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芬太尼诱导的啮齿动物呼吸抑制可被生物可吸收的皮下纳曲酮植入物抑制,抑制时间为 3.5 个月。

Fentanyl-induced respiratory depression in rodents is inhibited by bioabsorbable, subcutaneous naltrexone implants at 3.5 months.

机构信息

The Drug Delivery Company, LLC dba Akyso, Salisbury, MD (JDB and SMC), LabCorp Drug Development Greenfield, IN (JAH), The Department of Psychiatry, Johns Hopkins School of Medicine and Maryland Treatment Centers, Baltimore, Maryland, USA.

出版信息

Addict Biol. 2023 Dec;28(12):e13350. doi: 10.1111/adb.13350.

Abstract

The aim of this study is to determine if extended-release, bioabsorbable, subcutaneous naltrexone (NTX) implants inhibit respiratory depression after an IV injection of fentanyl. Bioabsorbable implants fabricated from two different release-controlling polymers, poly-D-L-lactide (PDLLA) and polycaprolactone (PCL), alone (placebo) or containing NTX, were subcutaneously implanted in Sprague Dawley rats. After 3.5 months of implantation, the rodents were administered an IV bolus of fentanyl through the tail vein. The placebo implant rats received a dose of 4 micrograms (mcg) - (10 mcg/kg/dose), while the NTX implanted animals received a dose of 8 mcg (20 mcg/kg/dose). The minimum active dose of fentanyl that caused a > 50 ± 2% depression in the respiration rate in the placebo implanted rodents was 4 mcg. The respiration rate of the placebo implanted rats dropped from 208 ± 14 breaths/minute at predose, to 84 ± 12 breaths/minute (p = 0.0003) at 2 min. In contrast, all NTX implanted animals easily tolerated twice the dose of 8 mcg of fentanyl without any significant reduction in respiration rate. The mean respiration rate = increased from 164 ± 22 breaths/minute at predose to 178 ± 17 breaths/minute (p = 0.24) at 2 min. The mean plasma concentrations of NTX, 3.5 months after implantation, ranged from 7.4 (±1.1) ng/mL to 80.3 (±37.5) ng/mL. Bioabsorbable implants containing NTX effectively blocked fentanyl-induced respiratory depression in rodents as compared with placebo implants, 3.5 months after implantation.

摘要

本研究旨在确定是否可延长释放、可生物吸收的皮下纳曲酮(NTX)植入物可抑制芬太尼静脉注射后的呼吸抑制。单独(安慰剂)或包含 NTX 的两种不同控释聚合物,聚-D-乳酸(PDLLA)和聚己内酯(PCL)的可生物吸收植入物被皮下植入 Sprague Dawley 大鼠。植入 3.5 个月后,通过尾静脉给啮齿动物静脉注射芬太尼。安慰剂植入组的大鼠接受 4μg(mcg)-(10 mcg/kg/剂量)的剂量,而 NTX 植入组接受 8μg(20 mcg/kg/剂量)的剂量。导致安慰剂植入的啮齿动物呼吸率下降超过 50±2%的芬太尼最小有效剂量为 4 mcg。安慰剂植入大鼠的呼吸率从 208±14 次/分钟降至 2 分钟时的 84±12 次/分钟(p=0.0003)。相比之下,所有 NTX 植入动物均能轻松耐受两倍剂量的 8 mcg 芬太尼,而呼吸率无明显下降。平均呼吸率=从预给药时的 164±22 次/分钟增加到 2 分钟时的 178±17 次/分钟(p=0.24)。植入后 3.5 个月,NTX 的平均血浆浓度范围为 7.4(±1.1)ng/mL 至 80.3(±37.5)ng/mL。与安慰剂植入相比,植入后 3.5 个月,含有 NTX 的可生物吸收植入物可有效阻止芬太尼引起的啮齿动物呼吸抑制。

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