Tissue oxidative metabolism and microhemodynamics of the skin in rats exposed to stress factors of different duration and their combinations

M. Ravaeva, I. Cheretaev, Elena N. Chuyan, Pavel A. Galenko-Yaroshevskii, E. R. Dzheldubayeva, I. Mironyuk
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Abstract

BACKGROUND: Changes in tissue oxidative metabolism (OM) under the action of stressors of different duration have not been studied. The question of the relationship of NADH and FAD coenzymes with the microcirculatory bed (MCB) remains open. AIM: The work is devoted to identifying the features of the reaction of skin microhemodynamics (MHS) and tissue OM in rats exposed to acute and chronic stress factors of different duration and their combinations. MATERIALS AND METHODS: The experiment was carried out on 100 male rats of the Wistar line weighing 200-220 g. The animals were divided into 5 groups of 20 rats. The 1st control group, the 2nd and 3rd groups were exposed to acute (AS) and chronic hypokinetic stress (HS), respectively; the 4th group (AS-HS) was previously exposed to AS (on the 1st day), and then to HS (1-10 days); 5-th group (for 10 days of the HS, then the impact of the AS on the 10th day). On the 10th day, the indicators of tissue OM and MHS were recorded. RESULTS: It was shown that AS and HS increase the requirement of cells for ATP and contribute to the predominance of oxidative phosphorylation (OPh) over other processes, as indicated by an increase in FAD. AS-HS significantly changes the OM, separating the OPh and activating glycolysis. HS-AS does not cause such changes. AS increases the microcirculation index (MI) and reduces the coefficient of variation (Cv), HS reduces the MI and increases the mean square deviation (MSD). AS-HS significantly increases MI, and HS-AS MSD and Cv, but reduces MI. CONCLUSIONS: AS and HS increase the requirement of cells for ATP and contribute to the predominance of OPh over other processes. AS-HS modifies OM, disconnecting OPh and activating glycolysis. HS-AS depletes the metabolic reserves of the body. AS-HS rearranges metabolism along the path of glycolysis, protecting against stress factors and preventing the development of oxidative stress. AS leads to hyperemia and stasis of blood circulation in the microarray, reducing vasomotor activity of vessels. HS inhibits the level of tissue perfusion, reduces the inflow of arterial blood into the MCB and the outflow of venous blood, leading to spastic, stagnant phenomena and stasis. AS-HS reduces vasoconstriction, preparing the MCB for prolonged hypokinesia. HS-AS levels vasodilation, improves the parameters of MHS (MSD and Cv).
暴露于不同持续时间的应激因素及其组合的大鼠皮肤组织氧化代谢和微血流动力学
背景:在不同持续时间的应激源作用下,组织氧化代谢(OM)的变化尚未得到研究。NADH 和 FAD 辅酶与微循环床(MCB)的关系问题仍未解决。 目的:本研究致力于确定大鼠在不同持续时间的急性和慢性应激因素及其组合作用下皮肤微血流动力学(MHS)和组织 OM 的反应特征。 材料和方法:实验以 100 只体重为 200-220 克的 Wistar 系雄性大鼠为对象。第 1 组为对照组,第 2 组和第 3 组分别暴露于急性(AS)和慢性低运动应激(HS);第 4 组(AS-HS)先暴露于 AS(第 1 天),然后暴露于 HS(1-10 天);第 5 组(HS 10 天,然后在第 10 天暴露于 AS)。第 10 天记录组织 OM 和 MHS 指标。 结果:研究表明,AS 和 HS 增加了细胞对 ATP 的需求,并导致氧化磷酸化(OPh)优先于其他过程,这表现为 FAD 的增加。AS-HS 明显改变了 OM,分离了 OPh 并激活了糖酵解。而 HS-AS 不会引起这种变化。 AS 增加了微循环指数(MI)并降低了变异系数(Cv),HS 减少了 MI 并增加了均方差(MSD)。AS-HS 会明显增加微循环指数,HS-AS 会增加 MSD 和 Cv,但会减少微循环指数。 结论:AS和HS增加了细胞对ATP的需求,并导致OPh优先于其他过程。AS-HS 改变了 OM,切断了 OPh 并激活了糖酵解。HS-AS 会耗尽人体的代谢储备。AS-HS 沿着糖酵解的路径重新安排新陈代谢,抵御应激因素并防止氧化应激的发展。AS 会导致微阵列中血液循环的充血和淤滞,降低血管的运动活性。HS 会抑制组织灌注水平,减少流入 MCB 的动脉血和流出的静脉血,导致痉挛、停滞和瘀血现象。AS-HS 可减少血管收缩,为 MCB 长时间低运动做好准备。HS-AS 可促进血管舒张,改善 MHS 的参数(MSD 和 Cv)。
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