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特定抗体剂量和亲和力的不同组合对组织中丙咪嗪再分布的影响。

Influence of various combinations of specific antibody dose and affinity on tissue imipramine redistribution.

作者信息

Ragusi C, Boschi G, Risède P, Rips R, Harrison K, Scherrmann J M

机构信息

INSERM U26, Hôpital Fernand Widal, Paris, France.

出版信息

Br J Pharmacol. 1998 Sep;125(1):35-40. doi: 10.1038/sj.bjp.0702033.

DOI:10.1038/sj.bjp.0702033
PMID:9776341
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1565593/
Abstract
  1. This study was designed to evaluate the distribution kinetics of imipramine (Imip) in the brain and the main peripheral organs (heart, kidney, liver and lung) of rats, and to establish the relationship between the redistribution of Imip from these tissues and the immunoreactive capacity (dose and affinity) of anti-TCA IgG. 2. [3H]-Imip (1 nmol kg(-1) body weight) was injected intravenously 6 min before the i.v. injection of antibodies. At this time, the concentrations of Imip and its main metabolites in plasma were determined. The radioactivity measured corresponded to 91.7% Imip, indicating that the pharmacokinetics reflected essentially Imip. Plasma and tissue Imip contents were measured over the interval 1 to 90 min in control and in treated rats. The antibodies used were a murine monoclonal IgG1 (Ka=3.8 10(7) M(-1)) at an IgG1/Imip molar ratio of 1000 (IgG1 1000), and a sheep polyclonal IgG (TAb, Ka=1.3 10(10) M(-1)) at IgG/ Imip molar ratios of 1, 10 and 100 (TAb1, TAb10 and TAb100). 3. The anti-TCA IgG increased the plasma [3H]-Imip concentrations: the AUC1-->60 min for [3H]-Imip were 4 (IgG1 1000), 9 (TAb1), 33.9 (TAb10) and 41.4 (TAb100) times higher in the treated groups than in the controls. The opposite effect occurred in the brain, heart and lungs, with large, rapid decreases in Imip. The increase in plasma Imip and the decrease in tissue Imip depended on the immunoreactive capacity (NKa) of the antibody, where N=molar concentration of IgG binding sites and Ka=IgG affinity constant. Maximal plasma and tissue redistribution occurred when NKa=33.8 x 10(4). 4. Imip redistribution can be controlled using various doses or affinities of specific antibodies, and the resulting rapid, extensive Imip redistribution from the main target organs could be very promising for TCA detoxification.
摘要
  1. 本研究旨在评估丙咪嗪(Imip)在大鼠脑及主要外周器官(心脏、肾脏、肝脏和肺)中的分布动力学,并建立Imip从这些组织中的再分布与抗三环类抗抑郁药IgG的免疫反应能力(剂量和亲和力)之间的关系。2. 在静脉注射抗体前6分钟静脉注射[3H]-Imip(1 nmol kg(-1)体重)。此时,测定血浆中Imip及其主要代谢物的浓度。测得的放射性相当于91.7%的Imip,表明药代动力学基本上反映的是Imip。在对照组和治疗组大鼠中,在1至90分钟的时间间隔内测定血浆和组织中的Imip含量。所用抗体为鼠单克隆IgG1(Ka = 3.8×10(7) M(-1)),IgG1/Imip摩尔比为1000(IgG1 1000),以及羊多克隆IgG(TAb,Ka = 1.3×10(10) M(-1)),IgG/Imip摩尔比为1、10和100(TAb1、TAb10和TAb100)。3. 抗三环类抗抑郁药IgG增加了血浆中[3H]-Imip的浓度:治疗组中[3H]-Imip的AUC1→60分钟是对照组的4倍(IgG1 1000)、9倍(TAb1)、33.9倍(TAb10)和41.4倍(TAb100)。在脑、心脏和肺中则出现相反的效果,Imip大幅快速下降。血浆中Imip的增加和组织中Imip的减少取决于抗体的免疫反应能力(NKa),其中N为IgG结合位点的摩尔浓度,Ka为IgG亲和力常数。当NKa = 33.8×10(4)时,血浆和组织中的再分布达到最大。4. 可以使用不同剂量或亲和力的特异性抗体来控制Imip的再分布,由此导致的Imip从主要靶器官的快速、广泛再分布对于三环类抗抑郁药解毒可能非常有前景。

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