PINK1 kinase dysfunction triggers neurodegeneration in the primate brain without impacting mitochondrial homeostasis

Weili Yang; Xiangyu Guo; Zhuchi Tu; Xiusheng Chen; Rui Han; Yanting Liu; Sen Yan; Qi Wang; Zhifu Wang; Xianxian Zhao; Yunpeng Zhang; Xin Xiong; Huiming Yang; Peng Yin; Huida Wan; Xingxing Chen; Jifeng Guo; Xiao Xin Yan; Lujian Liao; Shihua Li; Xiao Jiang Li

doi:10.1007/s13238-021-00888-x

PINK1 kinase dysfunction triggers neurodegeneration in the primate brain without impacting mitochondrial homeostasis

Weili Yang^*
, Xiangyu Guo
, Zhuchi Tu
, Xiusheng Chen
, Rui Han
, Yanting Liu
, Sen Yan
, Qi Wang
, Zhifu Wang
, Xianxian Zhao
, Yunpeng Zhang
, Xin Xiong
, Huiming Yang
, Peng Yin
, Huida Wan
, Xingxing Chen
, Jifeng Guo
, Xiao Xin Yan
, Lujian Liao
, Shihua Li

Xiao Jiang Li^*

^*此作品的通讯作者

生命科学学院

Jinan University
East China Normal University
Central South University

科研成果: 期刊稿件 › 文章 › 同行评审

54 引用（Scopus）

摘要

In vitro studies have established the prevalent theory that the mitochondrial kinase PINK1 protects neurodegeneration by removing damaged mitochondria in Parkinson’s disease (PD). However, difficulty in detecting endogenous PINK1 protein in rodent brains and cell lines has prevented the rigorous investigation of the in vivo role of PINK1. Here we report that PINK1 kinase form is selectively expressed in the human and monkey brains. CRISPR/Cas9-mediated deficiency of PINK1 causes similar neurodegeneration in the brains of fetal and adult monkeys as well as cultured monkey neurons without affecting mitochondrial protein expression and morphology. Importantly, PINK1 mutations in the primate brain and human cells reduce protein phosphorylation that is important for neuronal function and survival. Our findings suggest that PINK1 kinase activity rather than its mitochondrial function is essential for the neuronal survival in the primate brains and that its kinase dysfunction could be involved in the pathogenesis of PD.

源语言	英语
页（从-至）	26-46
页数	21
期刊	Protein and Cell
卷	13
期	1
DOI	https://doi.org/10.1007/s13238-021-00888-x
出版状态	已出版 - 1月 2022

联合国可持续发展目标

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可持续发展目标 3 良好健康与福祉

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10.1007/s13238-021-00888-x

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Yang, W., Guo, X., Tu, Z., Chen, X., Han, R., Liu, Y., Yan, S., Wang, Q., Wang, Z., Zhao, X., Zhang, Y., Xiong, X., Yang, H., Yin, P., Wan, H., Chen, X., Guo, J., Yan, X. X., Liao, L., ... Li, X. J. (2022). PINK1 kinase dysfunction triggers neurodegeneration in the primate brain without impacting mitochondrial homeostasis. Protein and Cell, 13(1), 26-46. https://doi.org/10.1007/s13238-021-00888-x

@article{8b30eef8433b473d889980c63bdf2f50,

title = "PINK1 kinase dysfunction triggers neurodegeneration in the primate brain without impacting mitochondrial homeostasis",

abstract = "In vitro studies have established the prevalent theory that the mitochondrial kinase PINK1 protects neurodegeneration by removing damaged mitochondria in Parkinson{\textquoteright}s disease (PD). However, difficulty in detecting endogenous PINK1 protein in rodent brains and cell lines has prevented the rigorous investigation of the in vivo role of PINK1. Here we report that PINK1 kinase form is selectively expressed in the human and monkey brains. CRISPR/Cas9-mediated deficiency of PINK1 causes similar neurodegeneration in the brains of fetal and adult monkeys as well as cultured monkey neurons without affecting mitochondrial protein expression and morphology. Importantly, PINK1 mutations in the primate brain and human cells reduce protein phosphorylation that is important for neuronal function and survival. Our findings suggest that PINK1 kinase activity rather than its mitochondrial function is essential for the neuronal survival in the primate brains and that its kinase dysfunction could be involved in the pathogenesis of PD.",

keywords = "Parkinson{\textquoteright}s disease, mitochondria, neurodegeneration, neurogenesis, non-human primates",

