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脂质体包裹的糖皮质激素在健康兔和抗原诱导性关节炎兔关节腔内应用后的药代动力学及治疗效果研究。

Studies of pharmacokinetics and therapeutic effects of glucocorticoids entrapped in liposomes after intraarticular application in healthy rabbits and in rabbits with antigen-induced arthritis.

作者信息

Bonanomi M H, Velvart M, Stimpel M, Roos K M, Fehr K, Weder H G

机构信息

Abteilung für Physikalische Pharmazie und Biopharmazie, ETH-Zentrum, Zürich, Switzerland.

出版信息

Rheumatol Int. 1987;7(5):203-12. doi: 10.1007/BF00541378.

Abstract

Dexamethasone palmitate (DMP) entrapped in liposomes of defined sizes was administered intraarticularly in healthy rabbits and in rabbits with antigen-induced arthritis. The pharmacokinetics and therapeutic effect of liposomal DMP were measured and compared with corresponding experiments using microcrystalline triamcinolone acetonide (TAC). The small DMP liposomes (diameter 160 nm) showed a greater decrease in joint circumference than the 3-times-higher dose of microcrystalline TAC. Moreover, about 98% of administered TAC had already disappeared from the joint 6 h after injection, whereas about 36% of liposomal DMP was still measured in synovial fluid and synovium at the same time. Increasing the vesicle diameter from 160 to 750 nm (large liposomes) improved the retention of DMP by a factor of 2.6 within 48 h after injection in healthy rabbits. In addition, none of the liposomal glucocorticoid preparations ever suppressed the endogenous plasma cortisol level, which is in contrast to the suppression measured after administration of the microcrystalline preparation.

摘要

将包裹在特定大小脂质体中的地塞米松棕榈酸酯(DMP)关节内注射到健康兔和抗原诱导性关节炎兔体内。测定脂质体DMP的药代动力学和治疗效果,并与使用微晶曲安奈德(TAC)的相应实验进行比较。小的DMP脂质体(直径160nm)比3倍高剂量的微晶TAC使关节周长的减小幅度更大。此外,注射后6小时,约98%的给药TAC已从关节中消失,而此时在滑液和滑膜中仍可检测到约36%的脂质体DMP。在健康兔中,将囊泡直径从160nm增加到750nm(大脂质体)可使DMP在注射后48小时内的保留率提高2.6倍。此外,脂质体糖皮质激素制剂均未抑制内源性血浆皮质醇水平,这与微晶制剂给药后测得的抑制作用相反。

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