TY - JOUR T1 - Depleting Trim28 in adult mice is well tolerated and reduces levels of α-synuclein and tau JF - bioRxiv DO - 10.1101/284984 SP - 284984 AU - Maxime W.C. Rousseaux AU - Jean-Pierre Revelli AU - Gabriel E. Vázquez-Vélez AU - Ji-Yoen Kim AU - Evelyn Craigen AU - Kristyn Gonzales AU - Jaclyn Beckinghausen AU - Huda Y. Zoghbi Y1 - 2018/01/01 UR - http://biorxiv.org/content/early/2018/03/19/284984.abstract N2 - Alzheimer’s and Parkinson’s disease are late onset neurodegenerative diseases that will require therapy over decades to mitigate the effects of disease-driving proteins such tau and α-synuclein (α-Syn). We recently found that TRIM28 regulates the levels and toxicity of α-Syn and tau (Rousseaux et al., 2016), however, how TRIM28 regulates α-Syn and whether its chronic inhibition later in life is safe remained unknown. Here, we show that TRIM28 mediates the SUMOylation of α-Syn and tau, and that genetic suppression of Trim28 in adult mice is compatible with life. We were surprised to see that mice lacking Trim28 in adulthood do not exhibit behavioral or pathological phenotypes, and importantly, adult reduction of TRIM28 results in a decrease of α-Syn and tau levels. These results suggest that deleterious effects from TRIM28 depletion are limited to development and that its inhibition adulthood provides a potential path for modulating α-Syn and tau levels. ER -