首页> 外文期刊>Anesthesiology >QX-314 produces long-lasting local anesthesia modulated by transient receptor potential vanilloid receptors in mice.
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QX-314 produces long-lasting local anesthesia modulated by transient receptor potential vanilloid receptors in mice.

机译:QX-314在小鼠中产生由瞬态受体电位香草酸受体调节的持久局麻。

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BACKGROUND: The quaternary lidocaine derivative QX-314 is now known to produce long-lasting local anesthesia despite its positive charge. However, recent research suggests that the transient receptor potential vanilloid receptor agonist, capsaicin, should reduce the onset and offset times, whereas the transient receptor potential vanilloid receptor antagonist, capsazepine, should delay the onset time of sensory blockade by QX-314. METHODS: Sensory blockade in the tail of the conscious mouse was investigated using QX-314 2.5% in combination with capsaicin 0.1% and/or capsazepine (50 microg/ml). After tail injection, onset and offset times of local anesthesia were measured using the hot water tail-flick latency test. RESULTS: Capsaicin reduced the onset time of local anesthesia by QX-314 by more than 75% (Mann-Whitney test, P = 0.007; n = 10 per group) with no effect on the offset time of QX-314. For QX-314 without capsaicin, the onset and offset times were 23 min (interquartile range 15-30 min) and 300 min (interquartile range 285-375 min), respectively. For QX-314 with capsaicin, the onset and offset times were 4 min (interquartile range 3-8 min) and 360 min (interquartile range 285-435 min), respectively. In the antagonist study, capsazepine without added capsaicin decreased QX-314's efficacy, as 6 out of 9 mice did not develop sensory blockade after 90 min (Fisher exact test, P = 0.009). CONCLUSION: We have confirmed in a sensory blockade model that QX-314 is a local anesthetic with a slow onset and a long duration of reversible blockade. Capsaicin, a transient receptor potential vanilloid receptor agonist, accelerated QX-314's onset kinetics, whereas capsazepine, a transient receptor potential vanilloid receptor antagonist, decreased QX-314's efficacy. These observations raise the possibility that endovanilloids may modulate cell entry of QX-314.
机译:背景:尽管已知利多卡因季铵衍生物QX-314带正电荷,但仍可产生持久的局部麻醉。但是,最近的研究表明,短暂受体电位类香草素受体激动剂辣椒素应减少​​起效和抵消时间,而短暂受体电位类香草素受体拮抗剂Capsazepine应延迟QX-314感官阻滞的发作时间。方法:使用2.5%的QX-314与0.1%的辣椒素和/或50毫克/毫升的辣椒素联合研究清醒小鼠尾部的感觉阻滞。尾巴注射后,使用热水甩尾潜伏期试验测量局部麻醉的开始和偏移时间。结果:辣椒素使QX-314的局部麻醉发作时间缩短了75%以上(Mann-Whitney试验,P = 0.007;每组n = 10),而对QX-314的抵消时间没有影响。对于没有辣椒素的QX-314,其起效时间和偏移时间分别为23分钟(四分位间距15-30分钟)和300分钟(四分位间距285-375分钟)。对于具有辣椒素的QX-314,其起效时间和偏移时间分别为4分钟(四分位间距3-8分钟)和360分钟(四分位间距285-435分钟)。在拮抗剂研究中,不添加辣椒素的辣椒素会降低QX-314的疗效,因为9分钟中的6只小鼠在90分钟后未出现感觉阻滞(Fisher精确检验,P = 0.009)。结论:我们已经在感觉阻滞模型中证实QX-314是一种局麻药,起效缓慢,可逆性阻滞持续时间长。辣椒素是一种短暂的受体潜在的香草受体激动剂,可加速QX-314的发作动力学,而辣椒素(一种短暂的受体潜在的香草受体拮抗剂)可降低QX-314的疗效。这些观察结果提高了内皮素可能调节QX-314细胞进入的可能性。

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