TY - JOUR T1 - Pathogenic tau accelerates aging-associated activation of transposable elements in the mouse central nervous system JF - bioRxiv DO - 10.1101/2021.02.25.432716 SP - 2021.02.25.432716 AU - Paulino Ramirez AU - Wenyan Sun AU - Gabrielle Zuniga AU - Elizabeth Ochoa Thomas AU - Sarah L. DeVos AU - Bradley Hyman AU - Gabriel Chiu AU - Ethan R. Roy AU - Wei Cao AU - Miranda Orr AU - Virginie Buggia-Prevot AU - William J. Ray AU - Bess Frost Y1 - 2021/01/01 UR - http://biorxiv.org/content/early/2021/02/26/2021.02.25.432716.abstract N2 - Transposable elements comprise almost half of the mammalian genome. A growing body of evidence suggests that transposable element dysregulation accompanies brain aging and neurodegenerative disorders, and that transposable element activation is neurotoxic. Recent studies have identified links between pathogenic forms of tau, a protein that accumulates in Alzheimer disease and related tauopathies, and transposable element-induced neurotoxicity. Starting with transcriptomic analyses, we find that age- and tau-induced transposable element activation occurs in the mouse brain. Among transposable elements that are activated at the RNA level in the context of brain aging and tauopathy, we find that the endogenous retrovirus (ERV) class of retrotransposons is particularly enriched. We show that protein encoded by Intracisternal A-particle, a highly active mouse ERV, is elevated in brains of tau transgenic mice. We further demonstrate that brains of tau transgenic mice contain increased DNA copy number of transposable elements, raising the possibility that these elements actively retrotranspose in the context of tauopathy. Taken together, our study lays the groundwork for future mechanistic studies focused on transposable element regulation in the aging mouse brain and in mouse models of tauopathy, while providing support for therapeutic approaches targeting transposable element activation for Alzheimer disease and related tauopathies.Competing Interest StatementThe authors have declared no competing interest. ER -