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International Journal of Pharmaceutics

International Journal of Pharmaceutics

IF: 5.29
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Bromocriptine mesylate-loaded nanoparticles co-modified with low molecular weight protamine and lactoferrin for enhanced nose-to-brain delivery in Parkinson's …

Published:10 December 2024 DOI: 10.1016/j.ijpharm.2024.125054 PMID: 39667592
Huijing Cong, Jing Hu, Jing Wang, Baiyu Chang, Rongtao Li, Xinran Cui, Chenghao Zhang, Hongyu Ji, Congcong Lin, Jingling Tang, Jiaxin Liu

Abstract

Parkinson's disease confronts challenges in drug delivery due to the blood-brain barrier. Intranasal delivery bypasses the blood-brain barrier for improved drug bioavailability, yet narrow nasal space and brief retention time hinder clinical applicability. We conducted a Bromocriptine Mesylate-loaded PLGA nanoparticles co-modified with low molecular weight protamine (LMWP) and lactoferrin (Lf) (LMWP/Lf-BCM-NPs) for nose-to-brain delivery. The resulting LMWP/Lf-BCM-NPs were uniform spheres with an average size of 248.53 ± 16.25 nm and zeta potential of -2.63 ± 0.74 mV. Fourier transform infrared spectroscopy confirmed LMWP and Lf attachment. The co-modified nanoparticles showed improving cellular transport and good viability. The LMWP/Lf-BCM-NPs showed increased brain targeting efficiency in mice. In haloperidol-induced Parkinson mouse models, the LMWP/Lf-BCM-NPs showed increased brain targeting efficiency, enhanced behavioral regulatory effects, enhanced antioxidant effects and neuroprotection effects. This study paves the way for a novel, non-invasive brain-targeted therapy, offering a promising avenue for Parkinson's disease clinical treatment.

Substances (3)

Materials
Procduct Name CAS Molecular Formula Supplier Price
Sodium deoxycholate 302-95-4 C24H41NaO4 532 suppliers $19.00-$10811.00
Haloperidol 52-86-8 C21H23ClFNO2 406 suppliers $30.00-$1504.50
MTT 2348-71-2 C18H16BrN5S 47 suppliers Inquiry

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