Combined injection of rAAV with mannitol enhances gene expression in the rat brain

Thumbnail Image
Date
2000-09-06
DOI
10.1006/mthe.2001.0246
Open Access Location
https://www.sciencedirect.com/science/article/pii/S1525001601902461?via%3Dihub
Authors
Journal Title
Journal ISSN
Volume Title
Publisher
Cell Press
Rights
Under a Creative Commons license
Abstract
Recombinant adeno-associated viruses (rAAV) are highly efficient vectors for gene transfer into the central nervous system (CNS). However, a major hurdle for gene delivery to the mammalian brain is to achieve high-level transduction in target cells beyond the immediate injection site. Therefore, in addition to improvements in expression cassettes and viral titers, optimal injection parameters need to be defined. Here, we show that previous studies of somatic cell gene transfer to the mammalian brain have used suboptimal injection parameters, with even the lowest reported perfusion rates still excessively fast. Moreover, we evaluated the effect of local administration of mannitol to further enhance transgene expression and vector spread. Ultraslow microperfusion of rAAV, i.e., <33 nl/min, resulted in significantly higher gene expression and less injury of surrounding tissue than the previously reported rates of 100 nl/min or faster. Co-infusion of mannitol facilitated gene transfer to neurons, increasing both the total number and the distribution of transduced cells by 200-300%. Gene transfer studies in the CNS using rAAV should use very slow infusion rates and combined injection with mannitol to maximize transduction efficiency and spread.
Description
Keywords
rAAV, mannitol, injection parameters, CNS, gene therapy
Citation
MOLECULAR THERAPY, 2001, 3 (2), pp. 225 - 232
URI
Collections
Journal Articles