Biomolecules & Therapeutics

The Korean Society of Applied Pharmacology (한국응용약물학회)
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General Pharmacology of ADP

  • Ban, Ju-Yeon (College of Veterinary Medicine and Research Institute of Veterinary Medicine, Chungbuk National University) ;
  • Lee, Bo-Young (College of Veterinary Medicine and Research Institute of Veterinary Medicine, Chungbuk National University) ;
  • Hong, Eun-Kyung (Medvill Research Lab) ;
  • Jung, Young-shin (Medvill Research Lab) ;
  • Seong, Yeon-Hee (College of Veterinary Medicine and Research Institute of Veterinary Medicine, Chungbuk National University)
  • Published : 2003.03.01
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Abstract

General pharmacological properties of ADP, a new pharmaceutical composition, which contains a mixed water extract obtained from the mixture of Phellodendron cortex (Phellodendron amurense) and Anemarrhena rhizoma (Anemarrhena asphodeloides), as the active ingredients, were investigated in experimental animals administering orally and in vitro test system. ADP had no influences on general behavior, pentobarbital sleeping time, spontaneous motor activity, motor coordination of mice, normal body temperature, chemoshock produced by pentylenetetrazole and writhing syndromes induced by 0.8% acetic acid at the dose of 150 and 1500 mg/kg. Gastric secretion of rats and intestinal motility of mice were not also influenced by the administration of ADP at doses of 150 and 1500 mg/kg, with the exception of the significant decrease of free HCI concentration at a dose of 1500 mg/kg in rats. ADP (150 and 1500 mg/kg) did not alter mean arterial blood pressure and heart rate in conscious rats. ADP given to anesthetized rats showed no effect on respiratory rate at the same doses. In in vitro experiments, ADP at the concentration of 150 mg/L did not show direct effect and inhibitory or augmentative action on histamine- or acetylcholine-induced contractions in the isolated ileum of guinea-pig. Taken together, these results indicate that ADP does not induce any adverse effects in experimental animals.

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References

  1. Ahn, D. (1998). Illustrated Book of Korean Medicinal Herbs Kyo-Hak Publishing Co., Ltd., Seoul
  2. Collier, H. 0. J., Dinneen, L.C., Johnson, C.A., and Schneider, C.(1968). The abdominal constriction response and ils Supres-sion by analgesic drugs in the mouse. Brit. J. Pharmac.Chemother.. 32, 295-310 https://doi.org/10.1111/j.1476-5381.1968.tb00973.x
  3. Dunham, N.W., Miya, T.S., and Edwards, C.D. (1957). Pharma-cological activily of a series of basic esters mono and dialkylmalonic acid. J. Am. Pharm. Assoc., 46, 208-209
  4. Hong, E.K., Kim, S.J., Kim, K.M., Oh, S.J., Kang, J.Y., Kim, S.J.,and Chung, Y.S. (2002) Water extract of the mixture of Ane-marrhena rhizoma and Phellodendron cortex has a relaxationeffect on the prostate and urethral smooth muscle of the rat. InProceedings of 50th Annual Coneress of the society for Medic-inal Plant Research. P101, A037, Spain, Barcellona
  5. Huang, K.C. (1999). The Pharmacology of Chinese Herbs. CRCPress., Florida
  6. Irwin, S. (1968). Comprehensive observational assessment; la. Asystematic, quantitative procedure for assessing the behavioraland physiologic state of the mouse. Psychopharmacohgia, 13,222-257 https://doi.org/10.1007/BF00401402
  7. Rang, H.P. (1964). Stimulant actions of volatile anaesthetics onsmooth muscle. Br. J. Pharmacol., 27, 256-375
  8. Shay, H., Sun, D.C., and Gruenstein, M. (1954) A quantitativemethod for measuring spontaneous gastric secretion in the rat.Gastroenterol., 26, 906-913
  9. Takemori, A.E., Kupferberg, H.T., and Miller, J.W. (1969). Quan-titative sludies of the antagonism of morphine by nalorphineand naloxone. J. Pharmacol. Exp. Ther., 169 39-45