Anatomical circuitry is the foundation by which information travels within the brain. Therefore, comprehensive wiring diagrams are fundamental for understanding how circuits control complex behavioral and cognitive processes. However, only sparse connectivity datasets exist for mammalian model species, and most are collated from tract tracing literature. This is problematic due to the large variety of methods, targeted areas, nomenclature, and assessment of connection strengths by different labs. Instead, at the Allen Institute, we created an entirely new, standardized, publicly and freely available, dataset (Mouse Connectivity Atlas; ://connectivity.brain-map.org) based on modern anterograde axon tracing and high-throughput 2-photon imaging methods to visualize inter-areal and genetically defined cell type-specific projections across the entire young adult mouse brain from ~300 regions. The Mouse Connectivity Atlas data reveals general organizational principles in healthy brains, but many details are still missing. For example, subclasses of neurons within a region projecting to either single or multiple targets are not always defined, nor are the layers of origin of cortical input neurons to specific targets defined. Higher resolution descriptions of structural connection patterns at the cell type, rather than areal, level will enable more accurate modeling and hypotheses on cortical information processing and cognition in health and disease. In neurodegenerative diseases that rob patients of cognitive abilities, such as Alzheimer's disease (AD), pathology spreads in selectively vulnerable regions in specific patterns that resemble, but do not exactly duplicate, network architecture. Taking into account specific cortical projection pathways could thus provide a better structural framework for understanding, predicting, and treating disease. We propose to enhance the Mouse Connectivity Atlas through focused anatomical tracing of whole-brain axon pathways from neurons defined by their projection targets within and outside of disease- relevant large-scale cortical networks. This will be accomplished through the development of a combined viral- based retrograde and anterograde intersectional fluorescent labeling strategy, and our established, successful high-throughput imaging and informatics platform. We will densely survey and map cell type projections defined by target regions in the mouse default mode-like and hippocampal networks, which participate in essential normal cognitive tasks and are vulnerable to AD. New data will be integrated into Allen Institute online resources, providing external users access to raw 2-D images, annotated 3-D projection models, and other analysis tools. We will specifically test the prediction that anatomical classes of projection neurons within an area belonging to the functionally-defined default mode network preferentially connect to other areas within the network. We also propose to use this foundational dataset as a guide for generating and analyzing a brain- wide cell type structural connectivity matrix for an AD mouse model, which could facilitate research in the AD community on disease-related network dysfunction and propagation of pathology.

Public Health Relevance

Modern brain mapping projects share a goal of creating circuit diagrams with more detail than previously possible, expecting that any additional information will help illuminate functional implications of healthy brain organization and network breakdown in disease. We will develop and apply new, high-throughput methods for adding critical details of anatomical connections formed by specific neuron types in large-scale networks involved in cognition, and map brain-wide structural connectivity patterns in a widely used mouse model of Alzheimer's disease.

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG047589-04
Application #
9269950
Study Section
Neuroscience and Ophthalmic Imaging Technologies Study Section (NOIT)
Program Officer
Wise, Bradley C
Project Start
2014-05-15
Project End
2019-04-30
Budget Start
2017-05-15
Budget End
2018-04-30
Support Year
4
Fiscal Year
2017
Total Cost
$635,731
Indirect Cost
$273,491
Name
Allen Institute
Department
Type
Research Institutes
DUNS #
137210949
City
Seattle
State
WA
Country
United States
Zip Code
98103