Feedback amplification between Retrotransposons/endogenous retroviruses and TDP-43 in Alzheimers related dementias
State University New York Stony Brook, Stony Brook NY
Investigators
Linked publications & trials
Abstract
PROJECT ABSTRACT This proposal investigates a novel idea to explain how TDP-43 protein pathology is amplified and spread between glia and neurons after initiation of disease. TDP-43 aggregation pathology is a core feature of a suite of neurodegenerative disorders including frontotemporal dementia, Alzheimerâs and amyotrophic lateral sclerosis. We propose and will test the hypothesis that retrotransposons and endogenous retroviruses are both activated by TDP-43 pathology and can be upstream initiators of such pathology. We also will test the idea that these mobile elements contribute a mechanism of inter-cellular spread that could underlie progression of disease. We will use both Drosophila models and mammalian cell culture to test the core features of this proposed model.
View original record on NIH RePORTER →