Abstract

This new NIEHS Center for Neurodegeneration Science (CMS) application will study the effect of environmental toxins on Parkinson's disease (PD). The Grant is based at the Burnham Institute for Medical Research (BIMR), The Scripps Research Institute (TSRI), and the University of California at San Diego (UCSD), all within a mile of each other in La Jolla, California. This group of neuroscientists has a strong history of working together in PD-related projects. BIMR and TSRI represent two of six NIHdesignated Roadmap Chemical Screening Centers. We will leverage these chemical-screening centers in this proposal to look for new drugs to treat PD. The Center is comprised of four Projects and four Scientific Cores (plus an Administrative/ BioStatistical Core and a Research Development Core) to support these projects. The Overall Theme of the Projects concerns how S-nitrosylation (SNO adduct formation) and further oxidation can mimic genetic mutations involved in PD to cause protein misfolding, abnormal signaling, and eventually neuronal cell injury and death. Our final goal will be to generate novel """"""""hits"""""""" from chemical library screens to offset this damage. Human material will be assessed for new SNO-Biomarkers and correlated to disease state, representing a human clinical component as defined in the RFA. The projects describe a novel complex of parkin/PINK1/DJ-1 and how this complex influences parkin E3 ligase activity and neuronal cell death (Project 1). The projects then proceed to study the deleterious effects of oxidative/nitrosative stress on this complex and other PD-related molecules that affect protein misfolding (Projects 2 and 3). From this information, novel therapies are sought by high-throughput screening (HTS) of chemical libraries using platforms of lower organisms (drosophila-based screens of Project 2) and in recombinant protein and cell-based screens (Project 3). After medicinal chemistry optimization, these novel """"""""hits"""""""" are then further tested in human embryonic stem cell (hESC)-derived dopaminergic neurons (Project 4). This project will also study developmental vulnerability to PD-related abnormal proteins or oxidative/nitrosative stress as cells develop into dopaminergic neurons derived from hESCs. Taken together, this Center offers a comprehensive study of the effects of environmental stress (represented by oxidation and S-nitrosylation) on PD-related proteins, and will develop new therapeutics based on this novel approach.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Program Projects (P01)
Project #
3P01ES016738-04S1
Application #
8293499
Study Section
Special Emphasis Panel (ZES1-LWJ-G (CN))
Program Officer
Lawler, Cindy P
Project Start
2008-09-15
Project End
2013-06-30
Budget Start
2011-07-01
Budget End
2012-06-30
Support Year
4
Fiscal Year
2011
Total Cost
$172,664
Indirect Cost

  Institution

Name
Sanford-Burnham Medical Research Institute
Department
Type
DUNS #
020520466
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Oh, Chang-Ki; Sultan, Abdullah; Platzer, Joseph et al. (2017) S-Nitrosylation of PINK1 Attenuates PINK1/Parkin-Dependent Mitophagy in hiPSC-Based Parkinson's Disease Models. Cell Rep 21:2171-2182
Singec, Ilyas; Crain, Andrew M; Hou, Junjie et al. (2016) Quantitative Analysis of Human Pluripotency and Neural Specification by In-Depth (Phospho)Proteomic Profiling. Stem Cell Reports 7:527-542
Qu, Zhe; Greenlief, C Michael; Gu, Zezong (2016) Quantitative Proteomic Approaches for Analysis of Protein S-Nitrosylation. J Proteome Res 15:1-14
Spiering, Sean; Davidovics, Herman; Bushway, Paul J et al. (2015) High content screening for modulators of cardiac differentiation in human pluripotent stem cells. Methods Mol Biol 1263:43-61
Okamoto, Shu-ichi; Lipton, Stuart A (2015) S-Nitrosylation in neurogenesis and neuronal development. Biochim Biophys Acta 1850:1588-93
Satoh, Takumi; Stalder, Romain; McKercher, Scott R et al. (2015) Nrf2 and HSF-1 Pathway Activation via Hydroquinone-Based Proelectrophilic Small Molecules is Regulated by Electrochemical Oxidation Potential. ASN Neuro 7:
Qu, Zhe; Meng, Fanjun; Zhou, Hui et al. (2014) NitroDIGE analysis reveals inhibition of protein S-nitrosylation by epigallocatechin gallates in lipopolysaccharide-stimulated microglial cells. J Neuroinflammation 11:17
Jeon, Gye Sun; Nakamura, Tomohiro; Lee, Jeong-Seon et al. (2014) Potential effect of S-nitrosylated protein disulfide isomerase on mutant SOD1 aggregation and neuronal cell death in amyotrophic lateral sclerosis. Mol Neurobiol 49:796-807
Choi, Min Sik; Nakamura, Tomohiro; Cho, Seung-Je et al. (2014) Transnitrosylation from DJ-1 to PTEN attenuates neuronal cell death in parkinson's disease models. J Neurosci 34:15123-31
Zhu, Saiyong; Ambasudhan, Rajesh; Sun, Woong et al. (2014) Small molecules enable OCT4-mediated direct reprogramming into expandable human neural stem cells. Cell Res 24:126-9

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