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靶向囊泡转运以改善分子货物的非病毒递送。

Redirecting Vesicular Transport to Improve Nonviral Delivery of Molecular Cargo.

机构信息

Department of Biomedical Engineering, Duke University, Durham, NC, 27708, USA.

Center for Advanced Genomic Technologies, Duke University, Durham, NC, 27708, USA.

出版信息

Adv Biosyst. 2020 Aug;4(8):e2000059. doi: 10.1002/adbi.202000059. Epub 2020 Jul 21.

Abstract

Cell engineering relies heavily on viral vectors for the delivery of molecular cargo into cells due to their superior efficiency compared to nonviral ones. However, viruses are immunogenic and expensive to manufacture, and have limited delivery capacity. Nonviral delivery approaches avoid these limitations but are currently inefficient for clinical applications. This work demonstrates that the efficiency of nonviral delivery of plasmid DNA, mRNA, Sleeping Beauty transposon, and ribonucleoprotein can be significantly enhanced through pretreatment of cells with the nondegradable sugars (NDS), such as sucrose, trehalose, and raffinose. The enhancement is mediated by the incorporation of the NDS into cell membranes, causing enlargement of lysosomes and formation of large (>500 nm) amphisome-like bodies (ALBs). The changes in subcellular structures redirect transport of cargo to ALBs rather than to lysosomes, reducing cargo degradation in cells. The data indicate that pretreatment of cells with NDS is a promising approach to improve nonviral cargo delivery in biomedical applications.

摘要

细胞工程在将分子货物递送到细胞内时严重依赖病毒载体,因为它们比非病毒载体具有更高的效率。然而,病毒具有免疫原性,且制造成本高,并且递送容量有限。非病毒递送方法避免了这些限制,但目前在临床应用中效率不高。这项工作表明,通过用非降解糖(如蔗糖、海藻糖和棉子糖)预处理细胞,可以显著提高质粒 DNA、mRNA、Sleeping Beauty 转座子和核糖核蛋白的非病毒递送效率。这种增强是通过将 NDS 掺入细胞膜介导的,导致溶酶体增大并形成大(>500nm)的类 Amphisoome 体(ALB)。亚细胞结构的变化将货物的运输重新导向到 ALB 而不是溶酶体,从而减少了细胞内货物的降解。这些数据表明,用 NDS 预处理细胞是提高生物医学应用中非病毒货物递送的有前途的方法。

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