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大鼠体内质粒DNA的药代动力学

Pharmacokinetics of plasmid DNA in the rat.

作者信息

Houk B E, Martin R, Hochhaus G, Hughes J A

机构信息

Department of Pharmaceutics, College of Pharmacy, University of Florida, Gainesville 32610, USA.

出版信息

Pharm Res. 2001 Jan;18(1):67-74. doi: 10.1023/a:1011078711008.

Abstract

PURPOSE

The pharmacokinetics of plasmid DNA after IV bolus administration in the rat by following supercoiled (SC), open circular (OC), and linear (L) pDNA forms of the plasmid.

METHODS

SC, OC, and L pDNA were injected at 2,500, 500, 333, and 250 microg doses. The concentrations in the bloodstream of OC and L pDNA were monitored.

RESULTS

SC pDNA was detectable in the bloodstream only after a 2,500 microg dose, and had a clearance of 390(+/-50) ml/min and Vd of 81(+/-8) ml. The pharmacokinetics of OC pDNA exhibited non-linear characteristics with clearance ranging from 8.3(+/-0.8) to 1.3(+/-0.2) ml/min and a Vd of 39(+/-19) ml. L pDNA was cleared at 7.6(+/-2.3) ml/min and had a Vd of 37(+/-17) ml. AUC analysis revealed that 60(+/-10) % of the SC was converted to the OC form, and nearly complete conversion of the OC pDNA to L pDNA. Clearance of SC pDNA was decreased after liposome complexation to 87(+/-30) ml/min. However the clearance of OC and L pDNA was increased relative to naked pDNA at an equivalent dose to 37(+/-9) ml/min and 95(+/-37) ml/min respectively.

CONCLUSIONS

SC pDNA is rapidly metabolized and cleared from the circulation. OC pDNA displays non-linear pharmacokinetics. Linear pDNA exhibits first order kinetics. Liposome complexation protects the SC topoform, but the complexes are more rapidly cleared than the naked pDNA.

摘要

目的

通过追踪质粒的超螺旋(SC)、开环(OC)和线性(L)pDNA形式,研究大鼠静脉推注给药后质粒DNA的药代动力学。

方法

以2500、500、333和250微克剂量注射SC、OC和L pDNA。监测OC和L pDNA在血液中的浓度。

结果

仅在给予2500微克剂量后,血液中可检测到SC pDNA,清除率为390(±50)毫升/分钟,分布容积为81(±8)毫升。OC pDNA的药代动力学表现出非线性特征,清除率范围为8.3(±0.8)至1.3(±0.2)毫升/分钟,分布容积为39(±19)毫升。L pDNA的清除率为7.6(±2.3)毫升/分钟,分布容积为37(±17)毫升。AUC分析显示,60(±10)%的SC转化为OC形式,OC pDNA几乎完全转化为L pDNA。脂质体复合后,SC pDNA的清除率降至87(±30)毫升/分钟。然而,在等效剂量下,OC和L pDNA相对于裸pDNA的清除率分别增加至37(±9)毫升/分钟和95(±37)毫升/分钟。

结论

SC pDNA在循环中迅速代谢和清除。OC pDNA表现出非线性药代动力学。线性pDNA表现出一级动力学。脂质体复合可保护SC拓扑形式,但复合物的清除速度比裸pDNA更快。

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