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Published May 1, 2017 | Accepted Version
Journal Article Open

AAV-mediated delivery of optogenetic constructs to the macaque brain triggers humoral immune responses

Abstract

Gene delivery to the primate central nervous system via recombinant adeno-associated viral vectors (AAV) allows neurophysiologists to control and observe neural activity precisely. A current limitation of this approach is variability in vector transduction efficiency. Low levels of transduction can foil experimental manipulations, prompting vector readministration. The ability to make multiple vector injections into the same animal, even in cases where successful vector transduction has already been achieved, is also desirable. However, vector readministration has consequences for humoral immunity and gene delivery that depend on vector dosage and route of administration in complex ways. As part of optogenetic experiments in rhesus monkeys, we analyzed blood sera collected before and after AAV injections into the brain and quantified neutralizing antibodies to AAV using an in vitro assay. We found that injections of AAV1 and AAV9 vectors elevated neutralizing antibody titers consistently. These immune responses were specific to the serotype injected and were long lasting. These results demonstrate that optogenetic manipulations in monkeys trigger immune responses to AAV capsids, suggesting that vector readministration may have a higher likelihood of success by avoiding serotypes injected previously.

Additional Information

© 2016 Journal of Neurophysiology. Submitted 28 September 2016; accepted in final form 10 February 2017. This work was supported by National Institutes of Health Grants EY-024362 and OD-010425. No conflicts of interest, financial or otherwise, are declared by the authors. Author Contributions: S.D.M. and Y.E.-S. performed experiments; S.D.M. and Y.E.-S. analyzed data; S.D.M., Y.E.-S., and G.D.H. interpreted results of experiments; S.D.M. and Y.E.-S. prepared figures; S.D.M., Y.E.-S., and G.D.H. drafted manuscript; S.D.M., Y.E.-S., and G.D.H. edited and revised manuscript; S.D.M., Y.E.-S., and G.D.H. approved final version of manuscript. We thank the veterinary staff at the Washington National Primate Center for assistance with blood serum collection and Donna Prunkard at the University of Washington Department of Pathology Flow Cytometry Core Facility for assistance with FACS analysis. We also thank Adam Kohn and Mehrdad Jazayeri for helpful comments on the manuscript.

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Accepted Version - jn.00780.2016.full.pdf

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