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Radiographic dose‐dependency study of loperamide effects on gastrointestinal motor function in the rat. Temporal relationship with nausea‐like behavior

机译:罗伯拉胺对大鼠胃肠运动功能的碱基剂量依赖性研究。 与恶心的行为的颞关系

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Abstract Background Loperamide is a potent mu opioid receptor agonist available over the counter to treat diarrhea. Although at therapeutic doses loperamide is devoid of central effects, it may exert them if used at high doses or combined with drugs that increase its systemic and/or central bioavailability. Recently, public health and scientific interest on loperamide has increased due to a growing trend of misuse and abuse, and consequent reports on its toxicity. Our aim was to evaluate in the rat the effects of increasing loperamide doses, with increasing likelihood to induce central effects, on gastrointestinal motor function (including gastric dysmotility and nausea‐like behavior). Methods Male Wistar rats received an intraperitoneal injection of vehicle or loperamide (0.1, 1, or 10?mg?kg ?1 ). Three sets of experiments were performed to evaluate: (a) central effects (somatic nociceptive thresholds, immobility time, core temperature, spontaneous locomotor activity); (b) general gastrointestinal motility (serial X‐rays were taken 0‐8?hours after intragastric barium administration and analyzed semiquantitatively, morphometrically, and densitometrically); and (c) bedding intake (a rodent indirect marker of nausea). Animals from sets 1 and 3 were used to evaluate gastric dysmotility ex vivo at 2 and 4?hours after administration, respectively. Key Results Loperamide significantly induced antinociception, hypothermia, and hypolocomotion (but not catalepsy) at high doses and dose‐dependently reduced gastrointestinal motor function, with the intestine exhibiting higher sensitivity than the stomach. Whereas bedding intake occurred early and transiently, gastric dysmotility was much more persistent. Conclusions and inferences Our results suggest that loperamide‐induced nausea and gastric dysmotility might be temporally dissociated.
机译:摘要背景Loperamide是一种有效的亩阿片受体激动剂,可在柜台上提供治疗腹泻。虽然在治疗剂量的洛哌胺缺乏核心效应,但如果用高剂量使用或与增加其全身和/或中央生物利用度的药物合并,它可能会施加它们。最近,由于滥用和滥用的趋势日益增长,因此,洛哌米德的公共卫生和科学兴趣增加,结果是毒性的报告。我们的目的是评估大鼠增加洛哌胺剂量的影响,随着胃肠运动功能(包括胃缺陷和恶心的行为)诱导中枢效应的可能性增加。方法雄性Wistar大鼠接受腹膜内注射载体或洛哌米胺(0.1,1,或10×mg≤kg≤1)。进行三套实验以评估:(a)中枢效应(体细胞伤害阈值,不可用时间,核心温度,自发运动活性); (b)一般胃肠运动(胃肠钡施用后的串行X射线均为0-8小时,半定量地分析,平衡,密度分析); (c)床上用品摄入(恶心的啮齿动物间接标记)。来自组1和3的动物分别用于在施用后2和4小时评估胃缺陷率外体内。关键结果在高剂量和剂量依赖性降低的胃肠运动功能下,关键率酸少胺显着诱导抗闭合剂,低温和低温和低压致症(但不是催化),并且肠道胃肠比胃更高的敏感性。虽然床上用品摄入早期和瞬时发生,胃功能性更加持久。结论和推论我们的结果表明,洛丙胺诱导的恶心和胃功能困难可能在时间上解离。

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