Directed evolution of adeno-associated virus for efficient gene delivery to microglia

被引:0
作者
Rui Lin
Youtong Zhou
Ting Yan
Ruiyu Wang
Heng Li
Zhaofa Wu
Xinshuang Zhang
Xiangyu Zhou
Fei Zhao
Li Zhang
Yulong Li
Minmin Luo
机构
[1] National Institute of Biological Sciences (NIBS),School of Life Sciences
[2] Chinese Institute for Brain Research,Tsinghua
[3] Tsinghua University,Peking Center for Life Sciences
[4] Tsinghua University,School of Life Sciences
[5] Peking University,undefined
[6] Tsinghua Institute of Multidisciplinary Biomedical Research (TIMBR),undefined
来源
Nature Methods | 2022年 / 19卷
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摘要
As the resident immune cells in the central nervous system (CNS), microglia orchestrate immune responses and dynamically sculpt neural circuits in the CNS. Microglial dysfunction and mutations of microglia-specific genes have been implicated in many diseases of the CNS. Developing effective and safe vehicles for transgene delivery into microglia will facilitate the studies of microglia biology and microglia-associated disease mechanisms. Here, we report the discovery of adeno-associated virus (AAV) variants that mediate efficient in vitro and in vivo microglial transduction via directed evolution of the AAV capsid protein. These AAV-cMG and AAV-MG variants are capable of delivering various genetic payloads into microglia with high efficiency, and enable sufficient transgene expression to support fluorescent labeling, Ca2+ and neurotransmitter imaging and genome editing in microglia in vivo. Furthermore, single-cell RNA sequencing shows that the AAV-MG variants mediate in vivo transgene delivery without inducing microglia immune activation. These AAV variants should facilitate the use of various genetically encoded sensors and effectors in the study of microglia-related biology.
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页码:976 / 985
页数:9
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