Behavioral and developmental effects of prenatal exposure to pentazocine and tripelennamine combinations.

C D Driscoll, L S Meyer, E P Riley
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Abstract

Long-Evans, hooded rats were intubated with one of four dose combinations of pentazocine and tripelennamine on Days 7-20 of pregnancy: 0:0 (mg/kg pentazocine:tripelennamine), 20:10, 40:0, or 40:20. An additional group had free access to lab chow and water throughout pregnancy. At birth, reduced body weights were evident in all drug-treated offspring. Growth deficits were not noted at 5, 10, 15 or 20 days of age. Three measures of activity were collected at 18 days of age, however, none of these measures were differentially affected as a function of prenatal treatment. At 85 days of age, offspring were tested in a two-way shuttle avoidance paradigm. Although the number of avoidances was not significantly affected by prenatal treatment, offspring exposed to these drugs in combination had shorter response latencies than controls with increased training and made more intertrial crossing responses. Additional offspring were tested for seizure susceptibility at 100 days of age. None of the parameters of seizure activity were significantly affected by prenatal drug treatment. Prenatal exposure to pentazocine and tripelennamine resulted in prenatal growth deficits, increased activity during the intertrial interval and decreased response latencies in a shuttle avoidance learning task, suggesting that this polydrug combination may be associated with some long-term behavioral teratogenic risks.

产前暴露于pentazocine和tripelennamine组合对行为和发育的影响。
在妊娠第7-20天,用四种剂量组合中的一种给药,分别是0:0 (mg/kg戊唑嗪:三烯胺)、20:10、40:0和40:20。另外一组在怀孕期间可以免费获得实验室食物和水。出生时,所有接受药物治疗的后代体重明显减轻。在5、10、15或20日龄时没有发现生长缺陷。在18日龄时收集了三个活动测量值,然而,这些测量值都没有作为产前治疗的功能而受到差异影响。在85日龄时,在双向穿梭回避范式中对后代进行测试。虽然回避的数量不受产前治疗的显著影响,但暴露于这些药物组合的后代与对照组相比,随着训练的增加,反应潜伏期更短,并且产生了更多的试验间交叉反应。另外的子代在100日龄时进行癫痫易感性测试。产前药物治疗对癫痫发作的各项参数均无显著影响。产前暴露于pentazocine和tripelennamine导致产前生长缺陷,在试验间隔期间活动增加,在穿梭回避学习任务中反应潜伏期降低,表明这种多药组合可能与一些长期的行为致畸风险有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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