首页> 外文期刊>European Journal of Pharmacology: An International Journal >The anti-cancer drug-induced pica in rats is related to their clinical emetogenic potential.
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The anti-cancer drug-induced pica in rats is related to their clinical emetogenic potential.

机译:大鼠的抗癌药物诱发的异食癖与他们的临床生胎潜力有关。

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Cancer chemotherapy is frequently accompanied by severe emesis. The anti-cancer drugs are classified according to their clinical emetogenic potential. We have already found that kaolin ingestion behavior "pica" is analogous to emesis in rats. The aim of this study was to examine the effects of the clinical emetogenic potential of anti-cancer drugs on the induction of the pica in rats. Rats were housed in individual cages with free access to food and kaolin pellets and the daily food and kaolin intakes were measured for 3 days after the intraperitoneal administration of anti-cancer drugs (cisplatin, cyclophosphamide, actinomycin D, 5-fluorouracil and vincristine). The drugs with high potential for inducing emesis, such as cisplatin and cyclophosphamide, induced pica in all animals on the day of administration and the behavior lasted during the observation period. The drugs with moderate emetogenic potential, i.e. actinomycin D and 5-fluorouracil, also induced pica on the first and second day after the drug administration but the kaolin intake was less than that of the drugs with high potential. Vincristine, a drug with low emetogenic potential, slightly increased the kaolin intake in rats on the only first day of the administration. Cyclophosphamide, actinomycin D and vincristine induced anorexia and decreased their body weight during the observation period. These results suggested that the both amounts of kaolin intake and duration of behavior in the anti-cancer drug-induced pica are related to the clinical emetogenic potential of the drugs and the incidence of the anorexia is not related to their emetogenic potential.
机译:癌症化学疗法常伴有严重呕吐。抗癌药物根据其临床生胎潜力进行分类。我们已经发现高岭土的摄取行为“异食癖”类似于大鼠的呕吐。这项研究的目的是检查抗癌药物的临床促生潜力对大鼠皮卡诱发的影响。将大鼠关在单独的笼子中,自由进食食物和高岭土颗粒,并在腹膜内给予抗癌药物(顺铂,环磷酰胺,放线菌素D,5-氟尿嘧啶和长春新碱)后3天测量每日的食物和高岭土摄入量。在给药当天,顺铂和环磷酰胺等具有诱导呕吐潜能的药物会在所有动物体内诱发异食癖,并且这种行为在观察期内持续存在。具有中等致癌潜力的药物,即放线菌素D和5-氟尿嘧啶,在给药后的第一天和第二天也诱发了异食癖,但高岭土的摄入量少于高潜力的药物。长春新碱,一种具有低促生药潜力的药物,在给药的第一天,便稍微增加了大鼠的高岭土摄入量。在观察期间,环磷酰胺,放线菌素D和长春新碱可引起厌食症并减轻其体重。这些结果表明,在抗癌药物诱导的异食癖中高岭土的摄入量和行为持续时间均与该药物的临床促生潜力有关,而厌食症的发生与其促生潜力无关。

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