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Mito-specific cascade amplifier sniping metabolism homeostasis for multimodal imaging-guided antitumor bioenergetic therapy
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作者 Jingjing Yang Yuanlin Zhang +5 位作者 Maoquan Chu Jin Qian Jie Liu Manyu Wang Zhe Qiang Jie Ren 《Nano Research》 SCIE EI CSCD 2024年第11期9908-9919,共12页
Nicotinamide adenine dinucleotide (NAD+/NADH) pools homeostasis is recognized as an Achilles’ Heel in tumor metabolism reprogramming. However, mitochondria can enable cancer cells to overcome NADH exhaustion by provi... Nicotinamide adenine dinucleotide (NAD+/NADH) pools homeostasis is recognized as an Achilles’ Heel in tumor metabolism reprogramming. However, mitochondria can enable cancer cells to overcome NADH exhaustion by providing NAD+ precursors and/or intermediates, thus promoting their survival rate and potentially driving uncontrollable proliferation. Here, a synergistic intervention NAD+/NADH homeostasis and mitochondrial metabolism strategy with magnetic resonance imaging (MRI)/photoacoustic imaging (PAI) are developed to address grand challenge of metabolic reprogramming for antitumor bioenergetic therapy. A mitochondrial-targeted cascade amplification nanoplatform ([β-MQ]TRL), triggered by NAD(P)H: quinone oxidoreductase-1 (NQO1), can enable a continuous depletion of cytosol NADH until cell death. The end-product, hydrogen peroxide (H_(2)O_(2)), can be further catalytically converted to higher toxic ·OH in proximity to mitochondria based on [β-MQ]TRL mediated Fenton-like reaction, hijacking tumorigenic energy sources and leading to mitochondrial dysfunction. Additionally, the mild thermal ablation enabled by [β-MQ]TRL further amplifies this cascade reaction to effectively prevent tumor metastasis and recurrence. This synchronous intervention strategy with MRI/PAI establishes unprecedented efficiency in antitumor bioenergetic therapy in vivo, which shows excellent promise for clinical application. 展开更多
关键词 metabolism programming nicotinamide adenine dinucleotide(nad+/nadh)pools homeostasis disruption mitochondrial-targeting cascade therapy magnetic resonance imaging(MRI)/photoacoustic imaging(PAI)
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芯片毛细管电泳检测痕量酶活性的初步探讨
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作者 丛辉 王惠民 +3 位作者 鞠少卿 金庆辉 贾春平 宋宏伟 《生物化学与生物物理进展》 SCIE CAS CSCD 北大核心 2009年第4期512-516,共5页
微芯片技术是基于微机电加工技术(MEMS)工艺,在芯片上完成电泳检测过程的新型技术.利用自制的微流控芯片及激光诱导荧光系统建立了痕量乳酸脱氢酶(LDH)活性的检测方法.以pH9.4,75mmol/L硼酸为芯片电泳缓冲液,9.73μmol/L乳酸钙为添加剂... 微芯片技术是基于微机电加工技术(MEMS)工艺,在芯片上完成电泳检测过程的新型技术.利用自制的微流控芯片及激光诱导荧光系统建立了痕量乳酸脱氢酶(LDH)活性的检测方法.以pH9.4,75mmol/L硼酸为芯片电泳缓冲液,9.73μmol/L乳酸钙为添加剂,整个电泳过程4min结束,利用该法测得LDH检测限(S/N=3)为6×10-3U/L,出峰时间和峰面积的相对标准偏差分别为5.32%和3.17%,该法操作过程简单,检测灵敏度高,在临床痕量酶检测中具有较好的应用前景. 展开更多
关键词 芯片毛细管电泳 氧化型辅酶Ⅰ 还原型辅酶Ⅰ 乳酸脱氢酶
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