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不同的奥氮平药代动力学解释了为什么它在躁狂症的小鼠模型中比碳酸锂更有效、更有效、毒性更小。

Different pharmacokinetics of lithium orotate inform why it is more potent, effective, and less toxic than lithium carbonate in a mouse model of mania.

机构信息

Department of Pharmacology, College of Medicine, University of Saskatchewan, Saskatoon, Saskatchewan, S7N 5E5, Canada.

出版信息

J Psychiatr Res. 2023 Aug;164:192-201. doi: 10.1016/j.jpsychires.2023.06.012. Epub 2023 Jun 17.

DOI:10.1016/j.jpsychires.2023.06.012
PMID:37356352
Abstract

Lithium carbonate (LiCO) is a mainstay therapeutic for the prevention of mood-episode recurrences in bipolar disorder (BD). Unfortunately, its narrow therapeutic index is associated with complications that may lead to treatment non-compliance. Intriguingly, lithium orotate (LiOr) is suggested to possess unique uptake characteristics that would allow for reduced dosing and mitigation of toxicity concerns. We hypothesized that due to differences in pharmacokinetics, LiOr is more potent with reduced adverse effects. Dose responses were established for LiOr and LiCO in male and female mice using an amphetamine-induced hyperlocomotion (AIH) model; AIH captures manic elements of BD and is sensitive to a dose-dependent lithium blockade. LiCO induced a partial block of AIH at doses of 15 mg/kg in males and 20 mg/kg in females. In contrast, LiOr elicited a near complete blockade at concentrations of just 1.5 mg/kg in both sexes, indicating improved efficacy and potency. Prior application of organic anion transport inhibitors, or inhibition of orotate uptake into the pentose pathway, completely blocked the effects of LiOr on AIH while sparing LiCO effects, confirming differences in transport and compartmentalization between the two compounds. Next, the relative toxicities of LiOr and LiCO were contrasted after 14 consecutive daily administrations. LiCO, but not LiOr, elicited polydipsia in both sexes, elevated serum creatinine levels in males, and increased serum TSH expression in females. LiOr demonstrates superior efficacy, potency, and tolerability to LiCO in both male and female mice because of select transport-mediated uptake and pentose pathway incorporation.

摘要

碳酸锂 (LiCO) 是预防双相情感障碍 (BD) 情绪发作复发的主要治疗药物。不幸的是,其狭窄的治疗指数与可能导致治疗不依从的并发症有关。有趣的是,提示 1,5-戊二醛(LiOr)具有独特的摄取特性,可减少剂量并减轻毒性问题。我们假设由于药代动力学的差异,LiOr 的效力更强,副作用更少。我们使用安非他命诱导的过度活跃 (AIH) 模型在雄性和雌性小鼠中建立了 LiOr 和 LiCO 的剂量反应;AIH 捕捉 BD 的躁狂元素,对锂依赖性阻断敏感。LiCO 在雄性中的 15mg/kg 和雌性中的 20mg/kg 剂量下诱导 AIH 的部分阻断。相比之下,LiOr 在两性中的浓度仅为 1.5mg/kg 就引起了近乎完全阻断,表明疗效和效力提高。先前应用有机阴离子转运抑制剂,或抑制 1,5-戊二醛进入戊糖途径的摄取,完全阻断 LiOr 对 AIH 的作用,而不影响 LiCO 的作用,证实了两种化合物在转运和区室化方面的差异。接下来,在连续 14 天给药后比较了 LiOr 和 LiCO 的相对毒性。LiCO 但不是 LiOr,在两性中均引起多饮,雄性血清肌酐水平升高,雌性血清 TSH 表达增加。LiOr 在雄性和雌性小鼠中表现出优于 LiCO 的疗效、效力和耐受性,因为它具有选择性的转运介导摄取和戊糖途径掺入。

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