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固定比例为 20:1 的 cafeedrine/去甲肾上腺素通过兰尼碱受体介导的钙释放增加人气管上皮细胞胞浆内钙离子浓度。

A fixed 20:1 combination of cafedrine/theodrenaline increases cytosolic Ca concentration in human tracheal epithelial cells via ryanodine receptor-mediated Ca release.

机构信息

Department of Anesthesiology, Operative Intensive Care Medicine and Pain Therapy, Justus Liebig University of Giessen, Rudolf-Buchheim-Strasse 7, 35392, Giessen, Germany.

Department of General and Thoracic Surgery, Justus Liebig University of Giessen, Rudolf-Buchheim-Strasse 7, 35392, Giessen, Germany.

出版信息

Sci Rep. 2023 Sep 27;13(1):16216. doi: 10.1038/s41598-023-43342-0.

Abstract

Mucociliary clearance is a pivotal physiological mechanism that protects the lung by cleaning the airways from pollution and colonization, thereby preventing infection. Ciliary function is influenced by various signal transduction cascades, and Ca represents a key second messenger. A fixed 20:1 combination of cafedrine and theodrenaline has been widely used to treat perioperative hypotension and emergency hypotensive states since the 1960s; however, its effect on the intracellular Ca concentration ([Ca]) of respiratory epithelium remains unknown. Therefore, human tracheal epithelial cells were exposed to the clinically applied 20:1 mixture of cafedrine/theodrenaline and the individual substances separately. [Ca] was assessed by FURA-2 340/380 fluorescence ratio. Pharmacological inhibitors were applied to elucidate relevant signal transduction cascades, and reverse transcription polymerase chain reaction (RT-PCR) was performed on murine tracheal epithelium to analyze ryanodine receptor (RyR) subtype expression. All three pharmacological preparations instantaneously induced a steep increase in [Ca] that quickly returned to its baseline value despite the persistence of each substance. Peak [Ca] following the administration of 20:1 cafedrine/theodrenaline, cafedrine alone, and theodrenaline alone increased in a dose-dependent manner, with median effective concentrations of 0.35 mM (7.32 mM cafedrine and 0.35 mM theodrenaline), 3.14 mM, and 3.45 mM, respectively. When extracellular Ca influx was inhibited using a Ca-free buffer solution, the peak [Ca] following the administration of cafedrine alone and theodrenaline alone were reduced but not abolished. No alteration in [Ca] compared with baseline [Ca] was observed during β-adrenergic receptor inhibition. Depletion of caffeine-sensitive stores and inhibition of RyR, but not IP receptors, completely abolished any increase in [Ca]. However, [Ca] still increased following the depletion of mitochondrial Ca stores using 2,4-dinitrophenol. RT-PCR revealed RyR-2 and RyR-3 expression on murine tracheal epithelium. Although our experiments showed that cafedrine/theodrenaline, cafedrine alone, or theodrenaline alone release Ca from intracellular stores through mechanisms that are exclusively triggered by β-adrenergic receptor stimulation, which most probably lead to RyR activation, clinical plasma concentrations are considerably lower than those used in our experiments to elicit an increase in [Ca]; therefore, further studies are needed to evaluate the ability of cafedrine/theodrenaline to alter mucociliary clearance in clinical practice.

摘要

黏液纤毛清除是一种重要的生理机制,通过清除气道中的污染物和定植物来保护肺部,从而预防感染。纤毛功能受多种信号转导级联的影响,而 Ca 是关键的第二信使。自 20 世纪 60 年代以来,固定的 20:1 比例的咖啡因和去甲肾上腺素组合已被广泛用于治疗围手术期低血压和紧急低血压状态;然而,其对呼吸上皮细胞内 Ca 浓度 ([Ca]) 的影响尚不清楚。因此,分别用临床应用的 20:1 比例的咖啡因/去甲肾上腺素混合物和单独的物质暴露于人气管上皮细胞。通过 FURA-2 340/380 荧光比评估 [Ca]。应用药理学抑制剂来阐明相关的信号转导级联,并用逆转录聚合酶链反应 (RT-PCR) 分析鼠气管上皮细胞中的 Ryanodine 受体 (RyR) 亚型表达。所有三种药理学制剂都立即引起 [Ca]的急剧增加,尽管每种物质持续存在,但 [Ca]很快恢复到基线值。给予 20:1 咖啡因/去甲肾上腺素、咖啡因和去甲肾上腺素后,[Ca]的峰值呈剂量依赖性增加,其半数有效浓度分别为 0.35 mM(7.32 mM 咖啡因和 0.35 mM 去甲肾上腺素)、3.14 mM 和 3.45 mM。当用无钙缓冲液抑制细胞外 Ca 内流时,给予咖啡因单独和去甲肾上腺素单独后 [Ca]的峰值降低,但未被消除。β-肾上腺素能受体抑制时,与基础 [Ca]相比,[Ca]没有变化。耗尽咖啡因敏感的储存库并抑制 RyR,但不抑制 IP 受体,完全消除了 [Ca]的任何增加。然而,用 2,4-二硝基苯酚耗尽线粒体 Ca 储存后,[Ca]仍会增加。RT-PCR 显示鼠气管上皮细胞表达 RyR-2 和 RyR-3。尽管我们的实验表明,咖啡因/去甲肾上腺素、咖啡因或去甲肾上腺素通过仅由 β-肾上腺素能受体刺激触发的机制从细胞内储存库释放 Ca,这很可能导致 RyR 激活,但临床血浆浓度明显低于我们实验中引起 [Ca]增加的浓度;因此,需要进一步研究来评估咖啡因/去甲肾上腺素改变临床实践中黏液纤毛清除的能力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a15/10533847/633358ed8c33/41598_2023_43342_Fig1_HTML.jpg

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