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定制型冰片修饰的脂质纳米粒鼻腔喷雾剂,用于增强针对中枢神经系统疾病的经鼻递药。

Tailored Borneol-Modified Lipid Nanoparticles Nasal Spray for Enhanced Nose-to-Brain Delivery to Central Nervous System Diseases.

机构信息

School of Pharmaceutical Sciences, Sun Yat-Sen University, Guangzhou 510006, Guangdong, P. R. China.

College of Pharmacy, Jinan University, Guangzhou 510006, Guangdong, P. R. China.

出版信息

ACS Nano. 2024 Aug 27;18(34):23684-23701. doi: 10.1021/acsnano.4c08279. Epub 2024 Aug 19.

Abstract

The nanodrug delivery system-based nasal spray (NDDS-NS) can bypass the blood-brain barrier and deliver drugs directly to the brain, offering unparalleled advantages in the treatment of central nervous system (CNS) diseases. However, the current design of NNDS-NS is excessively focused on mucosal absorption while neglecting the impact of nasal deposition on nose-to-brain drug delivery, resulting in an unsatisfactory nose-to-brain delivery efficiency. In this study, the effect of the dispersion medium viscosity on nasal drug deposition and nose-to-brain delivery in NDDS-NS was elucidated. The optimized formulation F5 (39.36 mPa·s) demonstrated significantly higher olfactory deposition fraction (ODF) of 23.58%, and a strong correlation between ODF and intracerebral drug delivery ( = 0.7755) was observed. Building upon this understanding, a borneol-modified lipid nanoparticle nasal spray (BLNP-NS) that combined both nasal deposition and mucosal absorption was designed for efficient nose-to-brain delivery. BLNP-NS exhibited an accelerated onset of action and enhanced brain targeting efficiency, which could be attributed to borneol modification facilitating the opening of tight junction channels. Furthermore, BLNP-NS showed superiority in a chronic migraine rat model. It not only provided rapid relief of migraine symptoms but also reversed neuroinflammation-induced hyperalgesia. The results revealed that borneol modification could induce the polarization of microglia, regulate the neuroinflammatory microenvironment, and repair the neuronal damage caused by neuroinflammation. This study highlights the impact of dispersion medium viscosity on the nose-to-brain delivery process of NDDS-NS and serves as a bridge between the formulation development and clinical transformation of NDDS-NS for the treatment of CNS diseases.

摘要

基于纳米药物递送系统的鼻喷雾剂(NDDS-NS)可以绕过血脑屏障,将药物直接递送到大脑,在治疗中枢神经系统(CNS)疾病方面具有无与伦比的优势。然而,目前的 NDDS-NS 设计过于关注黏膜吸收,而忽略了鼻腔沉积对鼻内递药的影响,导致鼻内递药效率不理想。在这项研究中,阐明了分散介质粘度对 NDDS-NS 中鼻腔药物沉积和鼻内递药的影响。优化的配方 F5(39.36 mPa·s)表现出显著更高的嗅觉沉积分数(ODF),为 23.58%,并且观察到 ODF 与脑内药物递送之间存在强相关性(=0.7755)。在此基础上,设计了一种结合鼻腔沉积和黏膜吸收的冰片修饰脂质纳米粒鼻喷雾剂(BLNP-NS),以实现高效的鼻内递药。BLNP-NS 表现出更快的作用起始和增强的脑靶向效率,这归因于冰片修饰促进了紧密连接通道的开放。此外,BLNP-NS 在慢性偏头痛大鼠模型中表现出优越性。它不仅提供了偏头痛症状的快速缓解,还逆转了神经炎症引起的痛觉过敏。结果表明,冰片修饰可以诱导小胶质细胞极化,调节神经炎症微环境,修复神经炎症引起的神经元损伤。这项研究强调了分散介质粘度对 NDDS-NS 鼻内递药过程的影响,为 NDDS-NS 的制剂开发和临床转化治疗 CNS 疾病提供了桥梁。

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