Literature DB >> 33199411

Regulatory Elements Inserted into AAVs Confer Preferential Activity in Cortical Interneurons.

Anna N Rubin1, Ruchi Malik2, Kathleen K A Cho2, Kenneth J Lim1, Susan Lindtner1, Sarah E Robinson Schwartz2, Daniel Vogt1, Vikaas S Sohal3, John L R Rubenstein4.   

Abstract

Cortical interneuron (CIN) dysfunction is thought to play a major role in neuropsychiatric conditions like epilepsy, schizophrenia and autism. It is therefore essential to understand how the development, physiology, and functions of CINs influence cortical circuit activity and behavior in model organisms such as mice and primates. While transgenic driver lines are powerful tools for studying CINs in mice, this technology is limited in other species. An alternative approach is to use viral vectors such as AAV, which can be used in multiple species including primates and also have potential for therapeutic use in humans. Thus, we sought to discover gene regulatory enhancer elements (REs) that can be used in viral vectors to drive expression in specific cell types. The present study describes the systematic genome-wide identification of putative REs (pREs) that are preferentially active in immature CINs by histone modification chromatin immunoprecipitation and sequencing (ChIP-seq). We evaluated two novel pREs in AAV vectors, alongside the well-established Dlx I12b enhancer, and found that they drove CIN-specific reporter expression in adult mice. We also showed that the identified Arl4d pRE could drive sufficient expression of channelrhodopsin for optogenetic rescue of behavioral deficits in the Dlx5/6 +/- mouse model of fast-spiking CIN dysfunction.
Copyright © 2020 Rubin et al.

Entities:  

Keywords:  AAV; cortical interneurons; enhancers; fast spiking; regular spiking

Mesh:

Substances:

Year:  2020        PMID: 33199411      PMCID: PMC7768279          DOI: 10.1523/ENEURO.0211-20.2020

Source DB:  PubMed          Journal:  eNeuro        ISSN: 2373-2822


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