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Chinese Journal of Clinical Pharmacology and Therapeutics ›› 2010, Vol. 15 ›› Issue (7): 794-797.

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Evaluation of sustained-release effect on Compound Danshen Skeleton Sustained-Release Tablet by pharmacodynamics method

XU Guo-liang, TANG Xi-lan, SHAN Yi-min, ZHANG Qi-yun, ZHENG Qin, YANG Ming   

  1. Key Laboratory of Modern Preparation of TCM (Ministry of Education), Jiangxi University of Traditional Chinese Medicine, Nanchang 330004, Jiangxi, China
  • Received:2010-05-24 Revised:2010-06-24 Online:2010-07-26 Published:2020-09-15

Abstract: AIM: To evaluate the sustained-release effect on Compound Danshen Skeleton Sustained-Release Tablet (CDSRT) by pharmacodynamics method.METHODS: By reference to Compound Danshen Tablet(CDT), Sprague-Dawley rats had been administrated with CDT and CDSRT with the content of crude drugs 2911.14 mg/kg. The medicated serum of CDT and CDSRT were prepared at the time of 0.25,0.5,0.75,1,2,4,8,12 h after single oral administration. The medicated serums were added to myocardial cells respectively. The protective effects of CDT and CDSRT on hypoxia/reoxygenation and the sustained-release effect of CDSRT were evaluated.RESULTS: Compared with the H/R model group, the medicated serum of CDT 4,8 h and CDSRT 2,4,8,12 h had apparent protective effects against proliferation inhibition caused by hypoxia/reoxygenation(H/R) induced injury in myocardial cells. The present half-life t1/2(ka) of CDT and CDSRT were 2.655 h and 0.719 h. The peak times of effective action were 5.213 h and 2.957 h. And the elimination half-life t1/2(ke) were 4.953 h and 10.166 h respectively. Compared with CDT, CDSRT had a higher speed of the effect present and the peak time of effective action and a lower speed of sustained-release.CONCLUSION: CDSRT has a certain sustained-release function as t1/2(ke) longer than that of CDT. Pharmacodynamics method is a feasible method for the evaluation of CDSRT sustained-release effect.

Key words: Compound Danshen Skeleton Sustained Release Tablet, Pharmacodynamics, Sustained-release function

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