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吸入型纳米mRNA 多聚物用于肺部上皮细胞的蛋白生产。

Inhaled Nanoformulated mRNA Polyplexes for Protein Production in Lung Epithelium.

机构信息

Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, MA, 02139, USA.

Division of Cancer and Stem Cells, School of Medicine, and Division of Advanced Materials and Healthcare Technologies, School of Pharmacy, University of Nottingham, Nottingham, NG7 2RD, UK.

出版信息

Adv Mater. 2019 Feb;31(8):e1805116. doi: 10.1002/adma.201805116. Epub 2019 Jan 4.

Abstract

Noninvasive aerosol inhalation is an established method of drug delivery to the lung, and remains a desirable route for nucleic-acid-based therapeutics. In vitro transcribed (IVT) mRNA has broad therapeutic applicability as it permits temporal and dose-dependent control of encoded protein expression. Inhaled delivery of IVT-mRNA has not yet been demonstrated and requires development of safe and effective materials. To meet this need, hyperbranched poly(beta amino esters) (hPBAEs) are synthesized to enable nanoformulation of stable and concentrated polyplexes suitable for inhalation. This strategy achieves uniform distribution of luciferase mRNA throughout all five lobes of the lung and produces 101.2 ng g of luciferase protein 24 h after inhalation of hPBAE polyplexes. Importantly, delivery is localized to the lung, and no luminescence is observed in other tissues. Furthermore, using an Ai14 reporter mouse model it is identified that 24.6% of the total lung epithelial cell population is transfected after a single dose. Repeat dosing of inhaled hPBAE-mRNA generates consistent protein production in the lung, without local or systemic toxicity. The results indicate that nebulized delivery of IVT-mRNA facilitated by hPBAE vectors may provide a clinically relevant delivery system to lung epithelium.

摘要

非侵入性气溶胶吸入是一种将药物递送到肺部的既定方法,并且仍然是核酸治疗药物的理想途径。体外转录(IVT)mRNA 具有广泛的治疗适用性,因为它可以实现对编码蛋白表达的时间和剂量依赖性控制。IVT-mRNA 的吸入递送尚未得到证实,需要开发安全有效的材料。为了满足这一需求,合成了超支化聚(β氨基酯)(hPBAE),以实现适用于吸入的稳定且浓缩的聚合物纳米粒的制剂。该策略实现了荧光素酶 mRNA 在肺部所有五个叶中的均匀分布,并在吸入 hPBAE 聚合物后 24 小时产生 101.2ng/g 的荧光素酶蛋白。重要的是,递送至肺部是局部的,在其他组织中观察不到发光。此外,使用 Ai14 报告小鼠模型,鉴定出单次剂量后,总肺上皮细胞群体中有 24.6%被转染。吸入 hPBAE-mRNA 的重复给药可在肺部产生一致的蛋白产生,而无局部或全身毒性。结果表明,由 hPBAE 载体介导的 IVT-mRNA 的雾化递送可能为肺上皮细胞提供一种有临床意义的递送系统。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/563a/7490222/4f92d78be724/nihms-1620593-f0001.jpg

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