健康志愿者吸入干粉状妥布霉素PulmoSphere制剂。
Inhalation of a dry powder tobramycin PulmoSphere formulation in healthy volunteers.
作者信息
Newhouse Michael T, Hirst Peter H, Duddu Sarma P, Walter Yulia H, Tarara Thomas E, Clark Andrew R, Weers Jeffry G
机构信息
Inhale Therapeutic Systems Inc., San Carlos, CA 94070, USA.
出版信息
Chest. 2003 Jul;124(1):360-6. doi: 10.1378/chest.124.1.360.
STUDY OBJECTIVES
To evaluate the efficiency and reproducibility of pulmonary delivery of an investigational tobramycin PulmoSphere formulation (PStob) [Inhale Therapeutic Systems; San Carlos, CA] by a passive dry powder inhaler, and to compare serum concentrations and whole-lung deposition with a commercial nebulized tobramycin product (TOBI; Chiron Corporation; Seattle, WA).
DESIGN
A five-period, open-label, nonrandomized crossover study.
PARTICIPANTS
Fourteen healthy volunteers were studied, and 12 completed the study.
INTERVENTIONS
PStob powder was manufactured using lipid-based PulmoSphere technology, producing highly dispersible porous particles. PStob was radiolabeled with (99m)Tc, and in vitro experiments confirmed it as a valid drug marker. To identify whole-lung distribution via scintigraphy, subjects inhaled contents of a single capsule (72 L/min) containing 25 mg of (99m)Tc-labeled PStob (13.5 mg of tobramycin free base) in periods 1 to 3. In period 4, subjects received (99m)Tc nebulized tobramycin, approximately 2.5 mL of 300 mg/5 mL. Deposition and blood samples were obtained. In period 5, six 25-mg doses of unlabeled PStob (81 mg of tobramycin base) were inhaled and blood samples were collected.
MEASUREMENTS AND RESULTS
Mean whole-lung deposition of PStob was 34 +/- 6% and nebulized tobramycin was 5 +/- 2%. Peak tobramycin concentration in serum (Cmax) values were 0.6 microg/mL with PStob and 0.28 microg/mL after nebulized tobramycin. Serum area under the curve was 4.4 microg x h/mL vs 2.1 micro g x h/mL for nebulized tobramycin. Median time to Cmax for PStob was comparable to nebulized tobramycin.
CONCLUSIONS
The aerosol doses of PStob (25 mg and 150 mg) were well dispersed and tolerated. Serum drug concentrations matched scintigraphy data and were roughly twice that of the comparator. Intrasubject dose variability for three equivalent periods did not exceed 18% relative SD. PStob Cmax (0.6 microg/mL) was well below the toxic threshold (2 micro g/mL).
研究目的
通过被动干粉吸入器评估研究性妥布霉素PulmoSphere制剂(PStob)[Inhale Therapeutic Systems公司;加利福尼亚州圣卡洛斯]肺部给药的效率和可重复性,并将血清浓度及全肺沉积情况与市售雾化妥布霉素产品(TOBI;Chiron公司;华盛顿州西雅图)进行比较。
设计
一项五阶段、开放标签、非随机交叉研究。
参与者
对14名健康志愿者进行研究,12人完成研究。
干预措施
PStob粉末采用基于脂质的PulmoSphere技术制造,产生高度分散的多孔颗粒。PStob用(99m)Tc进行放射性标记,体外实验证实其为有效的药物标志物。为通过闪烁扫描法确定全肺分布,受试者在第1至3阶段吸入一粒胶囊(72升/分钟)的内容物,其中含有25毫克(99m)Tc标记的PStob(13.5毫克妥布霉素游离碱)。在第4阶段,受试者接受(99m)Tc雾化妥布霉素,约2.5毫升300毫克/5毫升。采集沉积和血样。在第5阶段,吸入六剂25毫克未标记的PStob(81毫克妥布霉素碱)并采集血样。
测量与结果
PStob的平均全肺沉积率为34±6%,雾化妥布霉素为5±2%。PStob给药后血清中妥布霉素的峰值浓度(Cmax)为0.6微克/毫升,雾化妥布霉素给药后为0.28微克/毫升。血清曲线下面积,PStob为4.4微克·小时/毫升,雾化妥布霉素为2.1微克·小时/毫升。PStob达到Cmax的中位时间与雾化妥布霉素相当。
结论
PStob(25毫克和150毫克)的气雾剂剂量分散良好且耐受性良好。血清药物浓度与闪烁扫描数据相符,约为对照产品的两倍。三个等效阶段的受试者内剂量变异性相对标准差不超过18%。PStob的Cmax(0.6微克/毫升)远低于毒性阈值(2微克/毫升)。
Zotero 插件