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与术前大剂量阿芬太尼相关的迟发性超前镇痛。

Late-onset preemptive analgesia associated with preincisional large-dose alfentanil.

作者信息

Griffin M J, Hughes D, Knaggs A, Donnelly M B, Boylan J F

机构信息

Department of Anaesthesia and Intensive Care, Meath Hospital, Dublin, Ireland.

出版信息

Anesth Analg. 1997 Dec;85(6):1317-21. doi: 10.1097/00000539-199712000-00025.

Abstract

UNLABELLED

Few studies using systemic opioids have been adequately designed to demonstrate a preemptive effect. We investigated the preemptive effect of intraoperative large-dose intravenous (I.V.) opioids over a 72-h period after lower abdominal surgery. Thirty-eight ASA physical status I or II patients undergoing abdominal hysterectomy were studied in a prospective, randomized, double-blind design. Group PRE received alfentanil 70 microg/kg over 10 min before surgical incision; Group POST received alfentanil 70 microg/kg over 10 min after incision. Patients received no other intraoperative opioid. Pain was treated in the recovery room with 2-mg I.V. boluses of morphine and was subsequently managed via patient-controlled analgesia (PCA) using morphine sulfate. Visual analog scale pain scores at rest (VAS-R) and on movement (VAS-M) and PCA morphine consumption were recorded for 72 hours. VAS-M and VAS-R scores did not differ at any point, and morphine consumption was similar in both groups over the initial 48 h. Group PRE used significantly less morphine from 48 to 72 h postoperatively (P < 0.02). We conclude that presurgical incisional (i.e., compared with postincisional) large-dose opioid exposure results in a modest, late decrease in postoperative morphine consumption, with no clinical impact on early postoperative pain. Timing of the observed reduction coincides with maximal output of substances implicated in experimental hyperalgesia.

IMPLICATIONS

When given before surgical incision, alfentanil, a short-acting narcotic, was associated with a reduction in morphine requirements 48-72 h after surgery. Brief interventions may have a delayed and sustained impact on pain perception, possibly by reducing mechanisms of sensitization.

摘要

未标记

很少有使用全身性阿片类药物的研究进行了充分设计以证明超前镇痛效果。我们研究了下腹部手术后72小时内术中大剂量静脉注射阿片类药物的超前镇痛效果。采用前瞻性、随机、双盲设计对38例美国麻醉医师协会(ASA)身体状况为I或II级且接受腹部子宫切除术的患者进行了研究。超前组(PRE组)在手术切口前10分钟内静脉注射阿芬太尼70微克/千克;术后组(POST组)在切口后10分钟内静脉注射阿芬太尼70微克/千克。患者术中未使用其他阿片类药物。在恢复室,疼痛通过静脉注射2毫克吗啡推注进行治疗,随后通过使用硫酸吗啡的患者自控镇痛(PCA)进行管理。记录静息时视觉模拟量表疼痛评分(VAS-R)、活动时视觉模拟量表疼痛评分(VAS-M)以及PCA吗啡消耗量,记录时间为72小时。在任何时间点,VAS-M和VAS-R评分均无差异,且两组在最初48小时内的吗啡消耗量相似。PRE组在术后48至72小时使用的吗啡明显较少(P < 0.02)。我们得出结论,术前切开时(即与术后切开相比)大剂量阿片类药物暴露导致术后吗啡消耗量适度、后期减少,对术后早期疼痛无临床影响。观察到的减少时间与实验性痛觉过敏相关物质的最大释放时间一致。

启示

术前切开时给予短效麻醉剂阿芬太尼与术后48 - 72小时吗啡需求量减少有关。短暂干预可能对疼痛感知有延迟且持续的影响,可能是通过减少敏化机制实现的。

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