том 104 страницы 106489

Rizatriptan loaded Bilosomes for Nose to Brain Delivery: Fabrication, Statistical Optimization, and Biological Evaluation

Omar Awad Alsaidan 1
Ameeduzzafar Zafar 1
Hassan H Alhassan 2
Eyad Abdulrazaq Alburaykan 3
Aseel Awad Alsaidan 4
Mohd. Yasir 5
Тип публикацииJournal Article
Дата публикации2025-02-01
scimago Q1
wos Q1
БС1
SJR0.817
CiteScore8.3
Impact factor4.9
ISSN17732247, 25888943, 11571489
Краткое описание
Rizatriptan (RTP) is an anti-migraine drug and after oral administration, it exhibits low bioavailability (45 %) due to high first-pass hepatic metabolism. Therefore, to resolve this issue, RTP-loaded bilosomes (BLSs) for brain delivery through the intranasal route were developed. RTP-BLSs were prepared by the thin-film hydration technique and optimized by the L9 Taguchi model. Bile salt (sodium glycocholate, mg), surfactant (Span 40, mg), and edge activator (Cremophor RH 40, mg) were selected as independent factors and their influence was observed on vesicle size (nm) and entrapment efficiency (%). Selected optimized RTP-BLSs (F5) formulation exhibited low vesicle size (204.70 ± 5.8 nm) and polydispersity index (0.260 ± 0.022), good entrapment efficiency (78.32 ± 3.1 %), and high zeta potential (−27.6 ± 1.67 mV). The optimized RTP-BLSs formulation exhibited more sustained released profile (96.41 ± 4.48 % in 24 h) than RTP-Sol (98.65 ± 3.46 % RTP released in 4 h). The flux and apparent permeability coefficient for optimized RTP-BLSs were found to be 1.069 ± 0.026 μg cm−2 h1 and 10.690 × 10−4 ± 0.262 × 10−4 cm h−1, respectively which were significantly (P < 0.05) better than the flux (0.548 ± 0.148 μg cm−2 h−1) and apparent permeability coefficient (5.481 × 10−4 ± 1.476 × 10−4 cm h−1) of RTP-Sol. The relative bioavailability of RTP formulated within the optimized RTP-BLSs administered intranasally was 2.94 ± 0.78-fold higher than the one obtained with RTP-Sol. The optimized RTP-BLSs showed 1.91 ± 0.15-fold higher absolute bioavailability as compared to intravenous administration RTP-BLSs. The optimized RTP-BLSs showed 64.18 ± 2.34 % nose-to-brain drug transport, while RTP-Sol exhibited 20.72 ± 1.46 % after intranasal administration. The optimized RTP-BLSs showed a significantly higher brain drug targeting efficiency (279.16 ± 6.37 %) as compared to RTP-Sol (126.15 ± 4.79 %) given intranasally. From the findings, it can be concluded that the developed BLSs are novel alternative RTP carriers for direct nose-to-brain delivery for the improvement of brain drug targeting.
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Polymers
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Molecular Pharmaceutics
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Alruwaili N. K. et al. Rizatriptan loaded Bilosomes for Nose to Brain Delivery: Fabrication, Statistical Optimization, and Biological Evaluation // Journal of Drug Delivery Science and Technology. 2025. Vol. 104. p. 106489.
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Alsaidan O. A., Zafar A., Alhassan H. H., Alburaykan E. A., Alsaidan A. A., Yasir M. Rizatriptan loaded Bilosomes for Nose to Brain Delivery: Fabrication, Statistical Optimization, and Biological Evaluation // Journal of Drug Delivery Science and Technology. 2025. Vol. 104. p. 106489.
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TY - JOUR
DO - 10.1016/j.jddst.2024.106489
UR - https://linkinghub.elsevier.com/retrieve/pii/S1773224724011584
TI - Rizatriptan loaded Bilosomes for Nose to Brain Delivery: Fabrication, Statistical Optimization, and Biological Evaluation
T2 - Journal of Drug Delivery Science and Technology
AU - Alsaidan, Omar Awad
AU - Zafar, Ameeduzzafar
AU - Alhassan, Hassan H
AU - Alburaykan, Eyad Abdulrazaq
AU - Alsaidan, Aseel Awad
AU - Yasir, Mohd.
PY - 2025
DA - 2025/02/01
PB - Elsevier
SP - 106489
VL - 104
SN - 1773-2247
SN - 2588-8943
SN - 1157-1489
ER -
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@article{2025_Alruwaili,
author = {Omar Awad Alsaidan and Ameeduzzafar Zafar and Hassan H Alhassan and Eyad Abdulrazaq Alburaykan and Aseel Awad Alsaidan and Mohd. Yasir},
title = {Rizatriptan loaded Bilosomes for Nose to Brain Delivery: Fabrication, Statistical Optimization, and Biological Evaluation},
journal = {Journal of Drug Delivery Science and Technology},
year = {2025},
volume = {104},
publisher = {Elsevier},
month = {feb},
url = {https://linkinghub.elsevier.com/retrieve/pii/S1773224724011584},
pages = {106489},
doi = {10.1016/j.jddst.2024.106489}
}