Department of Psychiatry, Washington University School of Medicine , St. Louis, MO , USA.
PeerJ. 2013 Oct 29;1:e195. doi: 10.7717/peerj.195. eCollection 2013.
Background. This study's goal was to provide dose-response data for a dopamine agonist in the baboon using standard methods (replicate measurements at each dose, across a range of doses), as a standard against which to subsequently validate a novel pharmacological MRI (phMRI) method. Dependent variables were functional MRI (fMRI) data from brain regions selected a priori, and systemic prolactin release. Necessary first steps included estimating the magnitude and time course of prolactin response to anesthesia alone and to various doses of agonist. These first steps ("time course studies") were performed with three agonists, and the results were used to select promising agonists and to guide design details for the single-dose studies needed to generate dose-response curves. Methods. We studied 6 male baboons (Papio anubis) under low-dose isoflurane anesthesia after i.m. ketamine. Time course studies charted the changes in plasma prolactin levels over time after anesthesia alone or after an intravenous (i.v.) dose of the dopamine D 1-like agonists SKF82958 and SKF38393 or the D 2-like agonist pramipexole. In the single-dose dopamine agonist studies, one dose of SKF38393 (ranging from 0.0928-9.28 mg/kg, N = 5 animals) or pramipexole (0.00928-0.2 mg/kg, N = 1) was given i.v. during a 40-min blood oxygen level dependent (BOLD) fMRI session, to determine BOLD and plasma prolactin responses to different drug concentrations. BOLD response was quantified as the area under the time-signal curve for the first 15 min after the start of the drug infusion, compared to the linearly predicted signal from the baseline data before drug. The ED50 (estimated dose that produces 50% of the maximal possible response to drug) for SKF38393 was calculated for the serum prolactin response and for phMRI responses in hypothalamus, pituitary, striatum and midbrain. Results. Prolactin rose 2.4- to 12-fold with anesthesia alone, peaking around 50-90 min after ketamine administration and gradually tapering off but still remaining higher than baseline on isoflurane 3-5 h after ketamine. Baseline prolactin level increased with age. SKF82958 0.1 mg/kg i.v. produced no noticeable change in plasma prolactin concentration. SKF38393 produced a substantial increase in prolactin release that peaked at around 20-30 min and declined to pre-drug levels in about an hour. Pramipexole quickly reduced prolactin levels below baseline, reaching a nadir 2-3 h after infusion. SKF38393 produced clear, dose-responsive BOLD signal changes, and across the four regions, ED50 was estimated at 2.6-8.1 mg/kg. Conclusions. In the baboon, the dopamine D 1 receptor agonist SKF38393 produces clear plasma prolactin and phMRI dose-response curves. Variability in age and a modest sample size limit the precision of the conclusions.
背景。本研究的目的是使用标准方法(在每个剂量下重复测量,跨越一系列剂量)为巴 比 猴 中 的 一 种 多 巴 胺 激 动 剂 提 供 剂 量 - 反 应 数 据 , 作 为 随 后 验 证 新 的 药 理 学 MRI(phMRI)方法的标准。因变量是从预先选择的大脑区域获得的功能 MRI(fMRI)数据和全身催乳素释放。必要的第一步包括估计单独麻醉和各种激动剂剂量下催乳素反应的幅度和时程。这些第一步(“时程研究”)使用了三种激动剂,结果用于选择有前途的激动剂,并指导产生剂量 - 反应曲线所需的单剂量研究的设计细节。方法。我们在 6 只雄性巴 比 猴(狒狒属)接受低剂量异氟烷麻醉后,通过肌内注射氯胺酮进行研究。时程研究记录了麻醉后或静脉(i.v.)给予多巴胺 D 1 样激动剂 SKF82958 和 SKF38393 或 D 2 样激动剂普拉克索后,血浆催乳素水平随时间的变化。在单剂量多巴胺激动剂研究中,静脉给予 SKF38393(范围为 0.0928-9.28mg/kg,N = 5 只动物)或普拉克索(0.00928-0.2mg/kg,N = 1),以确定不同药物浓度对 BOLD 和血浆催乳素的反应。BOLD 反应通过在药物输注开始后 15 分钟内测量时间信号曲线下的面积来定量,与药物前基线数据的线性预测信号进行比较。计算了 SKF38393 血清催乳素反应和下丘脑、垂体、纹状体和中脑的 phMRI 反应的 ED50(估计产生药物最大可能反应的 50%的剂量)。结果。单独麻醉可使催乳素升高 2.4-12 倍,在氯胺酮给药后约 50-90 分钟达到峰值,并且在氯胺酮 3-5 小时后仍高于基线,但逐渐减弱。基础催乳素水平随年龄增长而增加。静脉给予 0.1mg/kg SKF82958 不会明显改变血浆催乳素浓度。SKF38393 引起催乳素大量释放,在约 20-30 分钟达到峰值,并在约 1 小时内降至药物前水平。普拉克索迅速将催乳素水平降低至基线以下,在输注后 2-3 小时达到最低点。SKF38393 产生了清晰的、剂量反应性的 BOLD 信号变化,在四个区域中,ED50 估计为 2.6-8.1mg/kg。结论。在巴 比 猴中,多巴胺 D 1 受体激动剂 SKF38393 产生了清晰的血浆催乳素和 phMRI 剂量 - 反应曲线。年龄的变化和适度的样本量限制了结论的准确性。
