Literature DB >> 16565515

Proteomic identification of a stress protein, mortalin/mthsp70/GRP75: relevance to Parkinson disease.

Jinghua Jin1, Christine Hulette, Yan Wang, Terry Zhang, Catherine Pan, Renu Wadhwa, Jing Zhang.   

Abstract

Functional impairment of mitochondria and proteasomes and increased oxidative damage comprise the main pathological phenotypes of Parkinson disease (PD). Using an unbiased quantitative proteomic approach, we compared nigral mitochondrial proteins of PD patients with those from age-matched controls. 119 of 842 identified proteins displayed significant differences in their relative abundance (increase/decrease) between the two groups. We confirmed that one of these, mortalin (mthsp70/GRP75, a mitochondrial stress protein), is substantially decreased in PD brains as well as in a cellular model of PD. In addition, nine candidate mortalin-binding partners were identified as potential mediators of PD pathology. Manipulations of mortalin level in dopaminergic neurons resulted in significant changes in sensitivity to PD phenotypes via pathways involving mitochondrial and proteasomal function as well as oxidative stress.

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Year:  2006        PMID: 16565515     DOI: 10.1074/mcp.M500382-MCP200

Source DB:  PubMed          Journal:  Mol Cell Proteomics        ISSN: 1535-9476            Impact factor:   5.911


  91 in total

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