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首页> 外文期刊>Molecular imaging and biology: MIB : the official publication of the Academy of Molecular Imaging >Role of Sodium Taurocholate Cotransporting Polypeptide as a New Reporter and Drug-Screening Platform: Implications for Preventing Hepatitis B Virus Infections
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Role of Sodium Taurocholate Cotransporting Polypeptide as a New Reporter and Drug-Screening Platform: Implications for Preventing Hepatitis B Virus Infections

机译:牛磺酸钠COT转化多肽作为新的记者和药物筛查平台的作用:对预防乙型肝炎病毒感染的影响

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Purpose Sodium taurocholate cotransporting polypeptide (NTCP) is a transmembrane protein responsible for delivering indocyanine green (ICG), an ideal infrared fluorescent dye, from extracellular space into the cytoplasm. Additionally, NTCP located in the hepatocyte membrane is the portal for hepatitis B and D virus (HBV/HDV) infections. This study verified the feasibility of NTCP as a reporter and further established a drug-screening platform for HBV/HDV infections. Procedures NTCP was transduced into HT-29, a colorectal cancer cell line. To examine the use of NTCP as a reporter, NTCP-expressing cells were treated with ICG and examined through flow cytometry, an in vivo imaging system (IVIS), and confocal microscopy. Furthermore, ICG was administrated to NTCP-expressing tumor-bearing nude mice and examined using the IVIS. To study the drug-screening platform, NTCP-expressing cells were treated with cyclosporin A, an NTCP inhibitor, and ICG, and examined using a multimode detection platform. Moreover, nude mice were injected with NTCP inhibitors and ICG, and subsequently, their ICG signal was examined in vivo and in the blood. Results In the reporter study, the ICG signal was higher in NTCP-expressing cells/tumors than in control cells/tumors after ICG treatment. In the drug-screening platform study, NTCP-expressing cells had decreased ICG intensity after treatment with NTCP inhibitors and ICG. Nude mice that were administered cyclosporin A had lower ICG intensity in the liver and higher intensity in the peripheral tissue and blood. Conclusions NTCP and ICG form an ideal reporter system with extensive applications in cancer biology, robust drug-drug interactions, and drug screening in HBV/HDV infections.
机译:目的牛磺酸钠COTRANSPORTING多肽(NTCP)是一种跨膜蛋白,其负责递送吲哚菁绿(ICG),理想红外荧光染料,从细胞外空间进入细胞质。另外,位于肝细胞膜中的NTCP是乙型肝炎和D病毒(HBV / HDV)感染的门户。本研究验证了NTCP作为记者的可行性,并进一步建立了用于HBV / HDV感染的药物筛查平台。程序NTCP被转导入HT-29,一种结肠直肠癌细胞系。为了检查NTCP作为报告的使用,用ICG处理NTCP表达细胞,并通过流式细胞术检查,体内成像系统(IVIS)和共聚焦显微镜检查。此外,ICG被施用于表达NTCP的肿瘤裸鼠并使用IVIS检查。为了研究药物筛选平台,用环孢菌素A,NTCP抑制剂和ICG处理NTCP表达细胞,并使用多模检测平台检查。此外,用NTCP抑制剂和ICG注射裸鼠,随后,它们的ICG信号在体内和血液中进行检查。结果在报告研究中,在ICG治疗后,NTCP表达细胞/肿瘤中的ICG信号较高。在药物筛选平台研究中,用NTCP抑制剂和ICG治疗后,NTCP表达细胞的ICG强度降低。施用环孢菌素A的裸鼠在肝脏中具有较低的ICG强度,并且在外周组织和血液中的更高强度。结论NTCP和ICG在HBV / HDV感染中具有广泛应用的理想报告系统,具有广泛应用,鲁棒药物 - 药物相互作用和药物筛选。

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