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通过物理表征提高载麻醉剂纳米液滴的可扩展性和潜力。

Physical Characterization to Improve Scalability and Potential of Anesthetic-Loaded Nanodroplets.

作者信息

Ting Siulam Ginni, Lea-Banks Harriet, Hynynen Kullervo

机构信息

Physical Sciences Platform, Sunnybrook Research Institute, Toronto, ON M4N 3M5, Canada.

Department of Medical Biophysics, University of Toronto, Toronto, ON M5S 1A1, Canada.

出版信息

Pharmaceutics. 2023 Aug 3;15(8):2077. doi: 10.3390/pharmaceutics15082077.

Abstract

Drug-loaded perfluorocarbon nanodroplets (NDs) can be activated non-invasively by focused ultrasound (FUS) and allow for precise drug-delivery. Anesthetic-loaded NDs and transcranial FUS have previously achieved targeted neuromodulation. To assess the clinical potential of anesthetic-loaded NDs, in depth physical characterization and investigation of storage strategies and triggered-activation is necessary. Pentobarbital-loaded decafluorobutane nanodroplets (PBNDs) with a Definity-derived lipid shell (237 nm; 4.08 × 10 particles/mL) were fabricated and assessed. Change in droplet stability, concentration, and drug-release efficacy were tested for PBNDs frozen at -80 °C over 4 weeks. PBND diameter and the polydispersity index of thawed droplets remained consistent up to 14 days frozen. Cryo-TEM images revealed NDs begin to lose circularity at 7 days, and by 14 days, perfluorocarbon dissolution and lipid fragmentation occurred. The level of acoustic response and drug release decreases through prolonged storage. PBNDs showed no hemolytic activity at clinically relevant concentrations and conditions. At increasing sonication pressures, liquid PBNDs vaporized into gas microbubbles, and acoustic activity at the second harmonic frequency (2 f) peaked at lower pressures than the subharmonic frequency (1/2 f). Definity-based PBNDs have been thoroughly characterized, cryo-TEM has been shown to be suitable to image the internal structure of volatile NDs, and PBNDs can be reliably stored at -80 °C for future use up to 7 days without significant degradation, loss of acoustic response, or reduction in ultrasound-triggered drug release.

摘要

载药全氟碳纳米液滴(NDs)可通过聚焦超声(FUS)进行非侵入性激活,并实现精确给药。此前,载麻醉剂的纳米液滴和经颅聚焦超声已实现靶向神经调节。为评估载麻醉剂纳米液滴的临床潜力,有必要对其进行深入的物理表征,并研究储存策略和触发激活情况。制备并评估了具有源自Definity脂质壳(237纳米;4.08×10颗粒/毫升)的载戊巴比妥十氟丁烷纳米液滴(PBNDs)。对在-80°C下冷冻4周的PBNDs的液滴稳定性、浓度和药物释放效果变化进行了测试。在冷冻长达14天的时间里,解冻后液滴的PBND直径和多分散指数保持一致。冷冻透射电子显微镜图像显示,纳米液滴在7天时开始失去圆形,到14天时,全氟碳溶解和脂质破碎发生。随着储存时间延长,声学响应水平和药物释放量降低。在临床相关浓度和条件下,PBNDs未表现出溶血活性。随着超声处理压力增加,液态PBNDs汽化成气体微泡,二次谐波频率(2f)处的声学活性在比次谐波频率(1/2f)更低的压力下达到峰值。基于Definity的PBNDs已得到充分表征,冷冻透射电子显微镜已被证明适用于对挥发性纳米液滴的内部结构进行成像,并且PBNDs可以在-80°C下可靠储存以备将来使用长达7天,而不会出现明显降解、声学响应丧失或超声触发药物释放减少的情况。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c12c/10457791/ba0ace47a5e6/pharmaceutics-15-02077-g001.jpg

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