Reducing of the respiratory effects of dizocilpine by recombinant interleukin-1β in experiment

T. Tumanova, Vladimir A. Merkurjev, G. Danilova, V. Aleksandrov
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Abstract

BACKGROUND: For a deeper understanding of the pathogenesis of COVID-19, it is necessary to study the mechanisms that implement the influence of pro-inflammatory cytokines on the processes of regulation of the external respiratory system. In experiments on anesthetized rats, the effect of the pro-inflammatory cytokine interleukin-1 on the respiratory effects of dizocilpine (MK-801), which has an inhibitory effect on neurotransmitter systems involved in the control of the respiratory system, was studied. It was considered that, first of all, dizocilpine is a highly effective non-competitive NMDA-type glutamate receptor blocker. AIM: The objectives of the study were to identify the effect of the influence of dizocilpine on the parameters of the breathing pattern and to assess the degree of change in this effect when dizocilpine was administered against the background of an elevated systemic level of interleukin-1. MATERIALS AND METHODS: The study was performed on 24 anesthetized tracheostomy spontaneously breathing rats. To register the volume-time parameters of external respiration, a pneumotachographic technique was used. In the process of processing the obtained results, the value of the recorded parameter was determined immediately before the introduction of MK-801 and 1 min after its introduction RESULTS: At a dosage of 0.1 mg/kg, dizocilpine was found to cause a reversible short-term decrease in respiratory rate, tidal volume, and minute respiratory volume. It has been shown that this effect of dizocilpine does not appear after intravenous administration of interleukin-1 (at a dosage of 2 g/kg). The results obtained confirm the assumption about the effect of an elevated systemic level of interleukin-1 on the state of neurotransmitter systems involved in the control of respiration. CONCLUSIONS: Based on the correlation of the obtained results with the literature data, an assumption was made about a change in the state of NMDA-type glutamate receptors under the influence of pro-inflammatory cytokines, which may be one of the mechanisms of cardiorespiratory dysfunctions observed in a systemic inflammatory reaction accompanied by hypercytokinemia.
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重组白细胞介素-1β降低二唑西平呼吸作用的实验研究
背景:为了更深入地了解COVID-19的发病机制,有必要研究促炎细胞因子对外呼吸系统调节过程的影响机制。在麻醉大鼠实验中,研究了促炎细胞因子白细胞介素-1对二唑西平(MK-801)呼吸作用的影响,二唑西平对参与呼吸系统控制的神经递质系统有抑制作用。认为,首先,二唑西平是一种高效的非竞争性nmda型谷氨酸受体阻滞剂。目的:本研究的目的是确定二唑西平对呼吸模式参数的影响,并评估在全身白细胞介素-1水平升高的背景下给予二唑西平时这种影响的变化程度。材料与方法:采用24只气管切开术麻醉自主呼吸大鼠进行实验。为了记录体外呼吸的体积-时间参数,使用了气相摄影技术。在处理所得结果的过程中,分别在MK-801引入前和引入后1分钟测定记录参数的值。结果:0.1 mg/kg的剂量下,二唑西平可引起呼吸频率、潮气量和分钟呼吸量的可逆性短期降低。研究表明,静脉注射白细胞介素-1(剂量为2g /kg)后,二唑西平的这种作用不会出现。所获得的结果证实了关于白细胞介素-1系统水平升高对参与呼吸控制的神经递质系统状态的影响的假设。结论:基于所得结果与文献数据的相关性,我们假设nmda型谷氨酸受体在促炎细胞因子的影响下状态发生变化,这可能是全身性炎症反应伴高细胞因子血症时出现心肺功能障碍的机制之一。
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