| Literature DB >> 34052184 |
Jixing Zhong1, Gen Tang2, Jiacheng Zhu3, Weiying Wu4, Ge Li5, Xiumei Lin3, Langchao Liang3, Chaochao Chai3, Yuying Zeng3, Feiyue Wang3, Lihua Luo3, Jiankang Li6, Fang Chen7, Zhen Huang8, Xiuqing Zhang6, Yu Zhang5, Hongde Liu9, Xin Qiu10, Shengping Tang11, Dongsheng Chen12.
Abstract
Parkinson's disease (PD) is a neurodegenerative disease, leading to the impairment of movement execution. PD pathogenesis has been largely investigated, either limited to bulk transcriptomic levels or at certain cell types, which failed to capture the cellular heterogeneity and intrinsic interplays among distinct cell types. Here, we report the application of single-nucleus RNA-seq on midbrain, striatum, and cerebellum of the α-syn-A53T mouse, a well-established PD mouse model, and matched controls, generating the first single cell transcriptomic atlas for the PD model mouse brain composed of 46,174 individual cells. Additionally, we comprehensively depicte the dysfunctions in PD pathology, covering the elevation of NF-κB activity, the alteration of ion channel components, the perturbation of protein homeostasis network, and the dysregulation of glutamatergic signaling. Notably, we identify a variety of cell types closely associated with PD risk genes. Taken together, our study provides valuable resources to systematically dissect the molecular mechanism of PD pathogenesis at the single-cell resolution, which facilitates the development of novel approaches for diagnosis and therapies against PD.Entities:
Keywords: Neuroinflammtion; Parkinson's disease; Pathogenesis; Single-nucleus RNA-Seq; α-syn-A53T
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Year: 2021 PMID: 34052184 DOI: 10.1016/j.jgg.2021.01.003
Source DB: PubMed Journal: J Genet Genomics ISSN: 1673-8527 Impact factor: 4.275