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与单次大剂量注射相比,多次小剂量注射八肽胆囊收缩素在诱导味觉厌恶条件反射方面更有效。

Multiple, small doses of cholecystokinin octapeptide are more efficacious at inducing taste aversion conditioning than single, large doses.

作者信息

Ervin G N, Mosher J T, Birkemo L S, Johnson M F

机构信息

Glaxo Research Institute, Research Triangle Park, NC 27709, USA.

出版信息

Peptides. 1995;16(3):539-45. doi: 10.1016/0196-9781(95)00001-z.

Abstract

Using a one-bottle taste aversion conditioning paradigm, sulfated cholecystokinin(26-33) (CCK-8) has again been shown to induce taste aversion conditioning in rats. Even though the effective doses of CCK-8 are relatively high, they do not induce as strong an aversion as has been demonstrated with LiCl. This pharmacodynamic profile of CCK-8 (i.e., relatively moderate, but not strong, taste aversion induction) may result, in part, from its unusual pharmacokinetic profile. CCK-8 seems to have a plasma half-life of just several minutes, whereas LiCl has a plasma half-life of 6 h in rats. In the present study, CCK-8, CCK-4, or LiCl was administered either as single, large doses immediately following consumption of 0.2% sodium saccharin (SACC), or as 10 half-hourly injections of one-tenth the large dose. Presumably, multiple small doses extended the time CCK-8 and CCK-4 were acting in the body, even though the peak plasma concentrations were quantitatively lower than after the large, single doses. Ten injections of CCK-8 of 10 or 100 nmol/kg (11.4 or 114.3 micrograms/kg) induced significantly stronger taste aversions than single injections of the same total dose of 100 or 1000 nmol/kg (114.3 or 1143.3 micrograms/kg), whereas multiple injections of LiCl of 70.8 mumol/kg (3.0 mg/kg x 10) did not induce stronger taste aversions than single injections of 708 mumol/kg (30.0 mg/kg). Neither single nor multiple injections of CCK-4 of 1000 nmol/kg (596.7 micrograms/kg) x 1, or 100 or 1000 nmol/kg (59.7 or 596.7 micrograms/kg) x 10 induced any sign of taste aversion conditioning.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

采用单瓶味觉厌恶条件反射范式,硫酸化胆囊收缩素(26 - 33)(CCK - 8)再次被证明能在大鼠中诱导味觉厌恶条件反射。尽管CCK - 8的有效剂量相对较高,但它们诱导的厌恶程度不如LiCl所表现出的那么强烈。CCK - 8的这种药效学特征(即相对中等但不强烈的味觉厌恶诱导)可能部分源于其不寻常的药代动力学特征。CCK - 8的血浆半衰期似乎只有几分钟,而LiCl在大鼠中的血浆半衰期为6小时。在本研究中,CCK - 8、CCK - 4或LiCl在大鼠饮用0.2%糖精钠(SACC)后,要么立即给予单次大剂量,要么给予10次大剂量十分之一的半小时一次的注射。据推测,多次小剂量延长了CCK - 8和CCK - 4在体内的作用时间,尽管血浆峰值浓度在数量上低于单次大剂量给药后的浓度。10次注射10或100 nmol/kg(11.4或114.3微克/千克)的CCK - 8比单次注射相同总剂量100或1000 nmol/kg(114.3或1143.3微克/千克)诱导出明显更强的味觉厌恶,而多次注射70.8 μmol/kg(3.0毫克/千克×10)的LiCl并不比单次注射708 μmol/kg(30.0毫克/千克)诱导出更强的味觉厌恶。单次或多次注射1000 nmol/kg(596.7微克/千克)×1或100或1000 nmol/kg(59.7或596.7微克/千克)×10的CCK - 4均未诱导出任何味觉厌恶条件反射的迹象。(摘要截短于250字)

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