Intravital multiphoton imaging of rhodamine 123 in the rat liver after intravenous dosing

IntraVital Pub Date : 2012-07-01 DOI:10.4161/intv.21450
Xin Liu, C. A. Thorling, Lu Jin, M. Roberts
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引用次数: 17

Abstract

Intravital imaging with multiphoton microscopy was used to investigate the hepatic disposition of rhodamine 123 (RH123) in the exposed liver of anesthetized rats after intravenous dosing. The role played by the biliary canalicular transporter P-glycoprotein (P-gp) on the disposition of RH123 was explored by administering a P-gp inhibitor, cyclosporine A prior to RH123 administration. The fluorescence intensity of RH123 was defined by multiphoton microscopy using a femtosecond laser excitation wavelength of 900 nm whereas the autofluorescence at an excitation wavelength of 740 nm was used to define the morphology of the liver acini. Intravital imaging showed that RH123 was rapidly taken up from the sinusoids into hepatocytes but slowly eliminated from the cells (half-life 2.89 ± 1.37 h). The presence of cyclosporine A did not affect the uptake of RH123 but markedly increased the fluorescence intensity of RH123 in the liver and was associated with a slower elimination of RH123 from the liver (half-life 11.5 ± 4.24 h). In conclusion, the spatial disposition of RH123 in the rat liver and the effects of a transporter inhibitor on its disposition have been monitored over time using intravital imaging.
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罗丹明123静脉给药后大鼠肝脏的多光子成像
采用多光子显微成像技术研究罗丹明123 (rhodamine 123, RH123)在麻醉大鼠暴露肝脏内静脉给药后的肝脏分布。通过在使用RH123之前使用p -糖蛋白抑制剂环孢素a,探讨了胆管转运蛋白p -糖蛋白(P-gp)在RH123处置中的作用。RH123的荧光强度用多光子显微镜测定,激发波长为900 nm的飞秒激光,激发波长为740 nm的自身荧光测定肝腺泡的形态。活体显像显示RH123从窦状体迅速被摄取到肝细胞,但从细胞中缓慢被清除(半衰期2.89±1.37 h),环孢素A的存在不影响RH123的摄取,但显著增加了RH123在肝脏中的荧光强度,并与RH123从肝脏中清除较慢(半衰期11.5±4.24 h)有关。RH123在大鼠肝脏中的空间分布以及转运体抑制剂对其分布的影响已经通过活体成像进行了长期监测。
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