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Loss of Hap1 selectively promotes striatal degeneration in Huntington disease mice.


ABSTRACT: Huntington disease (HD) is an ideal model for investigating selective neurodegeneration, as expanded polyQ repeats in the ubiquitously expressed huntingtin (HTT) cause the preferential neurodegeneration in the striatum of the HD patient brains. Here we report that adeno-associated virus (AAV) transduction-mediated depletion of Hap1, the first identified huntingtin-associated protein, in adult HD knock-in (KI) mouse brains leads to selective neuronal loss in the striatum. Further, Hap1 depletion-mediated neuronal loss via AAV transduction requires the presence of mutant HTT. Rhes, a GTPase that is enriched in the striatum and sumoylates mutant HTT to mediate neurotoxicity, binds more N-terminal HTT when Hap1 is deficient. Consistently, more soluble and sumoylated N-terminal HTT is presented in HD KI mouse striatum when HAP1 is absent. Our findings suggest that both Rhes and Hap1 as well as cellular stress contribute to the preferential neurodegeneration in HD, highlighting the involvement of multiple factors in selective neurodegeneration.

SUBMITTER: Liu Q 

PROVIDER: S-EPMC7443904 | biostudies-literature | 2020 Aug

REPOSITORIES: biostudies-literature

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Loss of Hap1 selectively promotes striatal degeneration in Huntington disease mice.

Liu Qiong Q   Cheng Siying S   Yang Huiming H   Zhu Louyin L   Pan Yongcheng Y   Jing Liang L   Tang Beisha B   Li Shihua S   Li Xiao-Jiang XJ  

Proceedings of the National Academy of Sciences of the United States of America 20200803 33


Huntington disease (HD) is an ideal model for investigating selective neurodegeneration, as expanded polyQ repeats in the ubiquitously expressed huntingtin (HTT) cause the preferential neurodegeneration in the striatum of the HD patient brains. Here we report that adeno-associated virus (AAV) transduction-mediated depletion of Hap1, the first identified huntingtin-associated protein, in adult HD knock-in (KI) mouse brains leads to selective neuronal loss in the striatum. Further, Hap1 depletion-  ...[more]

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