Delivery of mutant huntingtin-lowering antisense oligonucleotides to the brain by intranasally administered apolipoprotein A-I nanodisks

鼻腔给药 亨廷顿蛋白 纹状体 嗅球 药理学 中枢神经系统 医学 基底神经节 亨廷顿病 神经科学 生物 病理 内科学 疾病 多巴胺
作者
Amirah E.-E. Aly,Nicholas S. Caron,Hailey Findlay Black,Mandi E. Schmidt,Thomas Anderson,Seung‐Hyun Ko,Helen J. E. Baddeley,Lisa M. Anderson,Lorenzo Casal,Reza S.M. Rahavi,Dale D. O. Martin,Michael R. Hayden
出处
期刊:Journal of Controlled Release [Elsevier]
卷期号:360: 913-927 被引量:5
标识
DOI:10.1016/j.jconrel.2023.07.027
摘要

Lowering mutant huntingtin (mHTT) in the central nervous system (CNS) using antisense oligonucleotides (ASOs) is a promising approach currently being evaluated in clinical trials for Huntington disease (HD). However, the therapeutic potential of ASOs in HD patients is limited by their inability to cross the blood-brain barrier (BBB). In non-human primates, intrathecal infusion of ASOs results in limited brain distribution, with higher ASO concentrations in superficial regions and lower concentrations in deeper regions, such as the basal ganglia. To address the need for improved delivery of ASOs to the brain, we are evaluating the therapeutic potential of apolipoprotein A-I nanodisks (apoA-I NDs) as novel delivery vehicles for mHTT-lowering ASOs to the CNS after intranasal administration. Here, we have demonstrated the ability of apoA-I nanodisks to bypass the BBB after intranasal delivery in the BACHD model of HD. Following intranasal administration of apoA-I NDs, apoA-I protein levels were elevated along the rostral-caudal brain axis, with highest levels in the most rostral brain regions including the olfactory bulb and frontal cortex. Double-label immunohistochemistry indicates that both the apoA-I and ASO deposit in neurons. Most importantly, a single intranasal dose of apoA-I ASO-NDs significantly reduces mHTT levels in the brain regions most affected in HD, namely the cortex and striatum. This approach represents a novel non-invasive means for improving delivery and brain distribution of oligonucleotide therapies and enhancing likelihood of efficacy. Improved ASO delivery to the brain has widespread application for treatment of many other CNS disorders.
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