ÕªÒª£º Ä¿µÄ£º ³õ²½Ì½ÌÖ²ÝÃÞ»¨»¨°êÌáÈ¡Îï×Ü»Æͪ(FGF)¶Ô´ó¡¢Ð¡Êó¼±ÐÔʵÑéÐÔ¸ÎËðÉ˵ÄÓ°Ïì¡£·½·¨£º ÓÃDª²GalN(400 mg/kg)¼°CCl4(50%éÏé­ÓÍÈÜÒº,5 ml/kg)¶Ô´óÊó½øÐй¥»÷£»Óôó¼ÁÁ¿PAR(200 mg/kg)¶ÔСÊó½øÐй¥»÷£¬·Ö±ð½¨Á¢3ÖÖ¼±ÐÔʵÑéÐÔ¸ÎËðÉËÄ£ÐÍ£¬¹Û²ìFGF¶Ô´ó¡¢Ð¡ÊóѪÇå¹È±ûת°±Ã¸(ALT)¡¢¹È²Ýת°±Ã¸(AST)¡¢¸Î×éÖ¯³¬Ñõ»¯ÎïÆ绯ø(SOD)»îÐÔ¡¢±û¶þÈ©(MDA)º¬Á¿ÒÔ¼°¸Î×éÖ¯²¡Àí±ä»¯µÈÖ¸±êµÄÓ°Ïì¡£½á¹û£º·¢ÏÖFGF¶ÔDª²GalNÒýÆðµÄ¸ÎËðÉËÄ£ÐÍ(400 mg/kg¡Á7 d)µÄALTËä±ÈÄ£ÐÍ×éµÍ£¬µ«²îÒìÎÞͳ¼ÆѧÒâÒå(P>0.05)£»FGF (800 mg/kg¡Á7 d)ʹALTÃ÷ÏÔ½µµÍ£¬ÓëÄ£ÐÍ×éÏà±È£¬²îÒìÓÐͳ¼ÆѧÒâÒå(P<0.01)£»FGF(400¡¢800 mg/kg)ʹAST¾ùÃ÷ÏÔ½µµÍ£¬²îÒìÓÐͳ¼ÆѧÒâÒå(P<0.01)£»FGFÁ½¸ö¼ÁÁ¿×é¾ùʹMDAµÄº¬Á¿½µµÍ¡£FGFÁ½¸ö¼ÁÁ¿×é(400¡¢800 mg/kg)¶ÔCCl4ÒýÆðµÄ¸ÎËðÉËÄ£Ð;ùʹѪÇåALT¡¢ASTˮƽÃ÷ÏÔ½µµÍ£¬²¢ÄÜÌá¸ß¸Î×éÖ¯SOD»îÐÔ£¬½µµÍMDAº¬Á¿¡£FGF(800¡¢1 200 mg/kg)¶ÔPARÒýÆðµÄ¸ÎËðÉËÄ£Ð;ùʹѪÇåALT¡¢ASTˮƽÃ÷ÏÔ½µµÍ£¬²¢ÄÜÌá¸ß¸Î×éÖ¯SOD»îÐÔ£¬½µµÍMDAº¬Á¿¡£ÔÚ3ÖÖÄ£ÐÍÖÐFGF¾ùÄÜÃ÷ÏÔ¸ÄÉƸÎ×éÖ¯²¡ÀíËðÉ˳̶ȡ£½áÂÛ£ºFGF¶Ô´ó¡¢Ð¡Êó3ÖÖ»¯Ñ§ÐÔ¸ÎËðÉËÓÐÃ÷ÏԵı£»¤×÷Óã¬Æä»úÖÆ¿ÉÄÜÓëFGFµÄ¿¹Ñõ»¯×÷ÓÃÓйء£

    ¹Ø¼ü´Ê£º ²ÝÃÞ»¨×Ü»Æͪ£» ¼±ÐÔʵÑéÐÔ¸ÎÑ×£» ¹È±ûת°±Ã¸£» ³¬Ñõ»¯ÎïÆ绯ø£» ±û¶þÈ©

    Hepatoprotective effect of the total Flos Gossypium Flavonoid on the acute experimental hepatitis

    Subat, Parhat, Asiya

    (College of Pharmacay£¬ Xinjiang Medical University£¬ Urumqi 830054,China)

    Abstract: Objective: The effects of Flos Gossypium Flavonoid (FGF) on the acute experimental hepatitis induced by Dª²Galactasamine (Dª²GalN), carbon tetrachloride (CCl4) and paracetamol (PAR) were observed. Methods: Experimental hepatitis animal models were established in Wistar rats by an single intraperitoneal injection of Dª²GalN (400 mg/kg), a subdermal injection of CCl4 (5 ml/kg, 1¡Ã1 in olive oil) and an intraperitoneal injection of Par (200 mg/kg) in mice, respectively. Serum Alanine transferase (ALT), Aspartate tranferase (AST), liver super oxide dismutase (SOD), malondialdehyde (MDA) were examined. Results: FGF at a dose of 400 mg/kg decreased the serum ALT level but there is no significant difference compared with the hepatitis model induced by Dª²GalN (P>0.05); there was an significant difference when it was administered at a dose of 800 mg/kg (P<0.01), both dosages lowered the liver MDA content in the CCl4 induced hepatitis model, both dosages (FGF400 mg/kg), FGF significantly decreased serum ALT and AST elevation at both dosages and increased the SOD and GSH activities while lowered MDA content. In the PAR induced hepatitis model serum ALT and AST levels reduced with a preadministration of FGF at dosages of 800 mg/kg and 1200 mg/kg, and elevation in the SOD activity and a drop in MDA content were observed. Conclusion: FGF possesses a significant hepatoprotection against the three kinds of chemically induced hepatitis. ......