author = "Weili Yang and Xiangyu Guo and Zhuchi Tu and Xiusheng Chen and Rui Han and Yanting Liu and Sen Yan and Qi Wang and Zhifu Wang and Xianxian Zhao and Yunpeng Zhang and Xin Xiong and Huiming Yang and Peng Yin and Huida Wan and Xingxing Chen and Jifeng Guo and Yan, \{Xiao Xin\} and Lujian Liao and Shihua Li and Li, \{Xiao Jiang\}",

note = "Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2022",

month = jan,

doi = "10.1007/s13238-021-00888-x",

language = "英语",

volume = "13",

pages = "26--46",

journal = "Protein and Cell",

issn = "1674-800X",

publisher = "Oxford University Press",

number = "1",

}

Yang, W, Guo, X, Tu, Z, Chen, X, Han, R, Liu, Y, Yan, S, Wang, Q, Wang, Z, Zhao, X, Zhang, Y, Xiong, X, Yang, H, Yin, P, Wan, H, Chen, X, Guo, J, Yan, XX, Liao, L, Li, S & Li, XJ 2022, 'PINK1 kinase dysfunction triggers neurodegeneration in the primate brain without impacting mitochondrial homeostasis', Protein and Cell, 卷 13, 号码 1, 页码 26-46. https://doi.org/10.1007/s13238-021-00888-x

TY - JOUR

T1 - PINK1 kinase dysfunction triggers neurodegeneration in the primate brain without impacting mitochondrial homeostasis

AU - Yang, Weili

AU - Guo, Xiangyu

AU - Tu, Zhuchi

AU - Chen, Xiusheng

AU - Han, Rui

AU - Liu, Yanting

AU - Yan, Sen

AU - Wang, Qi

AU - Wang, Zhifu

AU - Zhao, Xianxian

AU - Zhang, Yunpeng

AU - Xiong, Xin

AU - Yang, Huiming

AU - Yin, Peng

AU - Wan, Huida

AU - Chen, Xingxing

AU - Guo, Jifeng

AU - Yan, Xiao Xin

AU - Liao, Lujian

AU - Li, Shihua

AU - Li, Xiao Jiang

PY - 2022/1

Y1 - 2022/1

N2 - In vitro studies have established the prevalent theory that the mitochondrial kinase PINK1 protects neurodegeneration by removing damaged mitochondria in Parkinson’s disease (PD). However, difficulty in detecting endogenous PINK1 protein in rodent brains and cell lines has prevented the rigorous investigation of the in vivo role of PINK1. Here we report that PINK1 kinase form is selectively expressed in the human and monkey brains. CRISPR/Cas9-mediated deficiency of PINK1 causes similar neurodegeneration in the brains of fetal and adult monkeys as well as cultured monkey neurons without affecting mitochondrial protein expression and morphology. Importantly, PINK1 mutations in the primate brain and human cells reduce protein phosphorylation that is important for neuronal function and survival. Our findings suggest that PINK1 kinase activity rather than its mitochondrial function is essential for the neuronal survival in the primate brains and that its kinase dysfunction could be involved in the pathogenesis of PD.

AB - In vitro studies have established the prevalent theory that the mitochondrial kinase PINK1 protects neurodegeneration by removing damaged mitochondria in Parkinson’s disease (PD). However, difficulty in detecting endogenous PINK1 protein in rodent brains and cell lines has prevented the rigorous investigation of the in vivo role of PINK1. Here we report that PINK1 kinase form is selectively expressed in the human and monkey brains. CRISPR/Cas9-mediated deficiency of PINK1 causes similar neurodegeneration in the brains of fetal and adult monkeys as well as cultured monkey neurons without affecting mitochondrial protein expression and morphology. Importantly, PINK1 mutations in the primate brain and human cells reduce protein phosphorylation that is important for neuronal function and survival. Our findings suggest that PINK1 kinase activity rather than its mitochondrial function is essential for the neuronal survival in the primate brains and that its kinase dysfunction could be involved in the pathogenesis of PD.

KW - Parkinson’s disease

KW - mitochondria

KW - neurodegeneration

KW - neurogenesis

KW - non-human primates

UR - https://www.scopus.com/pages/publications/85119427412

U2 - 10.1007/s13238-021-00888-x

DO - 10.1007/s13238-021-00888-x

M3 - 文章

C2 - 34800266

AN - SCOPUS:85119427412

SN - 1674-800X

VL - 13

SP - 26

EP - 46

JO - Protein and Cell

JF - Protein and Cell

IS - 1

ER -

PINK1 kinase dysfunction triggers neurodegeneration in the primate brain without impacting mitochondrial homeostasis

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