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TSA-SAB Co-Loaded Liposome Self-Dissolving Microneedle Synergistic Delivery System: A Breakthrough Dual-Drug Loading Strategy for Multi-Target Therapy of Hypertrophic Scars

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Taylor & Francis Group2025-10-21 更新2026-04-16 收录
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https://tandf.figshare.com/articles/dataset/TSA-SAB_Co-Loaded_Liposome_Self-Dissolving_Microneedle_Synergistic_Delivery_System_A_Breakthrough_Dual-Drug_Loading_Strategy_for_Multi-Target_Therapy_of_Hypertrophic_Scars/29875291/1
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The treatment of hypertrophic scars is constrained by inefficient transdermal delivery and challenges in co-delivery of multiple drugs. Although tanshinone IIA and salvianolic acid B exhibit multi-target antifibrotic potential, their divergent physicochemical properties limit combined application. This study proposes a novel transdermal system integrating co-loaded liposomes with dissolving microneedles (DMNs). TSA-SAB liposomes were prepared via thin-film dispersion with pH gradient method, optimized using Box-Behnken design to overcome traditional single-factor limitations. High-efficiency co-loading was achieved for lipophilic TSA (encapsulation efficiency: 86.10%) and hydrophilic SAB (98.43%). Integration with centrifugally cast microneedles yielded loadings of 216.01 μg/patch (TSA) and 371.65 μg/patch (SAB). Leveraging microneedle-mediated penetration and liposomal sustained release, the system showed 3-fold higher transdermal efficiency than free drugs, establishing a dermal reservoir. In vitro release followed Higuchi model (24 h: 68.33% TSA, 76.33% SAB) without burst release. Integrating nanocarriers with microneedles, this study provides a strategy to address multi-drug incompatibility and transdermal barriers, laying groundwork for HS therapy translation.
提供机构:
Yu, Jia-Hui; Li, Ying-Ping; Xu, Jing-Hang; Shi, Jun; Yao, Bi-Jin; Peng, Rui-Xiang; Cheng, Lu-Lu
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2025-08-09
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