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可生物降解的皮下纳曲酮植入物可减轻 3 个月时芬太尼引起的呼吸抑制 - 雄性犬的初步研究。

Bioabsorbable, subcutaneous naltrexone implants mitigate fentanyl-induced respiratory depression at 3 months-A pilot study in male canines.

机构信息

Richard A. Henson Research Institute, TidalHealth Peninsula Regional Salisbury, Salisbury, Maryland, USA.

Labcorp, Greenfield, Indiana, USA.

出版信息

Physiol Rep. 2024 Aug;12(15):e16176. doi: 10.14814/phy2.16176.

Abstract

The aim of this study is to determine if extended-release, bioabsorbable, subcutaneous naltrexone (NTX) implants can mitigate respiratory depression after an intravenous injection (IV) of fentanyl. Six different BIOabsorbable Polymeric Implant Naltrexone (BIOPIN) formulations, comprising combinations of Poly-d,l-Lactic Acid (PDLLA) and/or Polycaprolactone (PCL-1 or PCL-2), were used to create subcutaneous implants. Both placebo and naltrexone implants were implanted subcutaneously in male dogs. The active naltrexone implants consisted of two doses, 644 mg and 1288 mg. A challenge with IV fentanyl was performed in 33 male dogs at 97-100 days after implantation. Following the administration of a 30 μg/kg intravenous fentanyl dose, the placebo cohort manifested a swift and profound respiratory depression with a ~50% reduction in their pre-dose respiratory rate (RR). The BIOPIN NTX-implanted dogs were exposed to escalating doses of intravenous fentanyl (30 μg/kg, 60 μg/kg, 90 μg/kg, and 120 μg/kg). In contrast, the dogs implanted with the BIOPIN naltrexone implants tolerated doses up to 60 μg/kg without significant respiratory depression (<50%) but had severe respiratory depression with fentanyl doses of 90 μg/kg and especially at 120 μg/kg. Bioabsorbable, extended-release BIOPIN naltrexone implants are effective in mitigating fentanyl-induced respiratory depression in male canines at about 3 months after implantation. This technology may also have potential for mitigating fentanyl-induced respiratory depression in humans.

摘要

本研究旨在确定皮下缓释、可生物吸收的纳曲酮(NTX)植入物是否可以减轻芬太尼静脉注射(IV)后的呼吸抑制。使用了六种不同的 BIOabsorbable Polymeric Implant Naltrexone(BIOPIN)制剂,这些制剂由聚-DL-乳酸(PDLLA)和/或聚己内酯(PCL-1 或 PCL-2)组合而成,用于制造皮下植入物。雄性犬均皮下植入安慰剂和纳曲酮植入物。活性纳曲酮植入物包含两种剂量,分别为 644mg 和 1288mg。在植入后 97-100 天,33 只雄性犬接受了 IV 芬太尼挑战。在给予 30μg/kg 的静脉芬太尼剂量后,安慰剂组表现出迅速而深刻的呼吸抑制,其呼吸频率(RR)比基础值降低了约 50%。BIOPIN NTX 纳曲酮植入犬暴露于递增剂量的静脉芬太尼(30μg/kg、60μg/kg、90μg/kg 和 120μg/kg)。相比之下,植入 BIOPIN 纳曲酮植入物的犬在没有明显呼吸抑制(<50%)的情况下耐受 60μg/kg 的剂量,但在 90μg/kg 和特别是 120μg/kg 的芬太尼剂量下出现严重呼吸抑制。在植入后约 3 个月,可生物吸收的、缓释的 BIOPIN 纳曲酮植入物可有效减轻雄性犬中芬太尼引起的呼吸抑制。这项技术也可能具有减轻人类中芬太尼引起的呼吸抑制的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ba8/11310269/a4dc22c51ffb/PHY2-12-e16176-g002.jpg

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