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一氧化氮合酶-1在快肌氧化型肌纤维中含量丰富。

Nitric oxide synthase-1 is enriched in fast-twitch oxidative myofibers.

作者信息

Planitzer G, Miethke A, Baum O

机构信息

Institute of Anatomy, Universitätsklinikum Benjamin Franklin, Freie Universität Berlin, Königin-Luise-Str. 15, 14195 Berlin-Dahlem, Germany.

出版信息

Cell Tissue Res. 2001 Nov;306(2):325-33. doi: 10.1007/s004410100449.

Abstract

Nitric oxide synthase-1 (NOS-1) is found in high concentrations in skeletal muscles, where its synthesis product nitric oxide (NO) is reported to be involved in a number of processes, including the modulation of the oxidative metabolism of myofibers. Performing immunoblot analysis and quantification of formazan produced by its specific NADPH diaphorase activity, we found NOS-1 to be enriched in rat skeletal muscles with a high proportion of fast-twitch myofibers. Since these myofibers represent a metabolically heterogeneous subpopulation, we extended our investigation to the level of individual myofibers. Using serial sections we combined myosin heavy chain-based fiber-typing with quantitative succinate dehydrogenase histochemistry to determine three groups of fiber-types, comprising fast-oxidative, fast-glycolytic and slow-oxidative myofibers. Image analysis showed that NOS-1 diaphorase activity is significantly enriched in fast-oxidative myofibers compared with fast-glycolytic and slow-oxidative ones. In order to characterize potential biological effects of the fiber-type-specific enrichment of NOS-1, we performed cytochrome oxidase histochemistry in the presence of the NO donors NOC-9 and SNAP. Both NO donors reduced cytochrome oxidase activity in all myofibers investigated with almost identical semi-maximal inhibition rates, although fast-oxidative and slow-oxidative myofibers contained twice as much basal catalytic activity than fast-glycolytic ones. In summary, we suggest that the NOS-1/NO system of skeletal muscles exerts its biological role especially in fast-oxidative myofibers, since these myofibers express more NOS-1 than fast-glycolytic or slow-oxidative ones and also contain the highest concentrations of cytochrome oxidases as potential target molecules of NO.

摘要

一氧化氮合酶-1(NOS-1)在骨骼肌中含量很高,据报道其合成产物一氧化氮(NO)参与了许多过程,包括对肌纤维氧化代谢的调节。通过免疫印迹分析及其特异性NADPH黄递酶活性产生的甲臜进行定量,我们发现NOS-1在快肌纤维比例高的大鼠骨骼肌中富集。由于这些肌纤维代表代谢异质性亚群,我们将研究扩展到单个肌纤维水平。使用连续切片,我们将基于肌球蛋白重链的纤维分型与定量琥珀酸脱氢酶组织化学相结合,以确定三组纤维类型,包括快氧化型、快糖酵解型和慢氧化型肌纤维。图像分析表明,与快糖酵解型和慢氧化型肌纤维相比,NOS-1黄递酶活性在快氧化型肌纤维中显著富集。为了表征NOS-1纤维类型特异性富集的潜在生物学效应,我们在NO供体NOC-9和SNAP存在的情况下进行了细胞色素氧化酶组织化学。尽管快氧化型和慢氧化型肌纤维的基础催化活性是快糖酵解型肌纤维的两倍,但两种NO供体均以几乎相同的半最大抑制率降低了所有研究肌纤维中的细胞色素氧化酶活性。总之,我们认为骨骼肌的NOS-1/NO系统尤其在快氧化型肌纤维中发挥其生物学作用,因为这些肌纤维比快糖酵解型或慢氧化型肌纤维表达更多的NOS-1,并且还含有作为NO潜在靶分子的最高浓度的细胞色素氧化酶。

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