Parkin, PINK1, and DJ-1 form a ubiquitin E3 ligase complex promoting unfolded protein degradation
Hui Xiong, … , Xiaoxi Zhuang, Zhuohua Zhang
Hui Xiong, … , Xiaoxi Zhuang, Zhuohua Zhang
Published February 23, 2009
Citation Information: J Clin Invest. 2009;119(3):650-660. https://doi.org/10.1172/JCI37617.
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Parkin, PINK1, and DJ-1 form a ubiquitin E3 ligase complex promoting unfolded protein degradation

Abstract

Mutations in PARKIN, pten-induced putative kinase 1 (PINK1), and DJ-1 are individually linked to autosomal recessive early-onset familial forms of Parkinson disease (PD). Although mutations in these genes lead to the same disease state, the functional relationships between them and how their respective disease-associated mutations cause PD are largely unknown. Here, we show that Parkin, PINK1, and DJ-1 formed a complex (termed PPD complex) to promote ubiquitination and degradation of Parkin substrates, including Parkin itself and Synphilin-1 in neuroblastoma cells and human brain lysates. Genetic ablation of either Pink1 or Dj-1 resulted in reduced ubiquitination of endogenous Parkin as well as decreased degradation and increased accumulation of aberrantly expressed Parkin substrates. Expression of PINK1 enhanced Parkin-mediated degradation of heat shock–induced misfolded protein. In contrast, PD-pathogenic Parkin and PINK1 mutations showed reduced ability to promote degradation of Parkin substrates. This study identified a functional ubiquitin E3 ligase complex consisting of PD-associated Parkin, PINK1, and DJ-1 to promote degradation of un-/misfolded proteins and suggests that their PD-pathogenic mutations impair E3 ligase activity of the complex, which may constitute a mechanism underlying PD pathogenesis.

Authors

Hui Xiong, Danling Wang, Linan Chen, Yeun Su Choo, Hong Ma, Chengyuan Tang, Kun Xia, Wei Jiang, Ze’ev Ronai, Xiaoxi Zhuang, Zhuohua Zhang

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Figure 8

PINK1 promotes degradation of Parkin that has accumulated as a result of heat shock treatment.

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PINK1 promotes degradation of Parkin that has accumulated as a result of...
Cells expressing Parkin alone (lanes 2–4); Parkin and ubiquitin (lanes 5–7); and Parkin, ubiquitin, and PINK1 (lanes 8–10) without heat shock treatment (lanes 1, 2, 5, 8), with heat shock treatment (lanes 3, 6, 9), or with heat shock treatment followed by a 4-h recovery time (RT) at 37°C (lanes 4, 7, 10). The cells were lysed and immunoprecipitated with an anti-Parkin antibody, followed by immunoblotting with either an anti-ubiquitin antibody (A) or an anti-Parkin antibody (B). Expression of PINK1 (C) and tubulin (D) were shown with immunoblotting. Note that heat shock treatment increased accumulation of Parkin protein (B; lanes 6–7). PINK1 promoted degradation of Parkin even with heat shock treatment (B; lanes 9–10).