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基于犬2型腺病毒(CAV2)载体对非转基因大鼠蓝斑进行光遗传学激活的可行性:对功能研究的启示

Feasibility of Canine Adenovirus Type 2 (CAV2) Based Vector for the Locus Coeruleus Optogenetic Activation in Non-Transgenic Rats: Implications for Functional Studies.

作者信息

Kabanova Anna, Cavani Elena, Logothetis Nikos K, Eschenko Oxana

机构信息

Department of Physiology of Cognitive Processes, Max Planck Institute for Biological Cybernetics, 72076 Tübingen, Germany.

Division of Imaging Science and Biomedical Engineering, University of Manchester, Manchester M13 9PT, UK.

出版信息

Brain Sci. 2022 Jul 10;12(7):904. doi: 10.3390/brainsci12070904.

Abstract

The locus coeruleus norepinephrine (LC-NE) system modulates many visceral and cognitive functions, while LC-NE dysfunction leads to neurological and neurodegenerative conditions such as sleep disorders, depression, ADHD, or Alzheimer's disease. Innovative viral-vector and gene-engineering technology combined with the availability of cell-specific promoters enabled regional targeting and selective control over phenotypically specific populations of neurons. We transduced the LC-NE neurons in adult male rats by delivering the canine adenovirus type 2-based vector carrying the NE-specific promoter PRSx8 and a light-sensitive channelrhodopsin-2 receptor (ChR2) directly in the LC or retrogradely from the LC targets. The highest ChR2 expression level was achieved when the virus was delivered medially to the trigeminal pathway and ~100 μm lateral to the LC. The injections close or directly in the LC compromised the tissue integrity and NE cell phenotype. Retrograde labeling was more optimal given the transduction of projection-selective subpopulations. Our results highlight a limited inference of ChR2 expression from representative cases to the entire population of targeted cells. The actual fraction of manipulated neurons appears most essential for an adequate interpretation of the study outcome. The actual fraction of manipulated neurons appears most essential for an adequate interpretation of the study outcome. Thus, besides the cell-type specificity and the transduction efficiency, the between-subject variability in the proportion of the remaining viral-transduced targeted cell population must be considered in any functional connectivity study.

摘要

蓝斑去甲肾上腺素(LC-NE)系统调节许多内脏和认知功能,而LC-NE功能障碍会导致神经和神经退行性疾病,如睡眠障碍、抑郁症、注意力缺陷多动障碍或阿尔茨海默病。创新的病毒载体和基因工程技术与细胞特异性启动子的可用性相结合,实现了对表型特异性神经元群体的区域靶向和选择性控制。我们通过直接在蓝斑内或从蓝斑靶点逆行递送携带NE特异性启动子PRSx8和光敏感通道视紫红质-2受体(ChR2)的犬2型腺病毒载体,转导成年雄性大鼠的LC-NE神经元。当病毒向内侧递送至三叉神经通路且在蓝斑外侧约100μm处时,ChR2表达水平最高。在蓝斑附近或直接在蓝斑内注射会损害组织完整性和NE细胞表型。考虑到投射选择性亚群的转导,逆行标记更为理想。我们的结果强调了从代表性案例到整个靶向细胞群体的ChR2表达推断有限。实际被操纵的神经元比例对于充分解释研究结果似乎最为关键。实际被操纵的神经元比例对于充分解释研究结果似乎最为关键。因此,除了细胞类型特异性和转导效率外,在任何功能连接性研究中都必须考虑剩余病毒转导靶向细胞群体比例的个体间变异性。

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