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小鼠体内苯并(a)芘羟化酶的产前诱导

Prenatal induction of benzo(a)pyrene hydroxylases in mice.

作者信息

Neubert D, Tapken S

机构信息

Institut für Toxikologie und Embryopharmakologie, Freie Universität Berlin.

出版信息

Arch Toxicol. 1988;62(2-3):192-9. doi: 10.1007/BF00570139.

Abstract
  1. Benzo(a)pyrene hydroxylase (BPH) activity was measured in homogenates of fetal liver (day 18) or of whole-embryos of mice on day 9, 10 or 12 of gestation after maternal pretreatment with B(a)P on 3 consecutive days. A 3H-liberation assay with 3H-B(a)P labelled either generally or at the 6-position was used. The values obtained with the embryonic/fetal tissues were compared with those found in maternal liver. 2. Three oral doses of 17.5 mg B(a)P/kg body wt were found to just significantly induce BPH in maternal liver. An induction was observed after pretreatment with 24 mg B(a)P/kg body wt in 9-, 10- or 12-day-old whole-embryos, but the Vmax reached was only 10-20% (1% on day 9) of that of adult non-induced liver. The Km (6-hydroxylation) for all tissues tested were in the same range (600-900 nM). The induction was demonstrable in embryos at tissue levels about one order of magnitude lower than those required for induction in maternal liver. 3. Treatment with 25 mg B(a)P/kg body wt on 3 consecutive days was required to induce BPH in fetal liver on day 18 of gestation. The required B(a)P tissue concentrations were about one half of those necessary for induction in maternal liver. 4. Among a variety of other polycyclic hydrocarbons only chrysene showed an inducing potency similar to that of B(a)P in adult and fetal liver. For all compounds tested there was no correlation found in the inducing potency between adult and fetal liver (e.g. coronene).(ABSTRACT TRUNCATED AT 250 WORDS)
摘要
  1. 在妊娠第9、10或12天的小鼠全胚胎或第18天的胎肝匀浆中,测量苯并(a)芘羟化酶(BPH)活性。孕母连续连续连续连续3天经苯并(a)芘预处理。使用用3H标记的苯并(a)芘(一般标记或在6位标记)的3H释放测定法。将胚胎/胎儿组织获得的值与母肝中的值进行比较。2. 发现口服3剂17.5毫克/千克体重的苯并(a)芘仅能显著诱导母肝中的BPH。在9、10或12日龄的全胚胎中,用24毫克/千克体重的苯并(a)芘预处理后观察到诱导作用,但达到的Vmax仅为成年未诱导肝脏的10%-20%(第9天为1%)。所有测试组织的Km(6-羟基化)在相同范围内(600-900纳摩尔)。在胚胎中,诱导作用在组织水平上比母肝诱导所需水平低约一个数量级时即可显现。3. 在妊娠第18天的胎肝中诱导BPH需要连续3天用25毫克/千克体重的苯并(a)芘处理。所需的苯并(a)芘组织浓度约为母肝诱导所需浓度的一半。4. 在多种其他多环烃中,只有屈在成年和胎儿肝脏中的诱导能力与苯并(a)芘相似。对于所有测试的化合物,在成年和胎儿肝脏的诱导能力之间未发现相关性(例如晕苯)。(摘要截断于250字)

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