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功能坐骨神经阻滞持续时间与控释基质中利多卡因释放速率的关系。

The relationship between functional sciatic nerve block duration and the rate of release of lidocaine from a controlled-release matrix.

机构信息

Brigham and Women's Hospital, MRB-611, 75 Francis St., Boston, MA 02115-6110, USA.

出版信息

Anesth Analg. 2010 Jul;111(1):221-9. doi: 10.1213/ANE.0b013e3181dd2690. Epub 2010 Jun 3.

Abstract

BACKGROUND

Nerve blocks of long duration are often desirable in perioperative and postoperative situations. The relationship between the duration of such blocks and the rate at which a local anesthetic is released is important to know for developing a localized drug delivery system that will optimize block duration.

METHODS

Lidocaine concentration was varied in 1 series of formulations (OSB-L) containing a constant amount of release rate modifier. In another series (OST-R), the release rate modifier was varied while the lidocaine content was held constant. Release kinetics were measured in vitro and correlated to the in vivo duration of antinociceptive and motor block effects when the formulation was implanted next to the rat sciatic nerve. In parallel studies, rats receiving different formulations of slow-release lidocaine were fixed by intracardiac perfusion with 4% paraformaldehyde and nerve-muscle tissue taken for histopathological analysis.

RESULTS

In this study, we have demonstrated that the most important variable for effecting functional nerve block, i.e., the blockade of impulses in the relevant fibers of the sciatic nerve, is the rate of lidocaine release at that time. For the OSB-L formulations (lidocaine concentrations of 1.875%, 3.75%, 7.5%, and 15% at a constant release rate modifier of 5%), the average in vitro release rates at 50% recovery of motor block and nociceptive block were 0.91 +/- 0.28 and 1.75 +/- 0.61 mg/h, respectively. For the OST-R formulations (16% lidocaine with release rate modifier concentrations of 1.875%, 3.75%, 7.5%, and 15%), the average in vitro release rates at 50% recovery of motor block and nociceptive block were 2.33 +/- 1.39 and 4.34 +/- 1.09 mg/h, respectively. The OSB-L formulations showed a dose-dependent increase in block duration proportional to an increase in initial lidocaine concentration, whereas the OST-R formulations showed a nonmonotonic relationship between release rate modifier concentration and block duration. The histopathological studies at 24 hours, 3, 5, or 7 days, and 4 weeks after the implantation revealed inflammatory reactions with degrees correlated with lidocaine content, but limited to the connective tissue and muscle immediately surrounding the implanted material. Despite these observed inflammatory reactions, nociceptive and motor block function returned to normal, preimplantation values in all animals.

CONCLUSIONS

Increasing initial lidocaine content proportionately increased the duration of functional sciatic nerve block. However, decreasing the release rate per se does not give a proportional increase in block duration. Instead, there seems to be an optimal, intermediate release rate for achieving the maximum duration of block.

摘要

背景

在围手术期和术后情况下,长时间的神经阻滞往往是理想的。了解这种阻滞的持续时间与局部麻醉剂释放速度之间的关系对于开发优化阻滞持续时间的局部药物递送系统非常重要。

方法

在含有恒定释放速率调节剂的一系列配方(OSB-L)中改变利多卡因浓度。在另一个系列(OST-R)中,改变释放速率调节剂,同时保持利多卡因含量不变。在体外测量释放动力学,并将其与制剂植入大鼠坐骨神经旁时的抗伤害和运动阻滞作用的体内持续时间相关联。在平行研究中,通过心脏内灌注 4%多聚甲醛固定接受不同缓慢释放利多卡因配方的大鼠,并取出神经-肌肉组织进行组织病理学分析。

结果

在这项研究中,我们已经证明,影响功能神经阻滞的最重要变量,即坐骨神经相关纤维中冲动的阻滞,是当时利多卡因释放的速度。对于 OSB-L 配方(释放速率调节剂浓度为 5%时,利多卡因浓度为 1.875%、3.75%、7.5%和 15%),在运动阻滞和痛觉阻滞恢复 50%时的平均体外释放率分别为 0.91 +/- 0.28 和 1.75 +/- 0.61 mg/h。对于 OST-R 配方(16%利多卡因,释放速率调节剂浓度为 1.875%、3.75%、7.5%和 15%),在运动阻滞和痛觉阻滞恢复 50%时的平均体外释放率分别为 2.33 +/- 1.39 和 4.34 +/- 1.09 mg/h。OSB-L 配方显示阻滞持续时间与初始利多卡因浓度呈剂量依赖性增加,而 OST-R 配方显示阻滞持续时间与释放速率调节剂浓度之间呈非单调关系。在植入后 24 小时、3、5 或 7 天和 4 周的组织病理学研究显示,炎症反应的程度与利多卡因含量相关,但仅限于植入材料周围的结缔组织和肌肉。尽管存在这些观察到的炎症反应,但所有动物的痛觉和运动阻滞功能均恢复到植入前的正常水平。

结论

增加初始利多卡因含量会成比例地增加功能性坐骨神经阻滞的持续时间。然而,降低释放速率本身并不能使阻滞持续时间成比例增加。相反,似乎存在一个最佳的、中间的释放速率,可以实现阻滞持续时间的最大化。

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