新型近红外荧光胆汁酸衍生物 (NIRBAD) 的合成、表征及其在肝功能评估中的潜在用途。

IF 4 2区 化学 Q1 BIOCHEMICAL RESEARCH METHODS Bioconjugate Chemistry Bioconjugate Pub Date : 2024-07-03 DOI:10.1021/acs.bioconjchem.4c00168
Alvaro G Temprano, Beatriz Sanchez de Blas, Concepción Pérez-Melero, Ricardo Espinosa-Escudero, Oscar Briz, Paula Cinca-Fernando, Lucia Llera, Maria J Monte, Francisco A Bermejo-Gonzalez, Jose J G Marin, Marta R Romero
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引用次数: 0

摘要

传统的血清标记物往往不能准确检测出许多肝病所伴有的胆汁淤积。虽然血清胆汁酸(BA)水平的升高能灵敏地反映肝胆功能受损的情况,但改变胆汁酸池大小和肠肝循环的其他因素也会影响胆汁酸水平。为了通过实时监测方法开发用于体外无创肝胆功能评估的荧光探针,研究人员利用 1,3-二极环加成反应将近红外(NIR)荧光色素与叠氮功能化的 BA 衍生物(BAD)共轭。所得化合物(NIRBADs)经色谱(FC 和 PTLC)纯化(>95%),并通过荧光测定法、1H NMR 和使用 ESI 电离耦合四极 TOF 质量分析的 HRMS 进行表征。利用流式细胞仪对稳定表达 BA 载体 NTCP 的 CHO 细胞进行了运输研究。通过高分辨率成像分析检测了麻醉大鼠的体外荧光。通过酯类(NIRBAD-1)或酰胺类(NIRBAD-3)间隔物,或通过三唑连接(NIRBAD-2)在 3α 位将炔菁 718 与胆酸(CA)的 COOH 基连接,合成了三种 NIRBAD。表达 NTCP 的细胞能有效吸收 NIRBAD,而牛胆酸(TCA)能抑制 NIRBAD 的吸收。给大鼠静脉注射 NIRBAD-3 后,可在体外监测肝脏摄取和随之释放的近红外荧光。这种瞬时器官特异性处理与炔菁 718 不向肠道释放和其他探针(如吲哚菁绿)缺乏肝趋性形成鲜明对比。服用 NIRBAD-3 不会改变肝脏和肾脏毒性的血清生物标志物。NIRBAD 可作为探针,通过无创体外方法评估肝胆功能。
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Synthesis, Characterization, and Potential Usefulness in Liver Function Assessment of Novel Bile Acid Derivatives with Near-Infrared Fluorescence (NIRBAD).

Conventional serum markers often fail to accurately detect cholestasis accompanying many liver diseases. Although elevation in serum bile acid (BA) levels sensitively reflects impaired hepatobiliary function, other factors altering BA pool size and enterohepatic circulation can affect these levels. To develop fluorescent probes for extracorporeal noninvasive hepatobiliary function assessment by real-time monitoring methods, 1,3-dipolar cycloaddition reactions were used to conjugate near-infrared (NIR) fluorochromes with azide-functionalized BA derivatives (BAD). The resulting compounds (NIRBADs) were chromatographically (FC and PTLC) purified (>95%) and characterized by fluorimetry, 1H NMR, and HRMS using ESI ionization coupled to quadrupole TOF mass analysis. Transport studies using CHO cells stably expressing the BA carrier NTCP were performed by flow cytometry. Extracorporeal fluorescence was detected in anesthetized rats by high-resolution imaging analysis. Three NIRBADs were synthesized by conjugating alkynocyanine 718 with cholic acid (CA) at the COOH group via an ester (NIRBAD-1) or amide (NIRBAD-3) spacer, or at the 3α-position by a triazole link (NIRBAD-2). NIRBADs were efficiently taken up by cells expressing NTCP, which was inhibited by taurocholic acid (TCA). Following i.v. administration of NIRBAD-3 to rats, liver uptake and consequent release of NIR fluorescence could be extracorporeally monitored. This transient organ-specific handling contrasted with the absence of release to the intestine of alkynocyanine 718 and the lack of hepatotropism observed with other probes, such as indocyanine green. NIRBAD-3 administration did not alter serum biomarkers of hepatic and renal toxicity. NIRBADs can serve as probes to evaluate hepatobiliary function by noninvasive extracorporeal methods.

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来源期刊
CiteScore
9.00
自引率
2.10%
发文量
236
审稿时长
1.4 months
期刊介绍: Bioconjugate Chemistry invites original contributions on all research at the interface between man-made and biological materials. The mission of the journal is to communicate to advances in fields including therapeutic delivery, imaging, bionanotechnology, and synthetic biology. Bioconjugate Chemistry is intended to provide a forum for presentation of research relevant to all aspects of bioconjugates, including the preparation, properties and applications of biomolecular conjugates.
期刊最新文献
Permutational Encoding Strategy Accelerates HIT Validation from Single-Stranded DNA-Encoded Libraries. Photoinduced Charge Centralization Quenches the Fluorescence of Conjugation-Fused Tetrazine Labels with Red-to-Near-Infrared Emissions. Size-Dependent Glioblastoma Targeting by Polymeric Nanoruler with Prolonged Blood Circulation. Synthesis, Characterization, and Potential Usefulness in Liver Function Assessment of Novel Bile Acid Derivatives with Near-Infrared Fluorescence (NIRBAD). Development of an FAP-Targeted PET Probe Based on a Novel Quinolinium Molecular Scaffold.
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