Histone H2A ubiquitination resulting from Brap loss of function connects multiple aging hallmarks and accelerates neurodegeneration



Guo Yan, Chomiak Alison A, Hong Ye, Lowe Clara C, Kopsidas Caroline A, Chan Wen-Ching, Andrade Jorge, Pan Hongna, Zhou Xiaoming, Monuki Edwin S, Feng Yuanyi

PublisherElsevier

2022

iScience

iScience

iScience

104519

25

7

2589-0042

DOIhttps://doi.org/10.1016/j.isci.2022.104519

https://doi.org/10.1016/j.isci.2022.104519

https://research.utu.fi/converis/portal/detail/Publication/176037319


Aging is an intricate process characterized by multiple hallmarks including stem cell exhaustion, genome instability, epigenome alteration, impaired proteostasis, and cellular senescence. Whereas each of these traits is detrimental at the cellular level, it remains unclear how they are interconnected to cause systemic organ deterioration. Here we show that abrogating Brap, a BRCA1-associated protein essential for neurogenesis, results in persistent DNA double-strand breaks and elevation of histone H2A mono- and poly-ubiquitination (H2Aub). These defects extend to cellular senescence and proteasome-mediated histone H2A proteolysis with alterations in cells' proteomic and epigenetic states. Brap deletion in the mouse brain causes neuroinflammation, impaired proteostasis, accelerated neurodegeneration, and substantially shortened the lifespan. We further show the elevation of H2Aub also occurs in human brain tissues with Alzheimer's disease. These data together suggest that chromatin aberrations mediated by H2Aub may act as a nexus of multiple aging hallmarks and promote tissue-wide degeneration.

Last updated on 2024-26-11 at 13:26