Engineered AAVs for Efficient Noninvasive Gene Delivery to the Central and Peripheral Nervous Systems

Overview

Journal Nat Neurosci

Date 2017 Jul 4

PMID 28671695

Citations 683

Authors

Ken Y Chan

Min J Jang

Bryan B Yoo

Alon Greenbaum

Namita Ravi

Wei-Li Wu

Luis Sanchez-Guardado

Carlos Lois

Sarkis K Mazmanian

Benjamin E Deverman

Viviana Gradinaru

Affiliations

Soon will be listed here.

Abstract

Adeno-associated viruses (AAVs) are commonly used for in vivo gene transfer. Nevertheless, AAVs that provide efficient transduction across specific organs or cell populations are needed. Here, we describe AAV-PHP.eB and AAV-PHP.S, capsids that efficiently transduce the central and peripheral nervous systems, respectively. In the adult mouse, intravenous administration of 1 × 10 vector genomes (vg) of AAV-PHP.eB transduced 69% of cortical and 55% of striatal neurons, while 1 × 10 vg of AAV-PHP.S transduced 82% of dorsal root ganglion neurons, as well as cardiac and enteric neurons. The efficiency of these vectors facilitates robust cotransduction and stochastic, multicolor labeling for individual cell morphology studies. To support such efforts, we provide methods for labeling a tunable fraction of cells without compromising color diversity. Furthermore, when used with cell-type-specific promoters and enhancers, these AAVs enable efficient and targetable genetic modification of cells throughout the nervous system of transgenic and non-transgenic animals.

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