Brain Targeting of Venlafaxine via Intranasal Transbilosomes Thermogel for Improved Management of Depressive Disorder

文拉法辛 鼻腔给药 重性抑郁障碍 医学 药理学 麻醉 精神科 抗抑郁药 焦虑 认知
作者
Omar Awad Alsaidan,Mohammed H. Elkomy,Randa Mohammed Zaki,Alaa S. Tulbah,Rehab Mohammad Yusif,Hussein M. Eid
出处
期刊:Journal of Pharmaceutical Sciences [Elsevier]
卷期号:113 (11): 3304-3314 被引量:8
标识
DOI:10.1016/j.xphs.2024.08.026
摘要

The current research aimed to design and optimize hyaluronic acid-coated transbilosomes containing venlafaxine (VLF-HA-TBLs) for nose-to-brain delivery for improved management of depressive disorder. Venlafaxine-loaded transbilosomes (VLF-TBLs) were developed according to the film hydration procedure, optimized for maximum efficiency using the quality by design-based Box-Behnken design (BBD), and then coated with hyaluronic acid (HA). The optimized VLF-HA-TBLs were subjected to in vitro characterization, integrated into a thermolabile gel, and then exposed to in vivo evaluation studies. The results revealed that the VLF-HA-TBLs formulation exhibited acceptable size (185.6±4.9 nm), surface charge (-39.8±1.7 mV), and entrapment efficiency (69.6 ± 2.6%). The morphological study revealed that nanovesicles were spherical and displayed a consistent size distribution without particle aggregation. It also showed improved ex vivo nasal diffusion and a prolonged release profile. In addition, the formulated VLF-HA-TBLs were stable under the studied conditions and tolerable when applied intranasally. Compared to the intranasal administration of VLF solution (VLF-SOL), the biodistribution analysis showed that VLF-HA-TBLs delivered intranasally had a relative bioavailability of 441% in the brain and 288% in plasma. Moreover, the intranasal delivery of VLF-HA-TBLs demonstrated much higher bioavailability (512%) in the brain compared to VLF-SOL administered intravenously. Collectively, it could be possible to infer that HA-TBLs might be an effective nanocarrier to administer VLF to the brain via the nasal route.

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