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多效酶:多效性氧化碳纳米酶增强细胞代谢灵活性。

Pleozymes: Pleiotropic Oxidized Carbon Nanozymes Enhance Cellular Metabolic Flexibility.

作者信息

Vo Anh T T, Mouli Karthik, Liopo Anton V, Lorenzi Philip, Tan Lin, Wei Bo, Martinez Sara A, McHugh Emily A, Tour James M, Khan Uffaf, Derry Paul J, Kent Thomas A

机构信息

Center for Genomics and Precision Medicine, Institute of Bioscience and Technology, Texas A&M Health Science Center, Houston, TX 77030, USA.

Department of Chemistry, Rice University, Houston, TX 77005, USA.

出版信息

Nanomaterials (Basel). 2024 Dec 15;14(24):2017. doi: 10.3390/nano14242017.

Abstract

Our group has synthesized a pleiotropic synthetic nanozyme redox mediator we term a "pleozyme" that displays multiple enzymatic characteristics, including acting as a superoxide dismutase mimetic, oxidizing NADH to NAD, and oxidizing HS to polysulfides and thiosulfate. Benefits have been seen in acute and chronic neurological disease models. The molecule is sourced from coconut-derived activated charcoal that has undergone harsh oxidization with fuming nitric acid, which alters the structure and chemical characteristics, yielding 3-8 nm discs with broad redox potential. Prior work showed pleozymes localize to mitochondria and increase oxidative phosphorylation and glycolysis. Here, we measured cellular NAD and NADH levels after pleozyme treatment and observed increased total cellular NADH levels but not total NAD levels. A C-glucose metabolic flux analysis suggested pleozymes stimulate the generation of pyruvate and lactate glycolytically and from the tricarboxylic acid (TCA) cycle, pointing to malate decarboxylation. Analysis of intracellular fatty acid abundances suggests pleozymes increased fatty acid β-oxidation, with a concomitant increase in succinyl- and acetyl-CoA. Pleozymes increased total ATP, potentially via flexible enhancement of NAD-dependent catabolic pathways such as glycolysis, fatty acid β-oxidation, and metabolic flux through the TCA cycle. These effects may be favorable for pathologies that compromise metabolism such as brain injury.

摘要

我们的团队合成了一种具有多效性的合成纳米酶氧化还原介质,我们将其称为“多酶”,它具有多种酶促特性,包括作为超氧化物歧化酶模拟物、将NADH氧化为NAD,以及将HS氧化为多硫化物和硫代硫酸盐。在急性和慢性神经疾病模型中已观察到其益处。该分子来源于经过发烟硝酸剧烈氧化的椰子衍生活性炭,这种氧化改变了其结构和化学特性,产生了具有宽氧化还原电位的3-8纳米圆盘。先前的研究表明多酶定位于线粒体并增加氧化磷酸化和糖酵解。在此,我们在多酶处理后测量了细胞内NAD和NADH水平,观察到细胞内总NADH水平增加,但总NAD水平未增加。C-葡萄糖代谢通量分析表明,多酶通过糖酵解以及从三羧酸(TCA)循环刺激丙酮酸和乳酸的生成,表明存在苹果酸脱羧作用。细胞内脂肪酸丰度分析表明,多酶增加了脂肪酸β-氧化,同时琥珀酰辅酶A和乙酰辅酶A也增加。多酶增加了总ATP,可能是通过灵活增强依赖NAD的分解代谢途径,如糖酵解、脂肪酸β-氧化以及通过TCA循环的代谢通量。这些作用可能对诸如脑损伤等损害代谢的病症有利。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2e40/11728746/39d10ea14400/nanomaterials-14-02017-g001.jpg

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