TRANSCRIPTOMIC NEURONAL SUBTYPE-SPECIFIC RESPONSES TO TAU OVEREXPRESSION IN THE ENTORHINAL CORTEX POINT TO NEW PATHWAYS FOR UNDERSTANDING EARLY ALZHEIMER'S DISEASE PATHOGENESIS
Kavli Institute for Systems Neuroscience
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Poster Board
PS02-07PM-393
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We therefore injected AAVs expressing wildtype human Tau (hTau) and GFP under the control of the human synapsin promoter in both wildtype and AD rats such that hTau was overexpressed in a variety of neuronal cell types in the entorhinal and surrounding cortices. We then followed the development of pathological tau species in different neuronal subtypes with both immunohistochemistry and snRNAseq. Immunohistochemistry showed different pathological tau species are generated at different rates in different neuronal subtypes. We found that, as expected, the presumed cognate neurons of human pre-alpha cells were highly prone to turning hTau into pathological tau species. Surprisingly, other entorhinal neurons were even more susceptible, especially with certain antigens. Transcriptomic analysis of the snRNAseq data corroborates this, with entorhinal neuronal subtypes showing the greatest response to hTau overexpression in terms of changes in gene expression. We present gene-network analyses providing mechanistic insight into the enhanced vulnerability of distinct entorhinal celltypes to the development of tauopathy.
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