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利用近红外光激活蛋白偶联纳米颗粒进行高效的空间靶向基因编辑,用于脑科学应用。

Efficient spatially targeted gene editing using a near-infrared activatable protein-conjugated nanoparticle for brain applications.

机构信息

CNC-Center for Neurosciences and Cell Biology, University of Coimbra, Coimbra, Portugal.

Faculty of Medicine, University of Coimbra, Coimbra, Portugal.

出版信息

Nat Commun. 2022 Jul 16;13(1):4135. doi: 10.1038/s41467-022-31791-6.

Abstract

Spatial control of gene expression is critical to modulate cellular functions and deconstruct the function of individual genes in biological processes. Light-responsive gene-editing formulations have been recently developed; however, they have shown limited applicability in vivo due to poor tissue penetration, limited cellular transfection and the difficulty in evaluating the activity of the edited cells. Here, we report a formulation composed of upconversion nanoparticles conjugated with Cre recombinase enzyme through a photocleavable linker, and a lysosomotropic agent that facilitates endolysosomal escape. This formulation allows in vitro spatial control in gene editing after activation with near-infrared light. We further demonstrate the potential of this formulation in vivo through three different paradigms: (i) gene editing in neurogenic niches, (ii) gene editing in the ventral tegmental area to facilitate monitoring of edited cells by precise optogenetic control of reward and reinforcement, and (iii) gene editing in a localized brain region via a noninvasive administration route (i.e., intranasal).

摘要

空间控制基因表达对于调节细胞功能和剖析生物过程中单个基因的功能至关重要。光响应基因编辑配方最近已经开发出来;然而,由于组织穿透性差、细胞转染有限以及编辑细胞活性评估困难,它们在体内的应用受到限制。在这里,我们报告了一种由上转换纳米粒子与 Cre 重组酶通过光裂解连接子偶联而成的制剂,以及一种溶酶体增敏剂,可促进内体/溶酶体逃逸。这种配方允许在近红外光激活后进行体外空间控制基因编辑。我们通过三种不同的范例进一步证明了该配方在体内的潜力:(i)神经发生龛中的基因编辑,(ii)腹侧被盖区中的基因编辑,以通过精确的光遗传学控制奖励和强化来促进编辑细胞的监测,以及(iii)通过非侵入性给药途径(即鼻内)在局部脑区进行基因编辑。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dcf8/9287341/045e9d7c619d/41467_2022_31791_Fig1_HTML.jpg

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