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运动调理血浆的给予改变了大鼠肌肉过氧化氢酶动力学:体内样 K 而不是体外样 V 的论据。

Administration of exercise-conditioned plasma alters muscle catalase kinetics in rat: An argument for in vivo-like K instead of in vitro-like V.

机构信息

Department of Biochemistry and Biotechnology, University of Thessaly, Viopolis, Mezourlo, 41500, Larissa, Greece; Department of Physical Education and Sports Science at Serres, Aristotle University of Thessaloniki, Serres, Greece.

School of Physical Education and Sport Science, National and Kapodistrian University of Athens, Ethnikis Antistasis 41, 17237, Athens, Greece; Department of Health Sciences, School of Sciences, European University Cyprus, Nicosia, Cyprus.

出版信息

Redox Biol. 2018 May;15:375-379. doi: 10.1016/j.redox.2018.01.001. Epub 2018 Jan 3.

Abstract

Maximal velocity (V) is a well established biomarker for the assessment of tissue redox status. There is scarce evidence, though, that it does not probably reflect sufficiently in vivo tissue redox profile. Instead, the Michaelis constant (K) could more adequately image tissue oxidative stress and, thus, be a more physiologically relevant redox biomarker. Therefore, the aim of the present study was to side-by-side compare V and K of an antioxidant enzyme after implementing an in vivo set up that induces alterations in tissue redox status. Forty rats were divided into two groups including rats injected with blood plasma originating from rats that had previously swam until exhaustion and rats injected with blood plasma originating from sedentary rats. Tail-vein injections were performed daily for 21 days. Catalase V and K measured in gastrocnemius muscle were increased after administration of the exercise-conditioned plasma, denoting enhancement of the enzyme activity but impairment of its affinity for the substrate, respectively. These alterations are potential adaptations stimulated by the administered plasma pointing out that blood is an active fluid capable of regulating tissue homeostasis. Our findings suggest that K adequately reflects in vivo modifications of skeletal muscle catalase and seems to surpass V regarding its physiological relevance and biological interpretation. In conclusion, K can be regarded as an in vivo-like biomarker that satisfactorily images the intracellular environment, as compared to V that could be aptly parallelized with a biomarker that describes tissue oxidative stress in an in vitro manner.

摘要

最大速度 (V) 是评估组织氧化还原状态的一种既定生物标志物。然而,几乎没有证据表明它不能充分反映体内组织氧化还原谱。相反,米氏常数 (K) 可能更能反映组织氧化应激,因此是一种更具生理相关性的氧化还原生物标志物。因此,本研究的目的是在建立一种可诱导组织氧化还原状态改变的体内模型后,对抗氧化酶的 V 和 K 进行并排比较。40 只大鼠被分为两组,一组注射来自先前游泳至力竭的大鼠的血浆,另一组注射来自安静大鼠的血浆。尾静脉注射每天进行 21 天。在给予运动条件血浆后,比目鱼肌中测定的过氧化氢酶 V 和 K 增加,分别表示酶活性增强,但对底物的亲和力受损。这些变化是由给予的血浆刺激的潜在适应性,表明血液是一种能够调节组织内稳态的活性流体。我们的发现表明,K 能充分反映体内骨骼肌过氧化氢酶的变化,并且与 V 相比,其在生理相关性和生物学解释方面具有优势。总之,K 可以被视为一种类似于体内的生物标志物,能够很好地描绘细胞内环境,而 V 则可以与描述组织在体外氧化应激的生物标志物相媲美。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/78f7/5766480/21f37da523b7/gr1.jpg

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