阿瑞匹坦对人脑中神经激肽1受体占有率的正电子发射断层扫描研究。
Human positron emission tomography studies of brain neurokinin 1 receptor occupancy by aprepitant.
作者信息
Bergström Mats, Hargreaves Richard J, Burns H Donald, Goldberg Michael R, Sciberras David, Reines Scott A, Petty Kevin J, Ogren Mattias, Antoni Gunnar, Långström Bengt, Eskola Olli, Scheinin Mika, Solin Olof, Majumdar Anup K, Constanzer Marvin L, Battisti Wendy P, Bradstreet Thomas E, Gargano Cynthia, Hietala Jarmo
机构信息
Uppsala Positron Emission Tomography Centre, Uppsala, Sweden.
出版信息
Biol Psychiatry. 2004 May 15;55(10):1007-12. doi: 10.1016/j.biopsych.2004.02.007.
BACKGROUND
Aprepitant is a highly selective substance P (neurokinin 1 [NK(1)] receptor) antagonist that significantly improves the pharmacotherapy of acute and delayed highly emetogenic chemotherapy-induced nausea and vomiting, probably through an action in the brain stem region of the central nervous system. Here, we report the use of positron emission tomography imaging with the NK(1) receptor binding-selective tracer [(18)F]SPA-RQC to determine the levels of central NK(1) receptor occupancy achieved by therapeutically relevant doses of aprepitant in healthy humans.
METHODS
Two single-blind, randomized, placebo-controlled studies in healthy subjects were performed. The first study evaluated the plasma concentration-occupancy relationships for aprepitant dosed orally at 10, 30, 100, or 300 mg, or placebo (n = 12). The second study similarly evaluated oral aprepitant 30 mg and placebo (n = 4). In each study, dosing was once daily for 14 consecutive days. Data from both studies were combined for analyses. The ratio of striatal/cerebellar [(18)F]SPA-RQ (high receptor density region/reference region lacking receptors) was used to calculate trough receptor occupancy 24 hours after the last dose of aprepitant.
RESULTS
Brain NK(1) receptor occupancy increased after oral aprepitant dosing in both a plasma concentration-related (r =.97; 95% confidence interval [CI] =.94-1.00, p <.001) and a dose-related (r =.94; 95% CI =.86-1.00, p <.001) fashion. High (> or =90%) receptor occupancy was achieved at doses of 100 mg/day or greater. The plasma concentrations of aprepitant that achieved 50% and 90% occupancy were estimated as approximately 10 ng/mL and approximately 100 ng/mL, respectively.
CONCLUSIONS
Positron emission tomography imaging with [(18)F]SPA-RQ allows brain NK(1) receptor occupancy by aprepitant to be predicted from plasma drug concentrations and can be used to guide dose selection for clinical trials of NK(1) receptor antagonists in central therapeutic indications.
背景
阿瑞匹坦是一种高度选择性的P物质(神经激肽1 [NK(1)]受体)拮抗剂,可能通过作用于中枢神经系统的脑干区域,显著改善急性和迟发性高致吐性化疗引起的恶心和呕吐的药物治疗。在此,我们报告使用正电子发射断层扫描成像以及NK(1)受体结合选择性示踪剂[(18)F]SPA - RQC来确定治疗相关剂量的阿瑞匹坦在健康人体内所达到的中枢NK(1)受体占有率水平。
方法
在健康受试者中进行了两项单盲、随机、安慰剂对照研究。第一项研究评估了口服10、30、100或300 mg阿瑞匹坦或安慰剂(n = 12)时的血浆浓度 - 占有率关系。第二项研究同样评估了口服30 mg阿瑞匹坦和安慰剂(n = 4)。在每项研究中,连续14天每日给药一次。两项研究的数据合并进行分析。纹状体/小脑[(18)F]SPA - RQ(高受体密度区域/缺乏受体的参考区域)的比值用于计算最后一剂阿瑞匹坦后24小时的谷值受体占有率。
结果
口服阿瑞匹坦给药后,脑NK(1)受体占有率呈血浆浓度相关(r =.97;95%置信区间[CI] =.94 - 1.00,p <.001)和剂量相关(r =.94;95% CI =.86 - 1.00,p <.001)的方式增加。在剂量为100 mg/天或更高时达到高(≥90%)受体占有率。达到50%和90%占有率时阿瑞匹坦的血浆浓度估计分别约为10 ng/mL和约100 ng/mL。
结论
使用[(18)F]SPA - RQ的正电子发射断层扫描成像可根据血浆药物浓度预测阿瑞匹坦对脑NK(1)受体的占有率,并可用于指导NK(1)受体拮抗剂在中枢治疗适应症临床试验中的剂量选择。
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