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与ImmTOR纳米颗粒混合的腺相关病毒(AAV)载体初始剂量和重复剂量下肝脏定向转基因表达的增强。

Enhancement of liver-directed transgene expression at initial and repeat doses of AAV vectors admixed with ImmTOR nanoparticles.

作者信息

Ilyinskii Petr O, Michaud Alicia M, Roy Christopher J, Rizzo Gina L, Elkins Stephanie L, Capela Teresa, Chowdhury Aparajita C, Leung Sheldon S, Kishimoto Takashi K

机构信息

Selecta Biosciences, Watertown, MA 02472, USA.

出版信息

Sci Adv. 2021 Feb 24;7(9). doi: 10.1126/sciadv.abd0321. Print 2021 Feb.

Abstract

Systemic AAV (adeno-associated virus) gene therapy is a promising approach for the treatment of inborn errors of metabolism, but questions remain regarding its potency and durability. Tolerogenic ImmTOR nanoparticles encapsulating rapamycin have been shown to block the formation of neutralizing anti-capsid antibodies, thereby enabling vector re-administration. Here, we further demonstrate that ImmTOR admixed with AAV vectors also enhances hepatic transgene expression at the initial dose of AAV vector, independent of its effects on adaptive immunity. ImmTOR enhances AAV trafficking to the liver, resulting in increased hepatic vector copy numbers and transgene mRNA expression. Enhanced transgene expression occurs through a mechanism independent of the AAV receptor and cannot be replicated in vivo with free rapamycin or empty nanoparticles. The multipronged mechanism of ImmTOR action makes it an attractive candidate to enable more efficient transgene expression at first dose while simultaneously inhibiting adaptive responses against AAV to enable repeat dosing.

摘要

全身性腺相关病毒(AAV)基因疗法是治疗先天性代谢缺陷的一种很有前景的方法,但关于其效力和持久性仍存在问题。已证明封装雷帕霉素的耐受性ImmTOR纳米颗粒可阻止中和性抗衣壳抗体的形成,从而能够再次施用载体。在这里,我们进一步证明,与AAV载体混合的ImmTOR在AAV载体的初始剂量下也能增强肝脏转基因表达,这与其对适应性免疫的影响无关。ImmTOR增强了AAV向肝脏的转运,导致肝脏载体拷贝数和转基因mRNA表达增加。转基因表达的增强是通过一种独立于AAV受体的机制发生的,游离雷帕霉素或空纳米颗粒在体内无法复制这种增强作用。ImmTOR作用的多方面机制使其成为一个有吸引力的候选者,能够在首次给药时实现更有效的转基因表达,同时抑制针对AAV的适应性反应以实现重复给药。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/556e/7904260/4fec2284acc6/abd0321-F1.jpg

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