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首页> 外文期刊>Theranostics >A Turn-On Optoacoustic Probe for Imaging Metformin-Induced Upregulation of Hepatic Hydrogen Sulfide and Subsequent Liver Injury
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A Turn-On Optoacoustic Probe for Imaging Metformin-Induced Upregulation of Hepatic Hydrogen Sulfide and Subsequent Liver Injury

机译:用于成像成像的二甲双胍诱导的肝硫化氢上调和随后的肝损伤的光声探头。

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Metformin is currently the most prescribed oral agent for diabetes treatment; however the overdose or long-term use may cause some severe side effects such as liver injury. Researches indicate that metformin-induced liver injury is closely related to upregulation of hepatic Hsub2/subS. Hence, monitoring hepatic Hsub2/subS generation induced by metformin could be an effective approach for evaluating hepatoxicity of the drug. Methods: We present a novel turn-on and dual-mode probe for detecting and imaging metformin-induced liver injury by specifically tracking the upregulation of hepatic Hsub2/subS with fluorescent and optoacoustic methods. After reaction with Hsub2/subS, the strong electron-withdrawing group dinitrophenyl ether (which acts as both the recognition moiety and the fluorescence quencher) was cleaved and replaced by an electron-donating group hydroxyl. This correspondingly leads to the changes of the probe's electronic state and absorption red-shifting as well as the subsequent turn-on fluorescent and optoacoustic signals. Results: The probe was applied to the colon tumor-bearing mice model and the metformin-induced liver injury mice model to achieve tumor imaging and liver injury assessment. The biosafety of the probe was verified by histological analysis (hematoxylin and eosin staining) and serum biochemical assays. Conclusion: The probe responds quickly to Hsub2/subS in tumors and the liver, and MSOT imaging with the probe offers cross-secitonal and 3D spatial information of liver injury. This study may provide an effective approach for accessing medication side effects by tracking drug-metabolism-related products.
机译:二甲双胍是目前治疗糖尿病最常用的口服药物。但是,过量或长期使用可能会导致一些严重的副作用,例如肝损伤。研究表明,二甲双胍引起的肝损伤与肝H 2 S的上调密切相关。因此,监测二甲双胍诱导的肝H 2 S的产生可能是评估该药物肝毒性的有效方法。方法:我们提出了一种新颖的双模式探针,用于通过荧光和声光方法特异性跟踪肝H 2 S的上调来检测和成像二甲双胍引起的肝损伤。与H 2 S反应后,强吸电子基二硝基苯醚(同时充当识别部分和荧光猝灭剂)被裂解并被给电子基团羟基取代。这相应地导致探针的电子状态和吸收红移以及随后的开启荧光和光声信号的变化。结果:该探针应用于结肠结肠癌小鼠模型和二甲双胍诱导的肝损伤小鼠模型,以实现肿瘤成像和肝损伤评估。通过组织学分析(苏木精和曙红染色)和血清生化分析验证了探针的生物安全性。结论:该探针对肿瘤和肝脏中的H 2 S反应迅速,并且利用该探针进行MSOT成像可提供跨损伤和3D肝脏损伤的空间信息。这项研究可能通过跟踪与药物代谢有关的产品,为获得药物副作用提供有效的方法。

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