah反应性重组近交系B6NXAKN-12中也诱导了姐妹染色单体交换,但在Ah无反应性重组近交系B6NXAKN-3中没有。因此,培养的Ah反应性小鼠胚胎中的姐妹染色单体交换被证明是一种灵敏的检测方法。这些数据提供了直接证据,表明具有遗传反应性的小鼠胚胎(植入后早期阶段)拥有将苯并[a]芘代谢为其化学活性形式所需的亚细胞过程。因此,Ah调节基因产物(一种胞质受体)和结构基因产物(诱导型细胞色素P1-450)似乎在胚胎早期就发挥作用。此外,这种代谢能力可能在多环烃对胚胎细胞的损伤中起重要作用。

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