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Neurochem Int. 2019 Oct;129:104471. doi: 10.1016/j.neuint.2019.104471. Epub 2019 May 20.
Phosphodiesterase (PDE) inhibition has been broadly investigated as a target for a wide variety of indications including central nervous system (CNS) disorders. Cyclic nucleotide (cNT) changes within associated tissues may serve as a biomarker of PDE inhibition. We recently developed robust sample harvesting and bioanalytical methods to quantify cNT levels in rodent brain and cerebrospinal fluid (CSF). Herein, we report on the application of those methods to study rodent species-specific and rodent brain region-specific cNT changes following individual or concomitant PDE inhibitor administration. Male Sprague Dawley (Crl:CD [SD]) rats were dosed subcutaneously (sc) with a PDE1B inhibitor (DNS-0056), a PDE2A inhibitor (PF-05180999), a PDE9A inhibitor (PF-4447943), and a PDE10A inhibitor (MP10), each at a single dose of 10 or 30 mg/kg, or concomitantly with all 4 inhibitors at 10 mg/kg each. Male Carworth Farms (Crl:CF1 [CF-1]) mice were dosed intraperitoneally (ip) with the four individual inhibitors at a single dose of 10 mg/kg or concomitantly with all 4 inhibitors at 10 mg/kg each. The doses studied are generally adequate for affecting measurable cNT levels in the tissues of interest and were thereby chosen for this investigation. Measured 3',5'-cyclic adenosine monophosphate (cAMP) changes were generally statistically insignificant in the brain, striatum and CSF after administration of the aforementioned PDE inhibitors. However, the levels of 3',5'-cyclic guanosine monophosphate (cGMP) increased in both rat and mouse striatum (2.2-, 2.1- and 1.7-fold and 6.4-, 2.8- and 1.7-fold, respectively) after PDE2A, 9A, and 10A inhibitor dosing. In all cases, the cNT changes followed the same trend in the brain, striatum and CSF after PDE inhibitor dosing and dose response was observed in rats. Concomitant treatment with PDE1B, PDE2A, PDE9A and PDE10A inhibitors resulted in a 4.4- and 36.7-fold increase of cGMP in rat and mouse striatum. The drug exposures after concomitant treatment were also higher than in the individual inhibitor-treated animals. cGMP enhancement observed could be due to synergistic effects, though an additive effect of the combined inhibitor concentrations may also contribute.
磷酸二酯酶(PDE)抑制作用已被广泛研究,作为治疗多种适应症的靶点,包括中枢神经系统(CNS)疾病。相关组织中环核苷酸(cNT)的变化可作为 PDE 抑制作用的生物标志物。我们最近开发了强大的样本采集和生物分析方法,以定量检测啮齿动物大脑和脑脊液(CSF)中的 cNT 水平。本文报告了这些方法在研究单种或同时给予 PDE 抑制剂后,啮齿动物物种特异性和脑区特异性 cNT 变化中的应用。雄性 Sprague Dawley(Crl:CD [SD])大鼠经皮下(sc)给予 PDE1B 抑制剂(DNS-0056)、PDE2A 抑制剂(PF-05180999)、PDE9A 抑制剂(PF-4447943)和 PDE10A 抑制剂(MP10),每种药物的剂量为 10 或 30mg/kg,或同时给予 4 种抑制剂,每种药物的剂量均为 10mg/kg。雄性 Carworth Farms(Crl:CF1 [CF-1])小鼠经腹腔(ip)给予 4 种单种抑制剂,剂量为 10mg/kg,或同时给予 4 种抑制剂,剂量均为 10mg/kg。研究的剂量通常足以影响感兴趣的组织中可测量的 cNT 水平,因此选择这些剂量进行这项研究。上述 PDE 抑制剂给药后,大脑、纹状体和 CSF 中的 3',5'-环腺苷酸(cAMP)变化通常在统计学上无显著意义。然而,在大鼠和小鼠纹状体中,3',5'-环鸟苷酸(cGMP)水平分别增加了 2.2、2.1 和 1.7 倍和 6.4、2.8 和 1.7 倍,分别给予 PDE2A、9A 和 10A 抑制剂后。在所有情况下,PDE 抑制剂给药后,cNT 变化在大脑、纹状体和 CSF 中均呈现相同趋势,且在大鼠中观察到剂量反应。同时给予 PDE1B、PDE2A、PDE9A 和 PDE10A 抑制剂可使大鼠和小鼠纹状体中的 cGMP 分别增加 4.4 和 36.7 倍。同时治疗后的药物暴露水平也高于单独给予抑制剂的动物。观察到的 cGMP 增强可能是由于协同作用所致,尽管联合抑制剂浓度的相加作用也可能有贡献。
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