Nitric Oxide Donor Sodium Nitroprusside Reduces Racemic Ketamine─But Not Esketamine-Induced Pain Relief

IF 4.9 Q1 CHEMISTRY, MEDICINAL
Albert Dahan*, Simone Jansen, Rutger van der Schrier, Elise Sarton, David Dadiomov, Monique van Velzen, Erik Olofsen and Marieke Niesters, 
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引用次数: 0

Abstract

The anesthetic, analgesic and antidepressant drug ketamine produces dissociation with symptoms of psychosis and anxiety, an effect attributed to neuronal nitric oxide depletion following N-methyl-d-aspartate blockade. There is evidence that dissociation induced by racemic ketamine, containing both ketamine enantiomers (S- and R-ketamine) but not esketamine (the S-isomer) is inhibited by nitric oxide (NO) donor sodium nitroprusside (SNP). We tested whether a similar intervention would reduce racemic and esketamine-induced analgesia in a randomized double-blind placebo-controlled trial. Seventeen healthy volunteers were treated with 0.5 μg.kg–1.min–1 SNP or placebo during a 3-h infusion of escalating doses of racemic ketamine (total dose 140 mg) or esketamine (70 mg). Pain pressure threshold (PPT) and arterial blood samples for measurement of S- and R-ketamine and their metabolites, S- and R-norketamine, were obtained. The data were analyzed with a population pharmacokinetic-pharmacodynamic model that incorporated the measured S- and R- ketamine and S- and R-norketamine isomers as input and PPT as output to the model. The potency of the 2 formulations in increasing PPT from baseline by 100% was 0.47 ± 0.12 (median ± standard error of the estimate) nmol/mL for esketamine and 0.62 ± 0.19 nmol/mL for racemic ketamine, reflecting the 52 ± 27% lower analgesic potency of R-ketamine versus S-ketamine. Modeling showed that SNP had no effect on S-ketamine potency but abolished the R-ketamine analgesic effect. Similar observations were made for S- and R-norketamine. Since SNP had no effect on S-ketamine analgesia, we conclude that SNP interacts on R-ketamine nociceptive pathways, possibly similar to its effects on R-ketamine activated dissociation pathways.

Abstract Image

Abstract Image

一氧化氮供体硝普钠能减轻消旋氯胺酮引起的疼痛,但不能减轻艾司他敏引起的疼痛
麻醉、镇痛和抗抑郁药物氯胺酮会产生精神错乱和焦虑症状的解离现象,这种效应归因于 N-甲基-d-天冬氨酸受体阻断后神经元一氧化氮耗竭。有证据表明,一氧化氮(NO)供体硝普钠(SNP)可抑制外消旋氯胺酮(包含氯胺酮对映体(S-和R-氯胺酮))引起的分离,但不能抑制埃斯氯胺酮(S-异构体)。我们在一项随机双盲安慰剂对照试验中测试了类似的干预措施是否会减少外消旋酮和埃斯卡明引起的镇痛。在输注 3 小时递增剂量的外消旋氯胺酮(总剂量 140 毫克)或埃斯氯胺酮(70 毫克)期间,17 名健康志愿者接受了 0.5 μg.kg-1.min-1 SNP 或安慰剂治疗。研究人员采集了疼痛压力阈值(PPT)和动脉血样本,用于测量 S-和 R-氯胺酮及其代谢物 S-和 R-诺卡因。使用群体药代动力学-药效学模型对数据进行了分析,该模型将所测得的 S- 和 R- 氯胺酮以及 S- 和 R-诺克他敏异构体作为输入,将 PPT 作为输出。这两种制剂在使PPT从基线增加100%方面的效力是:埃斯氯胺酮为0.47 ± 0.12(中位数±估计值标准误差)毫摩尔/毫升,外消旋氯胺酮为0.62 ± 0.19毫摩尔/毫升,反映出R-氯胺酮的镇痛效力比S-氯胺酮低52 ± 27%。建模显示,SNP 对 S-Ketamine 的效力没有影响,但会消除 R-Ketamine 的镇痛效果。对 S-和 R-诺卡因也有类似的观察结果。由于 SNP 对 S-Ketamine 镇痛没有影响,我们得出结论:SNP 与 R-Ketamine 痛觉通路相互作用,可能与其对 R-Ketamine 激活解离通路的影响类似。
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来源期刊
ACS Pharmacology and Translational Science
ACS Pharmacology and Translational Science Medicine-Pharmacology (medical)
CiteScore
10.00
自引率
3.30%
发文量
133
期刊介绍: ACS Pharmacology & Translational Science publishes high quality, innovative, and impactful research across the broad spectrum of biological sciences, covering basic and molecular sciences through to translational preclinical studies. Clinical studies that address novel mechanisms of action, and methodological papers that provide innovation, and advance translation, will also be considered. We give priority to studies that fully integrate basic pharmacological and/or biochemical findings into physiological processes that have translational potential in a broad range of biomedical disciplines. Therefore, studies that employ a complementary blend of in vitro and in vivo systems are of particular interest to the journal. Nonetheless, all innovative and impactful research that has an articulated translational relevance will be considered. ACS Pharmacology & Translational Science does not publish research on biological extracts that have unknown concentration or unknown chemical composition. Authors are encouraged to use the pre-submission inquiry mechanism to ensure relevance and appropriateness of research.
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