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阿芬太尼:犬鞘内注射后皮下肥大细胞无效应与无肉芽肿形成之间的相关性。

Alfentanil: correlations between absence of effect upon subcutaneous mast cells and absence of granuloma formation after intrathecal infusion in the dog.

作者信息

Yaksh Tony L, Steinauer Joanne J, Veesart Samantha L, Malkmus Shelle A

机构信息

Anesthesiology Research, Department of Anesthesiology, University of California, San Diego, CA, USA.

出版信息

Neuromodulation. 2013 Sep-Oct;16(5):459-66; discussion 466. doi: 10.1111/j.1525-1403.2012.00534.x. Epub 2012 Nov 21.

Abstract

BACKGROUND

We hypothesize that intrathecal (IT) granulomas arising from the IT infusion of several opiates may result from the degranulation of meningeal mast cells (MC). Given functional covariance between cutaneous and meningeal MC, we propose that opioids that do not degranulate cutaneous MC will not produce a granuloma. An opioid meeting this criteria is the phenylpiperadine alfentanil HCl.

METHODS

Three experiments were accomplished in dogs. 1) Cutaneous MC degranulation. Flare areas on the dog abdomen were measured after intradermal alfentanil, morphine, or compound 48-80. 2) Dose ranging of analgesic effects of IT alfentanil infusion. Dogs with lumbar IT catheters received continuous infusion for 24 hours of different concentrations (1-20 mg/mL/d) of alfentanil and analgesic effects were assessed. 3) Granuloma inducing effects. Dogs received IT alfentanil (20 mg/mL/d; N = 5; 22-28 days) or morphine (12 mg/mL/d; N = 3; 22-30 days) and spinal cord harvested for histopathology after 22-30 days of infusion.

RESULTS

  1. Intradermal morphine (10 mg/mL) and compound 48-80 (1 mg/mL) but not alfentanil at concentrations up to 20 mg/mL produced a cutaneous flare. IT alfentanil infusion produced increases in thermal escape latency at concentrations as low as 2 mg/mL/day. A significant depression of arousal was noted in the dogs receiving 20 mg/mL. Over the 22- to 30-day infusion period, morphine (12 mg/mL/day) resulted in granulomas in all three animals examined whereas IT alfentanil at 20 mg/mL/day failed to initiate a granuloma in any animal.

CONCLUSIONS

These results support the hypothesis linking MC degranulation and IT granulomas.

摘要

背景

我们推测,几种阿片类药物鞘内(IT)输注引起的鞘内肉芽肿可能源于脑膜肥大细胞(MC)的脱颗粒。鉴于皮肤和脑膜MC之间存在功能协方差,我们提出,不会使皮肤MC脱颗粒的阿片类药物不会产生肉芽肿。符合这一标准的阿片类药物是苯哌啶阿芬太尼盐酸盐。

方法

在犬身上完成了三项实验。1)皮肤MC脱颗粒。在犬腹部皮内注射阿芬太尼、吗啡或化合物48-80后,测量皮肤潮红面积。2)鞘内输注阿芬太尼的镇痛效果剂量范围研究。将带有腰椎IT导管的犬连续24小时输注不同浓度(1-20mg/mL/天)的阿芬太尼,并评估镇痛效果。3)肉芽肿诱导作用。犬接受鞘内阿芬太尼(20mg/mL/天;N = 5;22-28天)或吗啡(12mg/mL/天;N = 3;22-30天)输注,输注22-30天后取出脊髓进行组织病理学检查。

结果

1)皮内注射10mg/mL的吗啡和1mg/mL的化合物48-80会产生皮肤潮红,但浓度高达20mg/mL的阿芬太尼不会。鞘内输注阿芬太尼,浓度低至2mg/mL/天时即可使热逃避潜伏期延长。接受20mg/mL阿芬太尼的犬出现明显的觉醒抑制。在22至30天的输注期内,12mg/mL/天的吗啡导致所有三只接受检查的动物出现肉芽肿,而20mg/mL/天的鞘内阿芬太尼未在任何动物中引发肉芽肿。

结论

这些结果支持了将MC脱颗粒与鞘内肉芽肿联系起来的假说。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1dc0/3582801/3d0c754e2830/nihms414564f1.jpg

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