期刊文献+
任意字段
题名或关键词
题名
关键词
文摘
作者
第一作者
机构
刊名
分类号
参考文献
作者简介
基金资助
栏目信息

肠道CYP3A和P-gp:口服药物的吸收屏障 被引量:6

The intestinal cytochrome P450 3A and P-glycoprotein:barriers to drug absorption
暂未订购
导出
摘要 细胞色素P4 5 0 3A (CYP3A)亚族是人类药物代谢最重要的I相酶。由MDR1基因编码的外向转运载体蛋白P糖蛋白 (P gp)为药物外排泵。这两种蛋白质在口服药物吸收的主要部位胃肠道均有高表达 ,同时二者的底物具有明显的重叠性。近来 ,大量研究表明 ,决定口服药物生物利用度的主要因素是肠道细胞CYP3A对已吸收药物的生物转化作用和肠道细胞中P gp对已吸收药物的主动外排作用。如果药物为CYP3A和 (或 )P gp的底物 ,当其与CYP3A和P gp的抑制剂同时服用后 。 Cytochrome P450 3A (CYP3A/CYP3A4), the major phase I drug metabolizing enzyme in humans, and the MDR1 gene expressed P-glycoprotein (P-gp), the drug efflux pump, are present at high levels in the villus tip of enterocytes of gastrointestinal tract, the primary site of absorption for orally administrated drugs, and share a significant overlap in substrate specificity. It has been recognized that metabolism by intestinal CYP3A/CYP3A4 is one of the major determinants of oral drug bioavailability. More recently, a large body of research has demonstrated that drug extrusion by intestinal P-gp can both reduce drug absorption and modulate the effects of inhibitors and inducers of CYP3A/CYP3A4-mediated metabolism. A growing number of animal data and clinical studies, both in vitro and in vivo, have indicated that concomitant administration of CYP3A/CYP3A4 inhibitors and/or P-gp inhibitors can increase the oral bioavailability of a wide range of drugs, which are CYP3A/CYP3A4 and P-glycoprotein substrates.
作者 王堃 仲来福
机构地区 大连医科大学毒理学教研室
出处 《中国药理学通报》 CAS CSCD 北大核心 2003年第11期1216-1219,共4页 Chinese Pharmacological Bulletin
关键词 细胞色素P450(CYP450) CYP3A CYP3A4 P糖 蛋白(P-gp) 口服生物利用度 肠道 cytochrome P450 (CYP450) CYP3A CYP3A4 P-glycoprotein oral bioavailability gut
分类号 R-05 [医药卫生] R329.24 [医药卫生—人体解剖和组织胚胎学]
  • 相关文献

参考文献19

  • 1Higgins CF. ABC transporters: From microorganisms to man.Annu Rev Cell Biol, 1992 ;8:67-113.
  • 2Schinkel AH, Smit J J, van Tellingen Oet al. Disrupion of the mouse mdrla P-glycopreotein gene leads to a deficiency in the blood-brain barrier and to increased sensitivity to drugs. Cell,1994;77(4):491 -502.
  • 3Schumacher U, Mollgard K. The muhidrug-resistanee P-glycoprotein (P-gp, MDR1)I an early marker of blood-brain barrier development in the microvessels of the developing of human brain. Histochem Cell Biol, 1997;108(2): 179-82.
  • 4Hoffermeyers S, Burk O, von Richter 0 et al. Functional polymorphisms of the human muhidrug-resistance gene: Multiple sequence variations and correlation of one allele with P-glycoprotein expression and activity in vlvo. Proc Natl Acad Sci USA,2000;97(7):3473~8.
  • 5Sparreboom A, van Asperen J, Mayer U et al. Limited oral bioavailability and active eothelial excertion of paclitaxel(Taxol) caused by P-glycoprotein in the intestine. Proc Natl Acad Sci USA, 1997;94(5) :2031-5.
  • 6Meerm-Terwogt JM, Beijnen JH, ten Bokkel Huinink WW et al. Co-adiministration of cyclosporin enables oral therapy with paclitaxel. Lancet,1998;352(9124) :285.
  • 7Kim Rb, Fromm MF, Wandel C etal. The drug transporter P-glyeoprotein limits oral absoption and brain entry of HIV-1 protease inhibitors. J Clin Invest, 1998 ; 101 (2) : 289- 94.
  • 8Schellens JH, Malingre MM, Kruijtzer CM et al. Modulaton of oral bioavailability of anticancer drugs: From mouse to man. EurJ Pharm Sci, 2000;12(2):103-10.
  • 9Bent LZ, Kroetz DL, Sheiner LB. Pharmaeokkineties:The dynamics of drug absorption, distribution, and elimination. In: Hardman JH, Limbird LE, Molinoff PB et al, editors. Goodman H Gilman's the pharmacological basis of therapetics. New York: McGraw-Hill, 1996:3-28.
  • 10Wacher VJ, Silverman JA, Zhang Y et al. Role of P-glycoprotein and cytochrome P450 3A in limiting oral absorption of peptides and peptidominetics. J Pharm Sci, 1998;87(11) : 1322-3O.

