Affiliation:
1. Département de Neuroscience Université de Montréal Montréal Québec Canada
2. CHU Sainte‐Justine Research Center Montréal Québec Canada
3. Oramacell Paris France
Abstract
AbstractThe hippocampus (HP) receives neurochemically diverse inputs from the raphe nuclei, including glutamatergic axons characterized by the expression of the vesicular glutamate transporter type 3 (VGLUT3). These raphe‐HP VGLUT3 projections have been suggested to play a critical role in HP functions, yet a complete anatomical overview of raphe VGLUT3 projections to the forebrain, and in particular to the HP, is lacking. Using anterograde viral tracing, we describe largely nonoverlapping VGLUT3‐positive projections from the dorsal raphe (DR) and median raphe (MnR) to the forebrain, with the HP receiving inputs from the MnR. A limited subset of forebrain regions such as the amygdaloid complex, claustrum, and hypothalamus receives projections from both the DR and MnR that remain largely segregated. This highly complementary anatomical pattern suggests contrasting roles for DR and MnR VGLUT3 neurons. To further analyze the topography of VGLUT3 raphe projections to the HP, we used retrograde tracing and found that HP‐projecting VGLUT3‐positive neurons (VGLUT3HP) distribute over several raphe subregions (including the MnR, paramedian raphe, and B9 cell group) and lack co‐expression of serotonergic markers. Strikingly, double retrograde tracing experiments unraveled two parallel streams of VGLUT3‐positive projections targeting the dorsal and ventral poles of the HP. These results demonstrate highly organized and segregated VGLUT3‐positive projections to the HP, suggesting independent modulation of HP functions such as spatial memory and emotion‐related behavior.
Funder
Natural Sciences and Engineering Research Council of Canada
Brain and Behavior Research Foundation
Cited by
2 articles.
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