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P-糖蛋白和多药耐药相关蛋白2介导的奥曲肽在近端肾小管中的转运

P-glycoprotein- and mrp2-mediated octreotide transport in renal proximal tubule.

作者信息

Gutmann H, Miller D S, Droulle A, Drewe J, Fahr A, Fricker G

机构信息

Mount Desert Island Biological Laboratory, Salsbury Cove, Maine, ME 04672 USA.

出版信息

Br J Pharmacol. 2000 Jan;129(2):251-6. doi: 10.1038/sj.bjp.0703003.

Abstract
  1. Transepithelial transport of a fluorescent derivative of octreotide (NBD-octreotide) was studied in freshly isolated, functionally intact renal proximal tubules from killifish (Fundulus heteroclitus). 2. Drug accumulation in the tubular lumen was visualized by means of confocal microscopy and was measured by image analysis. Secretion of NBD-octreotide into the tubular lumen was demonstrated and exhibited the all characteristics of specific and energy-dependent transport. Steady state luminal fluorescence averaged about five times cellular fluorescence and was reduced to cellular levels when metabolism was inhibited by NaCN. 3. NBD-octreotide secretion was inhibited in a concentration-dependent manner by unlabelled octreotide, verapamil and leukotriene C(4) (LTC(4)). Conversely, unlabelled octreotide reduced in a concentration dependent manner the p-glycoprotein (Pgp)-mediated secretion of a fluorescent cyclosporin A derivative (NBDL-CS) and the mrp2-mediated secretion of fluorescein methotrexate (FL-MTX). 4. This inhibition was not due to impaired metabolism or toxicity since octreotide had no influence on the active transport of fluorescein (FL), a substrate for the classical renal organic anion transport system. 5. The data are consistent with octreotide being transported across the brush border membrane of proximal kidney tubules by both Pgp and mrp2.
摘要
  1. 在从鳉鱼(Fundulus heteroclitus)新鲜分离的、功能完整的肾近端小管中,研究了奥曲肽荧光衍生物(NBD - 奥曲肽)的跨上皮转运。2. 通过共聚焦显微镜观察并通过图像分析测量药物在肾小管腔中的蓄积。证明了NBD - 奥曲肽分泌到肾小管腔中,并表现出特异性和能量依赖性转运的所有特征。稳态管腔荧光平均约为细胞荧光的五倍,当用NaCN抑制代谢时,其降低至细胞水平。3. 未标记的奥曲肽、维拉帕米和白三烯C4(LTC4)以浓度依赖性方式抑制NBD - 奥曲肽的分泌。相反,未标记的奥曲肽以浓度依赖性方式降低荧光环孢素A衍生物(NBDL - CS)的P - 糖蛋白(Pgp)介导的分泌和荧光素甲氨蝶呤(FL - MTX)的mrp2介导的分泌。4. 这种抑制不是由于代谢受损或毒性,因为奥曲肽对荧光素(FL)的主动转运没有影响,荧光素是经典肾有机阴离子转运系统的底物。5. 数据表明奥曲肽通过Pgp和mrp2跨近端肾小管刷状缘膜转运。

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