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Volume 43 Issue 6
Jun.  2016
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Parkin Somatic Mutations Link Melanoma and Parkinson's Disease

doi: 10.1016/j.jgg.2016.05.005
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  • Corresponding author: E-mail address: carmitlevy@post.tau.ac.il (Carmit Levy)
  • Received Date: 2015-10-30
  • Accepted Date: 2016-05-12
  • Rev Recd Date: 2016-05-11
  • Available Online: 2016-05-13
  • Publish Date: 2016-06-20
  • Epidemiological studies suggest a direct link between melanoma and Parkinson's disease (PD); however, the underlying molecular basis is unknown. Since mutations in Parkin are the major driver of early-onset PD and Parkin was recently reported to play a role in cancer development, we hypothesized that Parkin links melanoma and PD. By analyzing whole exome/genome sequencing of Parkin from 246 melanoma patients, we identified five non-synonymous mutations, three synonymous mutations, and one splice region variant in Parkin in 3.6% of the samples. In vitro analysis showed that wild-type Parkin plays a tumor suppressive role in melanoma development resulting in cell-cycle arrest, reduction of metabolic activity, and apoptosis. Using a mass spectrometry-based analysis, we identified potential Parkin substrates in melanoma and generated a functional protein association network. The activity of mutated Parkin was assessed by protein structure modeling and examination of Parkin E3 ligase activity. The Parkin-E28K mutation impairs Parkin ubiquitination activity and abolishes its tumor suppressive effect. Taken together, our analysis of genomic sequence and in vitro data indicate that Parkin is a potential link between melanoma and Parkinson's disease. Our findings suggest new approaches for early diagnosis and treatment against both diseases.
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