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A novel rat model of extremity trauma for prehospital pain management research

机译:一种新型痛苦疼痛管理研究的肢体创伤大鼠模型

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Pain management is important in prehospital care of patients with extremity trauma (ET). The goal of this study was to establish a rat model of ET for prehospital pain research and validate it using pain behaviors and analgesics.Rats were anesthetized using isoflurane, and ETwas induced in one hindlimb via clamping retrofemoral tissues for 30 seconds, followed by closed fibula fracture. Rats regained consciousness after ET. Pain responses in the injured hindlimb to thermal hyperalgesia (paw withdrawal latency [PWL]), mechanical allodynia (paw withdrawal pressure [PWP]), and weight bearing (WB) were determined before and 90 minutes after ET. Morphine (2 mg/kg), fentanyl (10 ug/kg), sufentanil (1 ug/kg), ketamine (5 mg/kg), or vehicle (saline) were then administered via intravenous (i.v.) injection, followed by PWL, PWP, and WB assessments at 10 minutes, 40 minutes, 80 minutes, and 120 minutes after analgesia.After ET, PWL, PWP, and WB were significantly decreased by 61 ± 4%, 64 ± 8%, and 65 ± 4%, respectively, compared with pre-ET values. These pain behaviors were maintained for 3 hours to 4 hours. Compared with the saline group, opioid analgesics significantly increased PWL for at least 80 minutes, with sufentanil exhibiting the highest analgesic effect. An increase in PWL was only observed at 10 minutes after ketamine. The PWP was transiently increased with opioid analgesics for 10 minutes to 40 minutes, but was not changed with ketamine. Weight bearing was improved with opioid analgesics for at least 2 hours, but only for up to 80 minutes with ketamine. Our ET model includes long bone fracture and soft tissue injury, but no fixation surgery, mimicking prehospital ET. Our model produces acute, steady, and reproducible trauma-related pain behaviors, and is clinically relevant regarding the pain behaviors and established responses to common analgesics. e
机译:疼痛管理在肢体创伤患者(ET)的患者中是重要的。本研究的目标是建立ET的RAT模型ET用于预孢子疼痛研究,并使用疼痛行为和镇痛药进行验证。使用异氟烷麻醉,并通过夹紧再生组织在一个后肢诱导的ETWAS诱导30秒,然后闭合腓骨断裂。大鼠在等之后恢复了意识。受伤后肢疼痛反应热痛觉(爪子取出潜伏期[PWL]),机械异常(爪子取出压力[PWP])和重量轴承(爪子戒断压力[PWP])和重量轴承(WB)以后90分钟。然后通过静脉内注射施用吗啡(10μg/ kg),芬太尼(10ug / kg),芬坦基(10μg/ kg),氯胺胺(5mg / kg)或载体(盐水),然后用pwl施用,PWP和WB评估在10分钟,40分钟,80分钟和120分钟后镇痛后120分钟,PWL,PWP和WB显着降低61±4%,64±8%和65±4%分别与ET值相比。将这些疼痛行为保持在3小时至4小时。与盐水组相比,阿片类镇痛药显着增加了PWL至少80分钟,苏芬太尼表现出最高的镇痛作用。仅在氯胺酮后10分钟观察到PWL的增加。通过阿片类镇痛药瞬时增加PWP 10分钟至40分钟,但不含氯胺酮。用阿片类药物镇痛药改善重量轴承至少2小时,但只有在氯胺酮中最长可达80分钟。我们的ET模型包括长骨骨折和软组织损伤,但没有固定手术,模仿预科疗法等。我们的模型产生急性,稳定和可重复的创伤相关的疼痛行为,并且在疼痛行为和对常见镇痛药的响应临床相关的临床相关。 E.

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