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使用冷冻微针进行皮内 mRNA 递药。

Intradermal delivery of mRNA using cryomicroneedles.

机构信息

Department of Biomedical Engineering, City University of Hong Kong, 83 Tat Chee Avenue, Kowloon, Hong Kong SAR, China.

School of Biomedical Sciences, Li Ka Shing Faculty of Medicine, University of Hong Kong, 21 Sassoon Road, Hong Kong SAR, China.

出版信息

Acta Biomater. 2022 Aug;148:133-141. doi: 10.1016/j.actbio.2022.06.015. Epub 2022 Jun 11.

Abstract

Microneedles can realize the intradermal and transdermal delivery of drugs. However, most conventional microneedles made of metal, polymer and ceramics are unsuitable for the delivery of mRNA drugs that are fragile and temperature-sensitive. This study explores the usage of cryomicroneedles (CryoMNs) for the intradermal delivery of mRNA molecules. Taking luciferase mRNA as an example, we first optimize the formulation of CryoMNs to maximize mRNA stability. Later, in the mouse model, we compare the delivery efficiency with the conventional subcutaneous injection for both the luciferase mRNA and COVID-19 Comirnaty mRNA vaccines, where CryoMNs delivered mRNA vaccines successfully induce specific B-cell antibody, neutralizing activity and T-cell responses. STATEMENT OF SIGNIFICANCE: mRNA vaccines are fragile and temperature-sensitive, so they are mainly delivered by intramuscular injection that often causes pain and requires clinical expertise to immunize patients. Microneedles permit convenient, fast and safe vaccination. However, existing microneedle platforms are ineffective to protect the integrity of mRNA vaccines in fabrication, storage, and administration. This work utilizes cryomicroneedles (CryoMNs) technology to intradermally deliver mRNA. In the mouse model, CryoMNs are compared with the subcutaneous injection for the delivery efficiency of both the luciferase mRNA and COVID-19 Comirnaty mRNA vaccines, where CryoMNs delivered mRNA vaccines successfully produce specific B-cell antibodies, T-cell responses, and neutralizing activity. This work is expected to provide a new delivery strategy for the emerging mRNA therapeutics.

摘要

微针可以实现药物的皮内和透皮递送。然而,大多数由金属、聚合物和陶瓷制成的常规微针不适合递送脆弱且对温度敏感的 mRNA 药物。本研究探讨了使用 cryomicroneedles(CryoMNs)进行 mRNA 分子的皮内递送。以荧光素酶 mRNA 为例,我们首先优化了 CryoMNs 的配方,以最大限度地提高 mRNA 的稳定性。随后,在小鼠模型中,我们比较了 CryoMNs 与传统的皮下注射在递送荧光素酶 mRNA 和 COVID-19 Comirnaty mRNA 疫苗方面的效率,结果表明 CryoMNs 成功地递送达了 mRNA 疫苗,诱导了特异性 B 细胞抗体、中和活性和 T 细胞反应。

意义声明

mRNA 疫苗脆弱且对温度敏感,因此主要通过肌肉注射进行递送,这往往会引起疼痛,并需要临床专业知识来为患者接种疫苗。微针允许方便、快速和安全的接种。然而,现有的微针平台在制造、储存和管理过程中无法有效地保护 mRNA 疫苗的完整性。本工作利用 cryomicroneedles(CryoMNs)技术经皮内递送达 mRNA。在小鼠模型中,我们比较了 CryoMNs 与皮下注射在递送荧光素酶 mRNA 和 COVID-19 Comirnaty mRNA 疫苗方面的效率,结果表明 CryoMNs 成功地递送达了 mRNA 疫苗,诱导了特异性 B 细胞抗体、T 细胞反应和中和活性。这项工作有望为新兴的 mRNA 治疗提供新的递送策略。

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