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顶端钠依赖性胆酸共转运蛋白,一种新型的吲哚菁绿转运体及其在药物筛选中的应用。

Apical Sodium-Dependent Bile Acid Cotransporter, A Novel Transporter of Indocyanine Green, and Its Application in Drug Screening.

机构信息

Department of Medical Imaging, Taipei TzuChi General Hospital, Buddhist Tzu-Chi Medical Foundation, No.289, Jianguo Rd., Xindian Dist., New Taipei city 23142, Taiwan.

School of Medicine, Tzu Chi University, No. 701, Sec. 3, Zhongyang Rd., Hualien 97004, Taiwan.

出版信息

Int J Mol Sci. 2020 Mar 23;21(6):2202. doi: 10.3390/ijms21062202.

Abstract

Bile acid plays critical roles in the elimination of inorganic compounds such as bilirubin, heavy metals, and drug metabolites. Apical sodium-dependent bile acid cotransporter (ASBT), a solute carrier membrane transport protein, transports bile acids. Several inhibitors of ASBT have been evaluated in clinical trials. Sodium taurocholate cotransporting polypeptide (NTCP), belonging to the same family as ASBT, has fluorescein 5(6)-isothiocyanate (FITC) and indocyanine green (ICG) transportability. ICG, a Food and Drug Administration-approved fluorophore at near-infrared range, has perfect optical characteristics, so it can be applied in cell tracking and drug screening. In this study, ASBT and NTCP were transduced into the HT-1080 cell line. Nude mice were subcutaneously xenografted with control and ASBT-expressing cells. ICG transportability was observed through flow cytometry, fluorescent microscopy, multi-mode plate readers, and an in vivo imaging system. Several molecules, including taurocholate, sodium deoxycholate, cyclosporine A, nifedipine, and Primovist, were used to evaluate an in vitro drug-screening platform by using the combination of ICG and ASBT through flow cytometry. ICG and FITC were validated and shown to be transported by ASBT. NTCP had a higher ICG intensity compared with ASBT. For cell tracking, the ASBT xenograft had similar ICG signals as the control. For a drug-screening platform, the ICG intensity decreased with 186 μM taurocholate (56.8%), deoxycholate (83.8%), and increased with nifedipine (133.2%). These findings are suggestive of opportunities for the high-throughput drug screening of cholestasis and other diseases that are related to the dynamics of bile acid reabsorption.

摘要

胆汁酸在消除胆红素、重金属和药物代谢物等无机化合物方面发挥着关键作用。顶膜钠依赖性胆汁酸共转运蛋白(ASBT)是一种溶质载体膜转运蛋白,可转运胆汁酸。已有几种 ASBT 抑制剂在临床试验中进行了评估。牛磺胆酸钠共转运蛋白(NTCP)与 ASBT 同属一个家族,具有荧光素 5(6)-异硫氰酸酯(FITC)和吲哚菁绿(ICG)转运能力。ICG 是近红外范围内获得美国食品和药物管理局批准的荧光团,具有完美的光学特性,因此可应用于细胞跟踪和药物筛选。在这项研究中,ASBT 和 NTCP 被转导到 HT-1080 细胞系中。裸鼠皮下异种移植对照和 ASBT 表达细胞。通过流式细胞术、荧光显微镜、多模式板读数器和体内成像系统观察 ICG 的转运能力。使用包括牛磺胆酸钠、脱氧胆酸钠、环孢素 A、硝苯地平、Primovist 在内的几种分子,通过流式细胞术评估了一种结合 ICG 和 ASBT 的体外药物筛选平台。验证了 ICG 和 FITC 可被 ASBT 转运。NTCP 的 ICG 强度高于 ASBT。用于细胞跟踪,ASBT 异种移植与对照具有相似的 ICG 信号。对于药物筛选平台,随着 186μM 牛磺胆酸钠(56.8%)、脱氧胆酸钠(83.8%)的增加,ICG 强度降低,而硝苯地平(133.2%)增加。这些发现为胆汁淤积症和其他与胆汁酸重吸收动力学相关的疾病的高通量药物筛选提供了机会。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ef32/7139337/cbf50565b034/ijms-21-02202-g001.jpg

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