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Evaluation of sulfane sulfur bioeffects via a mitochondria-targeting selenium-containing near-infrared fluorescent probe

机译:通过线粒体靶向含硒的近红外荧光探针评估亚磺烷硫生物效应

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As a crucial member in antioxidant regulatory systems, sulfane sulfur plays essential roles in cytoprotective mechanisms by directly eliminating ROS and altering ROS-mediated redox signaling. Despite the rising interests in sulfane sulfur, there only a few bio-compatible methods are available for its direct detection. Moreover, most of the existing methods cannot meet the requirements of real-time detection due to the reactive and labile chemical properties of sulfane sulfur. Therefore, we strive to clarify the mutual relationship between mitochondria sulfane sulfur and ROS under hypoxia stress. Herein, we report a near-infrared fluorescent probe Mito-SeH for the selective imaging of mitochondrial sulfane sulfur in cells and in vivo under hypoxia stress. Mito-SeH includes three moieties: a selenol group (-SeH) as the stronger sulfur-acceptor; a near-infrared azo-BODIPY fluorophore as the fluorescent modulator; a lipophilic alkyltriphenylphosphonium cation as the mitochondrial delivery. Mito-SeH exhibits excellent selectivity and sensitivity towards the detection of mitochondria sulfane sulfur. The hypoxia response behavior of Mito-SeH is evaluated in monolayer cell and three-dimensional multicellular spheroid to clarify the relationship between sulfane sulfur and hypoxia. We confirm that sulfane sulfur protection mechanism against hypoxia is to inhibition of caspase-dependent apoptosis through directly scavenging ROS pathway. The probe is also applied to measurement of sulfane sulfur in ex vivo-dissected organs of hypoxic mouse model, as well as the probe is successfully used for real-time monitoring the changes of sulfane sulfur and ROS in acute ischemia mice model. We suggest that sulfane sulfur may be a novel therapeutic agent for hypoxia-induced injury. (C) 2018 Elsevier Ltd. All rights reserved.
机译:作为抗氧化调节系统中的关键构件,磺胺硫在细胞保护机制中起主要作用通过直接消除ROS和改变ROS介导的氧化还原信号传导。尽管亚磺砜兴趣兴起,但只有少数生物相容方法可用于其直接检测。此外,由于磺胺硫的反应性和不稳定化学性质,大多数现有方法不能满足实时检测的要求。因此,我们努力阐明缺氧胁迫下线粒体磺胺硫和RO之间的相互关系。在此,我们报告了近红外荧光探针MITO-SEH,用于在缺氧胁迫下进行细胞中的线粒体磺胺硫的选择性成像和体内。 MITO-SEH包括三个部分:SELENOL组(-SEH)作为较强的硫 - 受体;近红外偶氮二桥荧光团作为荧光调制器;脂质酰基三苯基鏻阳离子作为线粒体递送。 MITO-SEH对检测线粒体磺胺硫的选择性以及敏感性。在单层细胞和三维多细胞球状体中评价MITO-SEH的缺氧响应行为,以阐明磺胺硫和缺氧之间的关系。我们证明,磺胺硫保护机制抗缺氧是通过直接清除ROS途径来抑制依赖胱天蛋白酶依赖性细胞凋亡。探针还应用于缺氧小鼠模型的离体沉积器官中磺胺硫的测量,以及探针成功地用于实时监测急性缺血小鼠模型中磺胺硫和RO的变化。我们认为磺胺硫可能是一种新的缺氧诱导损伤的治疗剂。 (c)2018年elestvier有限公司保留所有权利。

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