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首页> 外文期刊>Critical care medicine >Effects of chronic sepsis on contractile properties of fast twitch muscle in an experimental model of critical illness neuromyopathy in the rat.
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Effects of chronic sepsis on contractile properties of fast twitch muscle in an experimental model of critical illness neuromyopathy in the rat.

机译:慢性脓毒症对大鼠重症神经肌病实验模型中快速抽搐肌肉收缩特性的影响。

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OBJECTIVE: Critical illness polyneuromyopathy has been extensively studied in various animal models regarding electrophysiological aspects or molecular mechanisms involved in its physiopathology; however, little data are available on its main clinical feature, that is, muscular weakness. We have studied the effects of chronic sepsis in rats with special consideration to contractile and neuromuscular blockade properties in relation with the level of messenger RNA (mRNA) coding for ryanodine and acetylcholine receptors. DESIGN: This was an experimental animal study. SETTING: This study was conducted at a university laboratory. SUBJECTS: Subjects consisted of Wistar rats. INTERVENTIONS: Chronic sepsis was achieved by cecal ligation and needle perforation. Ten days after surgery, fast twitch extensor digitorum longus was excised for extraction and assays of mRNA coding for ryanodine and acetylcholine receptor subunits and contralateral muscle was tested in vivo on a mechanical bench. A fatigability index was measured and neuromuscular blockade properties using atracurium were evaluated. MEASUREMENTS AND MAIN RESULTS: A decrease in active force developed by extensor digitorum longus associated with an increase in passive force is induced by chronic sepsis. Maximal force at optimal length during twitch contraction was significantly reduced (0.25 +/- 0.09 N vs. 0.17 +/- 0.06 N); contraction and relaxation speeds were higher as shown by the decrease of respective time constants (3.75 +/- 0.01 msec vs. 2.70 +/- 0.0 msec, 10.76 +/- 0.03 msec vs. 7.62 +/- 0.03 msec) in the control group compared with the septic group. Fatigability index was significantly lower (23 +/- 0.11% vs. 59 +/- 0.19%) in septic rats. These rats also showed quicker blockade and shorter recovery after atracurium administration. Sepsis induced a significant increase of the expression of ryanodine receptor (RyR) RyR1 along with a steady expression of RyR3 mRNA, leading to a 5.6-fold increase of RyR1/RyR3 ratio with a steadiness of mRNA corresponding to acetylcholine-receptors. CONCLUSIONS: Chronic inflammation and sepsis induced a decrease in contractile performances of extensor digitorum longus along with accelerated kinetics of atracurium possibly induced by modified expression of RyR1 receptors and not acetylcholine-receptors.
机译:目的:危重病多发性神经病在各种动物模型中已被广泛研究,涉及其生理病理学的电生理学方面或分子机制。然而,关于其主要临床特征即肌肉无力的资料很少。我们已经研究了慢性脓毒症对大鼠的影响,其中特别考虑了收缩和神经肌肉阻滞特性,以及编码ryanodine和乙酰胆碱受体的信使RNA(mRNA)的水平。设计:这是一项实验动物研究。地点:这项研究是在大学实验室进行的。受试者:受试者由Wistar大鼠组成。干预:通过盲肠结扎和针穿刺实现了慢性败血症。手术十天后,切取长指伸肌抽搐,进行提取,并在机械凳上在体内测试编码莱ano碱和乙酰胆碱受体亚基的mRNA的测定方法以及对侧肌肉。测量疲劳指数并评估使用阿曲库铵的神经肌肉阻滞性能。测量和主要结果:慢性败血症可导致指趾长伸肌产生的主动力降低,而被动力则增加。抽搐收缩过程中最佳长度的最大力明显降低(0.25 +/- 0.09 N对0.17 +/- 0.06 N);对照组的收缩和放松速度较高,如相应时间常数的减少所示(3.75 +/- 0.01毫秒vs. 2.70 +/- 0.0毫秒,10.76 +/- 0.03毫秒vs. 7.62 +/- 0.03毫秒)与败血症组相比。在脓毒症大鼠中,疲劳指数显着降低(23 +/- 0.11%对59 +/- 0.19%)。这些大鼠在阿曲库铵给药后也表现出更快的阻断和更短的恢复。脓毒症诱导RyanR受体RyR1的表达以及RyR3 mRNA的稳定表达显着增加,从而导致RyR1 / RyR3的比例增加5.6倍,而对应于乙酰胆碱受体的mRNA则稳定。结论:慢性炎症和败血症可导致指趾长伸肌收缩性能下降,而RyR1受体而非乙酰胆碱受体表达的改变可能引起阿曲库铵的加速动力学。

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