Abstract

This is a new R01 proposal addressing neural pathways and gene expression in habenula- midbrain circuits. The habenula is a dorsal thalamic nucleus consisting of medial (MH) and lateral (LH) subnuclei that participate in distinct neural pathways. The MH and LH both send their output fibers to the ventral midbrain via the prominent fasciculus retroflexus (FR), but only the LH directly innervates midbrain dopamine (DA) and serotonin (5HT) systems, while the MH projects first to the interpeduncular nucleus (IP), which in turn projects to ventral midbrain. Recent behavioral experiments suggest strong functional interactions between the habenula-midbrain pathway and the monoamine systems, with major implications for mood disorders, cognitive disorders, and addiction. Using microarrays and bioinformatic approaches, we have recently shown that molecular markers identify subpopulations of neurons in the MH and LH which suggest functional heterogeneity within these nuclei. Further progress in understanding habenula function will require a much better understanding of these distinct molecular classes of habenula neurons, including their anatomic and functional connectivity, which are not accessible to conventional tract-tracing methods. Here we propose three Specific Aims that will explore habenula circuits and rapidly delineate the connections of defined populations of neurons in the MH, LH and IP. These experiments are planned in a short time-frame (3 years) and with cost-effective use of existing tools, including genomic and bioinformatic assets from the Gensat and Allen Brain Institute brain mapping projects.
Aim 1. Test the hypothesis that specific subpopulations of MH and LH neurons participate in distinct neural pathways. Use transgenic mice with LacZ, GFP, and Cre reporters to trace the projections of genetically defined classes of MH, LH, and IP neurons to the midbrain. Available lines target the Brn3a, Gpr151, Tac2/SK, Slc18a3, Chrnb4, Prokr2, Chrna5, Tac1/SP, and Chat genes.
Aim 2. Test the hypothesis that the LH provides input to the mesolimbic DA system via GABAergic neurons of the mesopontine rostromedial tegmental nucleus (RMTg) in mice as it does in rats. Localize the mouse RMTg using cFos induction, anterograde tract tracing from the LH, and GABA marker expression. Identify the LH subpopulations projecting to the RMTg using transgenic tracing.
Aim 3. In collaboration with the Allen Institute, use bioinformatic analysis to test the hypothesis that key nodes of the habenula pathway, specifically the forebrain septal nuclei, LH, IP and RMTg, have distinctive gene expression profiles, as previously demonstrated for the MH. These gene expression profiles will form the basis for the genetic manipulation of habenula pathways in future studies.

Public Health Relevance

Recent studies in rodents, primates and humans have implicated a poorly understood brain region, the habenula, in the perception of punishment or the absence of an expected reward. Circuits from the habenula to the midbrain, mediating these responses, may play a role in depression and addiction. The habenula is a complex brain region, containing multiple types of neurons, and cannot be understood as a single unit. We propose to use transgenic mice to show how distinct kinds of habenula neurons are """"""""wired"""""""" to the regions of the brainstem regulating reward, motivation and mood.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
1R01MH093667-01
Application #
8083850
Study Section
Neurobiology of Motivated Behavior Study Section (NMB)
Program Officer
Vicentic, Aleksandra
Project Start
2011-06-10
Project End
2014-03-31
Budget Start
2011-06-10
Budget End
2012-03-31
Support Year
1
Fiscal Year
2011
Total Cost
$390,000
Indirect Cost

  Institution

Name
Seattle Children's Hospital
Department
Type
DUNS #
048682157
City
Seattle
State
WA
Country
United States
Zip Code
98105

  Publications

Hsu, Yun-Wei A; Gile, Jennifer J; Perez, Jazmine G et al. (2017) The Dorsal Medial Habenula Minimally Impacts Circadian Regulation of Locomotor Activity and Sleep. J Biol Rhythms 32:444-455
Quina, Lely A; Harris, Julie; Zeng, Hongkui et al. (2017) Specific connections of the interpeduncular subnuclei reveal distinct components of the habenulopeduncular pathway. J Comp Neurol 525:2632-2656
Hsu, Yun-Wei A; Morton, Glenn; Guy, Elizabeth G et al. (2016) Dorsal Medial Habenula Regulation of Mood-Related Behaviors and Primary Reinforcement by Tachykinin-Expressing Habenula Neurons. eNeuro 3:
Quina, Lely A; Tempest, Lynne; Ng, Lydia et al. (2015) Efferent pathways of the mouse lateral habenula. J Comp Neurol 523:32-60
Han, V Z; Magnus, G; Zhang, Y et al. (2014) Bidirectional modulation of deep cerebellar nuclear cells revealed by optogenetic manipulation of inhibitory inputs from Purkinje cells. Neuroscience 277:250-66
Hsu, Yun-Wei A; Wang, Si D; Wang, Shirong et al. (2014) Role of the dorsal medial habenula in the regulation of voluntary activity, motor function, hedonic state, and primary reinforcement. J Neurosci 34:11366-84
Hsu, Yun-Wei A; Tempest, Lynne; Quina, Lely A et al. (2013) Medial habenula output circuit mediated by ?5 nicotinic receptor-expressing GABAergic neurons in the interpeduncular nucleus. J Neurosci 33:18022-35
Madisen, Linda; Mao, Tianyi; Koch, Henner et al. (2012) A toolbox of Cre-dependent optogenetic transgenic mice for light-induced activation and silencing. Nat Neurosci 15:793-802