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在短暂麻醉的犬中通过气管内滴注和气溶胶吸入进行地屈瑞林的肺部给药。

Pulmonary delivery of detirelix by intratracheal instillation and aerosol inhalation in the briefly anesthetized dog.

作者信息

Bennett D B, Tyson E, Nerenberg C A, Mah S, de Groot J S, Teitelbaum Z

机构信息

Center for Drug Delivery Research, Syntex Research, Palo Alto, CA 94304.

出版信息

Pharm Res. 1994 Jul;11(7):1048-55. doi: 10.1023/a:1018999707476.

Abstract

Pulmonary delivery of the decapeptide detirelix was studied in briefly anesthetized dogs and the pharmacokinetics were examined following intravenous administration, intratracheal instillation, and aerosol inhalation. Detirelix administrations to the lung gave plasma profiles that were extended over two days, and that differed markedly from those of similarly sized peptides. Absorption from the lung after instillation was slow (Tmax = 6.5 +/- 3.6 h) with a relative bioavailability of 29 +/- 10%. Administration of detirelix-containing aerosols resulted in similar plasma profiles as for administration by instillation. Compartmental and non-compartmental methods of pharmacokinetic analysis indicated no faster absorption from aerosols than from instilled solutions; an absorption rate limiting process may be an explanation. Plasma profiles were not affected by the use of detirelix liquid crystal favoring formulations or destabilizing formulations, and suggested that in situ liquid crystal formation was not an explanation for the slow absorption. No significant changes in pharmacokinetics or systemic uptake were observed during the five-month period of repeated pulmonary administrations. Histopathologic examination revealed the lungs to be essentially normal.

摘要

在短暂麻醉的犬中研究了十肽地屈瑞林的肺部给药,并在静脉注射、气管内滴注和气溶胶吸入后检测了其药代动力学。向肺部给予地屈瑞林后,血浆浓度曲线持续两天,且与大小相似的肽类有显著差异。滴注后肺部吸收缓慢(达峰时间Tmax = 6.5 +/- 3.6小时),相对生物利用度为29 +/- 10%。给予含地屈瑞林的气雾剂后,血浆浓度曲线与滴注给药相似。药代动力学分析的房室和非房室方法表明,气雾剂的吸收并不比滴注溶液更快;吸收速率限制过程可能是一个解释。血浆浓度曲线不受使用有利于地屈瑞林形成液晶的制剂或使制剂不稳定的制剂的影响,这表明原位液晶形成并非吸收缓慢的原因。在五个月的重复肺部给药期间,未观察到药代动力学或全身摄取有显著变化。组织病理学检查显示肺部基本正常。

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