Exploring brain circuitry with neurotropic viruses: new horizons in neuroanatomy.

Abstract

There have been substantial advances in methods for defining connections among neurons over the past quarter century. However, most tracers have been limited in their ability to define populations of functionally related neurons that contribute to a multisynaptic circuit because they are not transported across synapses. As a result, the large body of literature that has employed these tracers has established regional associations between regions that must be further explored with electron microscopy and electrophysiological methods to define the synaptic relations among constituent neurons. Recently, neurotropic alpha herpesviruses have been used to visualize ensembles of neurons that contribute to polysynaptic networks. These pathogens invade permissive cells, replicate, and pass transynaptically to infect other neurons. In effect, the viruses become self-amplifying tracers whose natural tropism and invasiveness define populations of functionally related neurons. The recent increase in the use of this experimental approach has emerged from advances in our understanding of the life cycle of these viruses and the resulting evidence in support of specific transynaptic passage of progeny virus rather than infection by lytic release into the extracellular space. This article reviews the advances that have made this a viable experimental approach and considers ways in which this method has been creatively used to illuminate aspects of nervous system circuit organization that could not be defined with conventional tracers.