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用于神经药理学和行为学研究的给幼年大鼠服用地昔帕明的合适给药方案。

Appropriate dosing regimens for treating juvenile rats with desipramine for neuropharmacological and behavioral studies.

作者信息

Kozisek Megan E, Deupree Jean D, Burke William J, Bylund David B

机构信息

Department of Pharmacology and Experimental Neuroscience, 985800 Nebraska Medical Center, University of Nebraska Medical Center, Omaha, NE 68198-5800, USA.

出版信息

J Neurosci Methods. 2007 Jun 15;163(1):83-91. doi: 10.1016/j.jneumeth.2007.02.015. Epub 2007 Feb 22.

Abstract

The tricyclic antidepressants, including desipramine (DMI), are no better than placebo in treating childhood and adolescent depression, but are effective in adult depression. Animal studies comparing the effects of DMI in juveniles and adults are complicated by age-related variations in elimination rates. Thus, different dosing regiments are needed to achieve similar brain drug levels in juvenile and adult rats. We compared the half-life of DMI as well as the brain and serum concentrations of DMI and its active metabolite desmethyldesipramine in juvenile and adult rats after various drug administration paradigms. After acute i.p. administration DMI is eliminated from the brain more slowly in postnatal day (PND) 21 and 28 rats as compared to adults. After chronic i.p. administration (for 4-5 days between PND 9 and 28), lower doses of DMI are needed with juvenile rats to obtain the same brain DMI concentrations as adults. By contrast, 2 weeks of continuous drug delivery (minipump) to PND 21-35 and adult rats result in similar brain DMI concentrations. Thus, the pharmacokinetic properties of DMI varies with the age of the animal and dosing of DMI and needs to be carefully adjusted in order to have appropriate brain levels of the drug.

摘要

包括地昔帕明(DMI)在内的三环类抗抑郁药在治疗儿童和青少年抑郁症方面并不比安慰剂更有效,但对成人抑郁症有效。比较DMI在幼年和成年动物中作用的研究因消除率的年龄相关差异而变得复杂。因此,需要不同的给药方案才能在幼年和成年大鼠中达到相似的脑内药物水平。我们比较了在不同给药模式下,幼年和成年大鼠体内DMI的半衰期以及DMI及其活性代谢产物去甲基地昔帕明在脑和血清中的浓度。急性腹腔注射后,与成年大鼠相比,出生后第21天和28天的大鼠脑内DMI消除得更慢。慢性腹腔注射(出生后第9天至28天之间连续4 - 5天)后,幼年大鼠需要较低剂量的DMI才能获得与成年大鼠相同的脑内DMI浓度。相比之下,对出生后第21 - 35天的大鼠和成年大鼠连续两周给药(微型泵)会导致相似的脑内DMI浓度。因此,DMI的药代动力学特性随动物年龄和DMI给药量而变化,为使药物在脑内达到适当水平,需要仔细调整给药量。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c4a3/1976307/91419819b744/nihms-23873-f0001.jpg

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