首页> 美国卫生研究院文献>Marine Drugs >Reporter Dyes Demonstrate Functional Expression of Multidrug Resistance Proteins in the Marine Flatworm Macrostomum lignano: The Sponge-Derived Dye Ageladine A Is Not a Substrate of These Transporters
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Reporter Dyes Demonstrate Functional Expression of Multidrug Resistance Proteins in the Marine Flatworm Macrostomum lignano: The Sponge-Derived Dye Ageladine A Is Not a Substrate of These Transporters

机译:记者染料证明了海洋扁虫Macrostomum lignano中多药耐药蛋白的功能性表达:海绵衍生的染料Ageladine A不是这些转运蛋白的底物

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摘要

The marine plathyhelminth Macrostomum lignano was recently isolated from Adriatic shore sediments where it experiences a wide variety of environmental challenges, ranging from hypoxia and reoxygenation, feeding on toxic algae, to exposure to anthropogenic contaminants. As multidrug resistance transporters constitute the first line of defense against toxins and toxicants we have studied the presence of such transporters in M. lignano in living animals by applying optical methods and pharmacological inhibitors that had been developed for mammalian cells. Application of the MDR1 inhibitor Verapamil or of the MRP1 inhibitors MK571 or Probenecid increased the intracellular fluorescence of the reporter dyes Fura-2 am, Calcein am, Fluo-3 am in the worms, but did not affect their staining with the dyes Rhodamine B, CMFDA or Ageladine A. The marine sponge alkaloid Ageladine A remained intracellularly trapped for several days in the worms, suggesting that it does not serve as substrate of multidrug resistance exporters. In addition, Ageladine A did not affect multidrug resistance-associated protein (MRP)-mediated dye export from M. lignano or the MRP1-mediated glutathione (GSH) export from cultured rat brain astrocytes. The data obtained demonstrate that life-imaging is a useful tool to address physiological drug export from intact marine transparent flatworms by using multiphoton scanning microscopy.
机译:最近,海洋疟原虫Macrostomum lignano是从亚得里亚海沿岸沉积物中分离出来的,在那里面临着各种各样的环境挑战,从缺氧和复氧,以有毒藻类为食到暴露于人为污染物。由于多药耐药转运蛋白是抵抗毒素和毒物的第一道防线,因此我们通过应用光学方法和针对哺乳动物细胞开发的药理抑制剂研究了活体动物中木质素支原体中此类转运蛋白的存在。使用MDR1抑制剂维拉帕米或MRP1抑制剂MK571或Probenecid可以提高蠕虫中报告染料Fura-2 am,Calcein am,Fluo-3 am的细胞内荧光,但不影响其被若丹明B染料染色。 CMFDA或AgeladineA。海洋海绵生物碱Ageladine A在蠕虫中仍被困在细胞内数天,这表明它不能作为多药耐药性输出者的底物。此外,Ageladine A不会影响木质素支原体从多药耐药相关蛋白(MRP)介导的染料输出或从培养的大鼠脑星形胶质细胞输出的MRP1介导的谷胱甘肽(GSH)。获得的数据表明,通过使用多光子扫描显微镜,生命成像是解决完整海洋透明扁虫的生理药物输出的有用工具。

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