同被引文献40

  • 1袁园,汪鋆植,邓李蓉,高元喜,叶汪阳,张晓兰,邓改改.栓菌酸对耐索拉非尼肝癌细胞HepG2/Sora的影响及机制[J].中药药理与临床,2022,38(3):76-81. 被引量:1
  • 2代方国,罗仁,王宇光,夏成云,谭洪玲,肖成荣,赵永红,高月.甘遂配伍甘草对大鼠肝脏CYP3A2影响[J].第四军医大学学报,2005,26(10):951-953. 被引量:44
  • 3刘念,耿小平,熊茂明.P-糖蛋白抑制剂的研究进展[J].国外医学(药学分册),2006,33(2):107-110. 被引量:7
  • 4郑姣,周宏灏.黄酮类化合物对细胞色素P450 CYP1,2E1,3A4和19的影响[J].药学学报,2007,42(1):8-12. 被引量:27
  • 5BAILEY D G, MALCOLM J, ARNOLD O, et al. Grapefruit juice-drug interactions[J]. Br J Clin Pharmacol, 1998, 46 (2): 101-110.
  • 6MOUNTFIELD R J, SENEPIN S, SCHLEIMER M, et al. Potential inhibitory effects of formulation ingredients on intestinal cytochrome P450[J].Int J Pharm, 2000, 211 (1): 89-92.
  • 7BRAVO G R C, BOESS F, DURR E, et al. In vitro investigation on the impact of Solutol HS 15 on the uptake of colchicine into rat hepatocytes[J].Int J Pharm, 2004, 279 (1): 27-31.
  • 8YAMANO K, YAMAMOTO K, KOTAKI H, et al. Quantitative prediction of metabolic inhibition of midazolam by itraconazole and ketoconazole in rats: Implication of concentrative uptake of inhibitors into liver[J]. Drug Metab Dispos, 1999, 27 (3) : 395-402.
  • 9TSUTOMU K B L, VON MOLTKE M C, MICHAEL D P, et al. In vitro, pharmacokinetic, and pharmacodynamic interactions of ketoconazole and midazolam in the rat [J]. J Pharmacol Exp Ther, 2002, 302 (3) : 1228-1237.
  • 10KIM R B, WANDEL C, LEAKE B, et al. Interrelationship between substrates and inhibitors of human CYP3A and P-glycoprotein[J]. Pharm Res, 1999, 16 (3): 408-414.

引证文献6

二级引证文献22

中国药理学通报
2003年 第11期

相关作者

内容加载中请稍等...

相关机构

内容加载中请稍等...

相关主题

内容加载中请稍等...

浏览历史

内容加载中请稍等...
;
使用帮助 返回顶部