4.7 Article

Toxic and Phenotypic Effects of AAV_Cre Used to Transduce Mesencephalic Dopaminergic Neurons

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MDPI
DOI: 10.3390/ijms23169462

关键词

toxicity; stereotaxic injection; Cre recombinase; dopamine; ventral tegmental area; adeno-associated virus; tyrosine hydroxylase

资金

  1. Intramural Research Program of the Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) [ZIA-HD000711]

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Microinjection of AAV_Cre in the ventral tegmental area can have neurotoxic effects on dopaminergic neurons and elicit behavioral abnormalities, which are independent of ErbB4 Cyt-1 recombination and also observed in wild-type controls. These non-specific effects can be prevented by reducing viral titers while maintaining sufficient recombination activity.
A popular approach to spatiotemporally target genes using the loxP/Cre recombination system is stereotaxic microinjection of adeno-associated virus (AAV) expressing Cre recombinase (AAV_Cre) in specific neuronal structures. Here, we report that AAV_Cre microinjection in the ventral tegmental area (VTA) of ErbB4 Cyt-1-floxed (ErbB4 Cyt-1(fl/fl)) mice at titers commonly used in the literature (similar to 10(12)-10(13) GC/mL) can have neurotoxic effects on dopaminergic neurons and elicit behavioral abnormalities. However, these effects of AAV_Cre microinjection are independent of ErbB4 Cyt-1 recombination because they are also observed in microinjected wild-type (WT) controls. Mice microinjected with AAV_Cre (10(12)-10(13) GC/mL) exhibit reductions of tyrosine hydroxylase (TH) and dopamine transporter (DAT) expression, loss of dopaminergic neurons, and they behaviorally become hyperactive, fail to habituate in the open field and exhibit sensorimotor gating deficits compared to controls microinjected with AAV GFP. Importantly, these AAV_Cre non-specific effects are: (1) independent of serotype, (2) occur with vectors expressing either Cre or Cre-GFP fusion protein and (3) preventable by reducing viral titers by 1000-fold (10(10) GC/mL), which retains sufficient recombination activity to target floxed genes. Our studies emphasize the importance of including AAV_Cre-injected WT controls in experiments because recombination-independent effects on gene expression, neurotoxicity and behaviors could be erroneously attributed to consequences of gene ablation.

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