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Plasma and Brain Pharmacokinetics of Previously Unexplored Lithium Salts

机译:以前未开发的锂盐的血浆和脑药代动力学

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摘要

Despite its narrow therapeutic window, lithium is still regarded as the gold standard comparator and benchmark treatment for mania. Recent attempts to find new drugs with similar therapeutic activities have yielded new chemical entities. However, these potential new drugs have yet to match the many bioactivities attributable to lithium's efficacy for the treatment of neuropsychiatric diseases. Consequently, an intense effort for re-engineering lithium therapeutics using crystal engineering is currently underway. We sought to improve the likelihood of success of these endeavors by evaluating the pharmacokinetics of previously unexplored lithium salts with organic anions (lithium salicylate and lithium lactate). We report that these lithium salts exhibit profoundly different pharmacokinetics compared to the more common FDA approved salt, lithium carbonate, in rats. Remarkably, lithium salicylate produced elevated plasma and brain levels of lithium beyond 48 hours post-dose without the sharp peak that contributes to the toxicity problems of current lithium therapeutics. These findings could be important for the development of the next generation of lithium therapeutics.
机译:尽管其治疗范围狭窄,但锂仍被认为是躁狂症的金标准对照和基准疗法。最近寻找具有类似治疗活性的新药物的尝试产生了新的化学实体。但是,这些潜在的新药尚未与锂具有的治疗神经精神疾病的功效相匹配的许多生物活性。因此,目前正在努力进行使用晶体工程技术对锂治疗剂进行再工程的工作。我们试图通过评估以前未开发的锂盐与有机阴离子(水杨酸锂和乳酸锂)的药代动力学来提高这些努力成功的可能性。我们报告说,与更常见的FDA批准的盐碳酸锂相比,这些锂盐在大鼠中表现出截然不同的药代动力学。值得注意的是,水杨酸锂在给药后48小时后血浆和大脑中的锂水平升高,而没有出现尖峰,这导致了目前锂治疗剂的毒性问题。这些发现对于下一代锂治疗剂的开发可能是重要的。

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