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前列腺素E1经不同途径给药后的大鼠体内药效学比较
引用本文:谷福根,崔福德,高永良. 前列腺素E1经不同途径给药后的大鼠体内药效学比较[J]. 药学学报, 2007, 42(7): 787-793
作者姓名:谷福根  崔福德  高永良
作者单位:1. 内蒙古医学院,附属医院,药剂部,内蒙古,呼和浩特,010059
2. 沈阳药科大学,药学院,辽宁,沈阳,110016
3. 军事医学科学院,毒物药物研究所,北京,100850
摘    要:本文研究了前列腺素E1(PGE1)分别经不同途径给药后的大鼠体内药效学,旨在寻找目前PGE1注射给药的替代途径。以PGE1降压效应作为药效学指标,以静脉注射为对照,分别测定PGE1经鼻腔、舌下、肌肉(im)、腹腔(ip)给药后的药效学参数,包括峰效应时间(Tmax),血压下降最大百分数(Emax,%),效应持续时间(Td)以及血压下降百分数-时间曲线下面积(AUC,%·min)。研究结果表明,PGE1经上述途径给药后,药效学参数Emax,Td,AUC等均随给药剂量的增加而增大,提示存在明显的剂量-效应关系。根据所测Tmax值,推断上述给药途径其吸收速率的大小顺序为:鼻腔≈im>ip>舌下;依据所测药理生物利用度(PF)值,预测药物绝对生物利用度的顺序为:鼻腔>im≈ip>舌下。上述研究结果提示,PGE1经鼻腔与舌下黏膜给药,有望替代目前的注射给药。

关 键 词:前列腺素E1  药效学  鼻腔吸收  舌下吸收
文章编号:0513-4870(2007)07-0787-07
收稿时间:2007-01-22
修稿时间:2007-01-22

Pharmacodynamic comparison of prostaglandin E1 administered by different routes to rats
GU Fu-gen,CUI Fu-de,GAO Yong-liang. Pharmacodynamic comparison of prostaglandin E1 administered by different routes to rats[J]. Acta pharmaceutica Sinica, 2007, 42(7): 787-793
Authors:GU Fu-gen  CUI Fu-de  GAO Yong-liang
Affiliation:1. Department of Pharmaceutics, Affiliated Hospital, Inner Mongolia Medical College, Hohhot 010059, China ; 2. School of Pharmacy, Shenyang Pharmaceutical University, Shenyang 110016, China ; 3. Institute of Pharmacology and Toxicology, Academy of Military Medical Sciences, Beijing 100850, China
Abstract:The pharmacodynamics of prostaglandin E1 (PGE1) administered by different routes to rats was investigated in this paper. The hypotensive effect of PGE, was used as an index of drug efficacy, pharmacodynamic parameters such as time to reach peak effect (Tmax), maximal percentage of blood pressure decrease (Emax, %), duration of effect (Td), and the area under the blood pressure decrease percent-time curves (AUC, % x min) were determined after PGE1 given to rats intranasally, sublingually, intraperitoneally (ip), and intramuscularly (im), separately, and compared with those obtained from intravenous (iv) administration. Similar to iv route, the pharmacodynamic parameters of PGE1 from the other administration routes, Emax, Td and in particular AUC values were all increased with increasing doses, showing dose-efficacy relationship. Tmax was found to be approximately 3-4 min for nasal route, 3-8 min for im, 6-8 min for ip and 12-30 min for sublingual route, separately. Thus, the order of magnitude of absorption rate of the drug was as follows: nasal approximately = im > ip > sublingual. If the pharmacological bioavailability (PF) for each administration route was used as a tentative measure of drug absorption extent, the order of magnitude of absolute bioavailability appeared as follows: nasal > im approximately = ip > sublingual. Furthermore, the interindividual difference was found to be larger for im and ip route than that for nasal and sublingual route. These results indicate nasal and sublingual routes are two promising routes for the systemic delivery of PGE1 in clinical applications.
Keywords:PGE1  pharmacodynamics  nasal delivery  sublingual absorption
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