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尼古丁通过血视网膜内屏障的载体介导转运:一种由外向H(+)梯度驱动的新型有机阳离子转运体的参与。

Carrier-Mediated Transport of Nicotine Across the Inner Blood-Retinal Barrier: Involvement of a Novel Organic Cation Transporter Driven by an Outward H(+) Gradient.

作者信息

Tega Yuma, Kubo Yoshiyuki, Yuzurihara Chihiro, Akanuma Shin-Ichi, Hosoya Ken-Ichi

机构信息

Department of Pharmaceutics, Graduate School of Medicine and Pharmaceutical Sciences, University of Toyama, Toyama, Japan.

出版信息

J Pharm Sci. 2015 Sep;104(9):3069-75. doi: 10.1002/jps.24453. Epub 2015 Apr 17.

Abstract

The present study was carried out to investigate the blood-to-retina transport of nicotine across the inner blood-retinal barrier (BRB). Using the in vivo vascular injection method, the blood-to-retina influx clearance of nicotine across the BRB was determined as 131 μL/(min?g retina), which is much higher than that of a nonpermeable paracellular marker, and blood-to-retina transport of nicotine was inhibited by organic cations such as pyrilamine and verapamil. The nicotine uptake by a conditionally immortalized rat retinal capillary endothelial cell line (TR-iBRB2 cells), an in vitro model of the inner BRB, exhibited time, temperature, and concentration dependence with a Km of 492 μM. These results suggest the involvement of a carrier-mediated transport process in nicotine transport in the inner BRB. The nicotine uptake by TR-iBRB2 cells was stimulated by an outwardly directed H(+) gradient, and the uptake was significantly inhibited by bulky and hydrophobic cationic drugs, whereas inhibitors of organic cation transporters did not show inhibitory effect. These results suggest that the novel organic cation transport system driven by an outwardly directed H(+) gradient is involved in the blood-to-retina transport of nicotine across the inner BRB.

摘要

本研究旨在调查尼古丁跨越内血视网膜屏障(BRB)的血视网膜转运情况。采用体内血管注射法,测定尼古丁跨越BRB的血视网膜流入清除率为131 μL/(min·g视网膜),这远高于非通透旁细胞标志物的清除率,并且尼古丁的血视网膜转运受到诸如吡苄明和维拉帕米等有机阳离子的抑制。在条件永生化大鼠视网膜毛细血管内皮细胞系(TR-iBRB2细胞)(内BRB的体外模型)中,尼古丁摄取呈现时间、温度和浓度依赖性,其米氏常数(Km)为492 μM。这些结果表明,在内BRB中,尼古丁转运涉及载体介导的转运过程。TR-iBRB2细胞对尼古丁的摄取受到外向H(+)梯度的刺激,并且摄取受到体积大且疏水的阳离子药物显著抑制,而有机阳离子转运体抑制剂未显示出抑制作用。这些结果表明,由外向H(+)梯度驱动的新型有机阳离子转运系统参与了尼古丁跨越内BRB的血视网膜转运。

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