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用于增强局部药物制剂经皮递送的微柱隧道压模

Micro-pillar tunnel stamp for enhanced transdermal delivery of topical drug formulations.

作者信息

Jeon Chansol, Choi Jaibyung, Shin Jiwoo, Min Hye Su, Nam Jeehye, Jeon Seonghun, Kim Jeongin, Kim Youseong, Sim Jeeho, Ahn Hyeri, Kim Minkyung, Yang Huisuk, Jung Hyungil

机构信息

Department of Biotechnology, Building 123, Yonsei University, 50 Yonsei-ro, Seodaemun-gu, Seoul 03722, Republic of Korea; Juvic Inc., 272 Digital-ro, Guro-gu, Seoul 08389, Republic of Korea.

Department of Biotechnology, Building 123, Yonsei University, 50 Yonsei-ro, Seodaemun-gu, Seoul 03722, Republic of Korea.

出版信息

Acta Biomater. 2023 Apr 1;160:112-122. doi: 10.1016/j.actbio.2023.02.001. Epub 2023 Feb 9.

Abstract

Dissolving microneedles (DMNs), despite their minimally invasive drug administration, face challenges in skin insertion and drug-loading capacity, which lead to less effective drug delivery. The micro-pillar tunnel stamp (MPTS) was designed to enhance the transdermal delivery efficacy of externally provided topical formulations via the creation of microchannels. The tunnel and canal of the MPTS enable the simultaneous application of DMNs and topical drugs. The application of micro-pillar-polycaprolactone (MP-PCL), which is a DMN made of a slowly dissolving polymer, exhibited a drug permeation rate 1.3-fold and 2.6-fold higher than that of micro-pillar-hyaluronic acid (MP-HA), a DMN made of a rapidly dissolving polymer, and the topical group, respectively. The base diameter of MP-PCL was set to 700 μm for maximized delivery efficacy, achieving 2.8-fold higher L-ascorbic acid accumulation than that of the topical group. In vivo analysis showed that, compared to topical administration, MPTS-delivered lidocaine had 5-fold greater permeation and the MPTS-delivered group showed 1.25-fold higher skin residual amount, confirming enhanced delivery. Thus, the optimized MPTS system can be presented as an attractive alternative to overcome the limitations of the existing MN systems such as incomplete insertion and limited drug-loading capacity, enhancing the delivery of topical formulations in the transdermal market. STATEMENT OF SIGNIFICANCE: We developed a micro-pillar tunnel stamp (MPTS) to enhance the delivery of externally provided topical formulations. The functional tunnel and canal of the MPTS enabled the simultaneous application of a dissolving microneedle (DMN) array insertion and administration of external topical drugs. Upon insertion, the DMNs created skin microchannels that allowed the externally administered drug to diffuse. DMNs were fabricated using polycaprolactone (PCL), a slowly dissolving polymer, to maintain their structure inside the skin and prolong the opening duration of the microchannels. This system achieved significantly improved delivery of topically administered external drugs via integration with slowly dissolving DMNs, while offering the possibility of its development as a universal delivery system for various topical pharmaceuticals.

摘要

溶蚀性微针(DMNs)尽管具有微创给药的特点,但在皮肤插入和载药量方面面临挑战,这导致药物递送效果不佳。微柱隧道印章(MPTS)旨在通过创建微通道来提高外部提供的局部制剂的透皮递送效果。MPTS的隧道和管道能够同时应用DMNs和局部药物。由缓慢溶解聚合物制成的DMN微柱聚己内酯(MP-PCL)的应用,其药物渗透速率分别比由快速溶解聚合物制成的DMN微柱透明质酸(MP-HA)和局部给药组高1.3倍和2.6倍。将MP-PCL的基部直径设定为700μm以实现最大递送效果,L-抗坏血酸积累量比局部给药组高2.8倍。体内分析表明,与局部给药相比,MPTS递送的利多卡因的渗透量高5倍,MPTS递送组的皮肤残留量高1.25倍,证实了递送效果的增强。因此,优化后的MPTS系统可以作为一种有吸引力的替代方案,以克服现有微针系统的局限性,如插入不完全和载药量有限,从而提高局部制剂在透皮市场的递送效果。重要意义声明:我们开发了一种微柱隧道印章(MPTS)以增强外部提供的局部制剂的递送。MPTS的功能性隧道和管道能够同时进行溶蚀性微针(DMN)阵列插入和外部局部药物给药。插入后,DMNs创建了皮肤微通道,使外部给药的药物得以扩散。使用缓慢溶解的聚合物聚己内酯(PCL)制造DMNs,以在皮肤内维持其结构并延长微通道的开放持续时间。该系统通过与缓慢溶解的DMNs整合,显著提高了局部给药的外部药物的递送效果,同时提供了将其开发为各种局部药物通用递送系统的可能性。

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