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用于佐剂和抗原顺序皮内递送的双微针阵列贴片的研发与评估

Development and Evaluation of Dual Microneedle Array Patch for Sequential Intradermal Delivery of Adjuvant and Antigen.

作者信息

Lee Ye-Lim, Cha Hye-Ran, Lee Da-Eun, Ryu Minwoo, Chung Hyeon Woo, Park Sunghoon, Choi Jung-Ah, Baek Seung-Ki, Lee Jae Myun, Park Jung-Hwan

机构信息

Department of BioNano Technology, Gachon BioNano Research Institute, Gachon University, Seongnam, Gyeonggi-Do, 13120, Republic of Korea.

Department of Microbiology and Immunology, Institute for Immunology and Immunological Diseases, Graduate School of Medical Science, Brain Korea 21 Project, Yonsei University College of Medicine, Seoul, 03722, Republic of Korea.

出版信息

Pharm Res. 2025 Sep 4. doi: 10.1007/s11095-025-03914-3.

Abstract

PURPOSE

Adjuvants are critical for enhancing immune responses to recombinant protein-based vaccines, which typically exhibit weak immunogenicity. Microneedle array patches (MAPs) offer a promising method for intradermal delivery, but conventional Co-Delivery MAPs (containing antigen and adjuvant together) have limited loading capacity and potential undesirable interactions. Adjuvants may also trigger adverse reactions in sensitive populations. This study aimed to develop a Dual-Delivery MAP system that enables separate and sequential administration of antigens and adjuvants, addressing these limitations and supporting personalized vaccination strategies.

METHODS

The Dual-Delivery MAP was developed using a coated MAP for ovalbumin (OVA) and a dissolving MAP for the CTA1 adjuvant. Patches were sequentially applied to the same skin site. Delivery efficiency, intradermal distribution, and immunogenicity were evaluated and compared to a conventional Co-Delivery MAP and an intramuscular (IM) injection group (OVA and CTA1 in solution). OVA- and CTA1-specific IgG titers were measured to assess immune responses.

RESULTS

Both Dual-Delivery and Co-Delivery MAPs demonstrated similar delivery efficiency (~ 70%). However, the Dual-Delivery MAP elicited significantly higher IgG titers against CTA1 and OVA compared to the Co-Delivery MAP, likely due to enhanced adjuvant functionality. The Dual-Delivery MAP induced immune responses comparable to IM injection, indicating that sequential delivery preserves adjuvant activity and enhances immunogenicity.

CONCLUSIONS

The Dual-Delivery MAP represents a novel, modular approach for skin-targeted vaccination. By separating antigen and adjuvant into distinct patches, it improves stability, maintains adjuvant efficacy, and enables personalized vaccine administration, offering a promising strategy for effective and safe vaccination.

摘要

目的

佐剂对于增强基于重组蛋白的疫苗的免疫反应至关重要,这类疫苗通常免疫原性较弱。微针阵列贴片(MAPs)为皮内给药提供了一种有前景的方法,但传统的共递送MAPs(同时包含抗原和佐剂)具有有限的负载能力和潜在的不良相互作用。佐剂也可能在敏感人群中引发不良反应。本研究旨在开发一种双递送MAP系统,能够分别且顺序地给予抗原和佐剂,解决这些局限性并支持个性化疫苗接种策略。

方法

使用包被有卵清蛋白(OVA)的MAP和溶解有CTA1佐剂的MAP来开发双递送MAP。将贴片顺序应用于同一皮肤部位。评估递送效率、皮内分布和免疫原性,并与传统的共递送MAP和肌肉注射(IM)组(溶液中的OVA和CTA1)进行比较。测量OVA和CTA1特异性IgG滴度以评估免疫反应。

结果

双递送MAP和共递送MAP均显示出相似的递送效率(约70%)。然而,与共递送MAP相比,双递送MAP诱导出针对CTA1和OVA的显著更高的IgG滴度,这可能是由于佐剂功能增强。双递送MAP诱导的免疫反应与IM注射相当,表明顺序递送保留了佐剂活性并增强了免疫原性。

结论

双递送MAP代表了一种用于皮肤靶向疫苗接种的新型模块化方法。通过将抗原和佐剂分离到不同的贴片中,它提高了稳定性,维持了佐剂功效,并实现了个性化疫苗给药,为有效和安全的疫苗接种提供了一种有前景的策略。

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