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A cyanine-derived 'turn-on' fluorescent probe for imaging nitroreductase in hypoxic tumor cells

机译:一种花青来源的“开启”荧光探针,用于对缺氧肿瘤细胞中的硝基还原酶进行成像

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摘要

A new "turn-on" fluorescent probe, composed of a protected phenol group with a p-nitrobenzyl moiety that functions as a latent donor and conjugated with two benzo[f] indolinium acceptors, was developed and applied for imaging nitroreductase (NTR) in hypoxic tumor cells. Nitrobenzyl moieties on the substrate can be conveniently converted into aminobenzyl groups with a nitroreductase-catalyzed reaction in the presence of reduced nicotinamide adenine dinucleotide (NADH). This is followed by a cleavage reaction and the release of the free phenol moiety, which is manifested in enhanced fluorescence intensity during the detection process. Our experimental results show that the NTR detection ability is over 100 equivalents of other biological reductants (1 mM), whereas the confocal fluorescence imaging of tumor cells indicates the possibility of its application in biomedical research fields for tumor hypoxia diagnosis.
机译:研制了一种新的“开启”荧光探针,该探针由受保护的酚基和对硝基苄基部分组成,该对硝基苄基部分用作潜在的供体,并与两个苯并[f]吲哚鎓受体缀合,并用于成像硝基还原酶(NTR)。缺氧肿瘤细胞。在还原的烟酰胺腺嘌呤二核苷酸(NADH)存在下,可以通过硝基还原酶催化的反应将底物上的硝基苄基部分方便地转化为氨基苄基。随后是裂解反应和游离酚部分的释放,这在检测过程中表现为荧光强度增强。我们的实验结果表明,NTR的检测能力超过其他生物还原剂的100当量(1 mM),而肿瘤细胞的共聚焦荧光成像则表明了其在生物医学研究领域中用于肿瘤缺氧诊断的可能性。

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