@article{66f2c0189592445c8fd2c54f4df80ef2,
title = "Parkin is transcriptionally regulated by ATF4: Evidence for an interconnection between mitochondrial stress and ER stress",
abstract = "Loss of parkin function is responsible for the majority of autosomal recessive parkinsonism. Here, we show that parkin is not only a stress-protective, but also a stress-inducible protein. Both mitochondrial and endoplasmic reticulum (ER) stress induce an increase in parkin-specific mRNA and protein levels. The stress-induced upregulation of parkin is mediated by ATF4, a transcription factor of the unfolded protein response (UPR) that binds to a specific CREB/ATF site within the parkin promoter. Interestingly, c-Jun can bind to the same site, but acts as a transcriptional repressor of parkin gene expression. We also present evidence that mitochondrial damage can induce ER stress, leading to the activation of the UPR, and thereby to an upregulation of parkin expression. Vice versa, ER stress results in mitochondrial damage, which can be prevented by parkin. Notably, the activity of parkin to protect cells from stress-induced cell death is independent of the proteasome, indicating that proteasomal degradation of parkin substrates cannot explain the cytoprotective activity of parkin. Our study supports the notion that parkin has a role in the interorganellar crosstalk between the ER and mitochondria to promote cell survival under stress, suggesting that both ER and mitochondrial stress can contribute to the pathogenesis of Parkinson's disease.",
keywords = "ATF4, ER stress, Parkinson's disease, UPR, c-Jun, parkin",
author = "L. Bouman and A. Schlierf and Lutz, {A. K.} and J. Shan and A. Deinlein and J. Kast and Z. Galehdar and V. Palmisano and N. Patenge and D. Berg and T. Gasser and R. Augustin and D. Tr{\"u}mbach and I. Irrcher and Park, {D. S.} and W. Wurst and Kilberg, {M. S.} and J. Tatzelt and Winklhofer, {K. F.}",
note = "Funding Information: Acknowledgements. This work was supported by the Deutsche Forschu-ngsgemeinschaft (SFB 596 {\textquoteleft}Molecular Mechanisms of Neurodegeneration{\textquoteright} to KFW, JT and WW), the German Ministry for Education and Research (NGFN plus {\textquoteleft}Functional Genomics of Parkinson{\textquoteright}s Disease{\textquoteright} to KFW, TG and WW), the Helmholtz Alliance {\textquoteleft}Mental Health in an Ageing Society{\textquoteright} (to KFW, TG and WW), the Hans and Ilse Breuer Foundation (to LB), the Heart and Stroke Foundation of Canada, Heart and Stroke Foundation of Ontario and the Canadian Institutes of Health Research (to DSP). Funding for MSK was from the National Institutes of Health (DK-52064). II was supported by a postdoctoral fellowship from Canadian Institutes of Health Research (CIHR). We are grateful to Christian Haass for continuous support and stimulating discussions. We thank Dr Tim Townes for providing the ATF4-knockout mice, Alexis Brice and Olga Corti for the parkin-knockout mice, Torsten Kluba for human skin fibroblasts from control individuals, Carsten Culmsee for primary mouse cortical neurons, Daniel Krappmann for the c-Jun plasmid, Kimitoshi Kohno and Hiroto Izumi for the ATF4 plasmid, Gerald Thiel for the ATF4DN and CHOP plasmids, David Ron for the PERK plasmid and Vicky W{\"a}tzig and Thomas Herdegen for the JNK3 plasmid. We thank Kerstin L{\"a}mmermann and Christian Naumann for technical assistance and Jonathan Lin for advice on ATF4 western blotting.",
year = "2011",
month = may,
doi = "10.1038/cdd.2010.142",
language = "English",
volume = "18",
pages = "769--782",
journal = "Cell Death and Differentiation",
issn = "1350-9047",
publisher = "Springer Nature",
number = "5",
}