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鉴定阳离子聚合物基因递送至人 T 细胞的关键障碍。

Identifying key barriers in cationic polymer gene delivery to human T cells.

机构信息

Department of Bioengineering and Molecular Engineering and Sciences Institute, University of Washington, Seattle, WA, USA.

出版信息

Biomater Sci. 2019 Feb 26;7(3):789-797. doi: 10.1039/c8bm01262h.

Abstract

T cells have emerged as a therapeutically-relevant target for ex vivo gene delivery and editing. However, most commercially available reagents cannot transfect T cells and designing cationic polymers for non-viral gene delivery to T cells has resulted in moderate success. Here, we assess various barriers to successful gene transfer in the Jurkat human T cell line and primary human T cells. Using two polymers previously developed by our group, we show that uptake is one barrier to gene delivery in primary human T cells but is not predictive of successful gene delivery. We then probe intracellular pathways for barriers to gene transfer including endosomal acidification, autophagy, and immune sensing pathways. We find that endosomal acidification is slower and not as robust in human T cells compared to the model HeLa human cell line commonly used to evaluate cationic polymers for gene delivery. These studies inform the future design of cationic polymers for non-viral gene delivery to T cells, specifically, to rely on alternative endosomal release mechanisms rather than on pH-triggered release.

摘要

T 细胞已成为体外基因传递和编辑的治疗相关靶标。然而,大多数市售试剂无法转染 T 细胞,并且为非病毒基因传递设计阳离子聚合物也只是取得了中等程度的成功。在这里,我们评估了 Jurkat 人 T 细胞系和原代人 T 细胞中成功基因转移的各种障碍。使用我们小组之前开发的两种聚合物,我们表明摄取是原代人 T 细胞中基因传递的一个障碍,但不能预测成功的基因传递。然后,我们探讨了细胞内途径中的基因转移障碍,包括内体酸化、自噬和免疫感应途径。我们发现与常用作评估阳离子聚合物基因传递的模型 HeLa 人细胞系相比,人 T 细胞中的内体酸化较慢且不那么稳健。这些研究为未来用于 T 细胞非病毒基因传递的阳离子聚合物的设计提供了信息,具体来说,要依赖替代的内体释放机制,而不是 pH 触发的释放。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/91c5/6391219/22c1ef5d5048/nihms-1006565-f0002.jpg

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