임상약리학회지 (Journal of Korean Society for Clinical Pharmacology and Therapeutics)
- 제13권1호
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- Pages.84-91
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- 2005
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- 1225-5467(pISSN)
인체 간 미세소체(microsome)를 이용한 loperamide의 시토크롬(cytochrome) P450 3A4에 대한 억제작용
Inhibitory effect of Loperamide on Cytochrome P450 3A4 in Human Liver Microsomes
- 정명섭 (왈레스 기념 침례병원 소아과) ;
- 이태호 (왈레스 기념 침례병원 소아과) ;
- 문정웅 (왈레스 기념 침례병원 소아과) ;
- 변순옥 (왈레스 기념 침례병원 소아과) ;
- 박지영 (왈레스 기념 침례병원 소아과) ;
- 김경아 (가천대학교 의과대학 약리학과)
- Jeong, Myung-Sup (Department of Pediatrics, Wallace Memorial Baptist Hospital) ;
- Lee, Tae-Ho (Department of Pediatrics, Wallace Memorial Baptist Hospital) ;
- Moon, Jeong-Woong (Department of Pediatrics, Wallace Memorial Baptist Hospital) ;
- Byun, Soon-Ok (Department of Pediatrics, Wallace Memorial Baptist Hospital) ;
- Park, Ji-Young (Department of Pediatrics, Wallace Memorial Baptist Hospital) ;
- Kim, Kyoung-Ah (Department of Pharmacology, Gachon Medical School)
- 발행 : 2005.06.30
초록
Background : Loperamide, a peripherally acting opioid receptor agonist with a methadone-like structure and antidiarrheal action, is mainly metabolized to desmethylloperamide through. N-demethylation pathway. It has been reported that CYP2C8 and CYP3A4 might playa crucial role in loperamide Ndemethylation in therapeutic concentrations and loperamide might be an inhibitor of CYP3A4. However, there has been no available data to reveal it. The inhibitory effect of loperamide on CYP3A4 using midazolam 1'-hydroxylation was evaluated in vitro by human liver microsomes. Methods : Various concentrations of loperamide or ketoconazole (a selective and potent inhibitor of CYP3A4) were co-incubated with midazolam in human liver microsomes. CYP3A4-catalyzed midazolam metabolite, l'-hydroxymidazolam was analyzed by high-performance liquid chromatography (HPLC) to determine the inhibitory potency of loperamide on midazolam 1'-hydroxylation using