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Funded Studies

The Foundation supports research across basic, translational and clinical science to speed breakthroughs that can lead to the creation of new treatments and a better quality of life for people with Parkinson's disease.

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Previously funded studies appear chronologically, with the most recent appearing first.

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  • Rapid Response Innovation Awards, 2010
    MicroRNAs as Biomarkers for Parkinson's Disease; A Comparison of CSF and Blood

    Objective/Rationale:
    We, and many other groups, hypothesize that miRNAs have the potential to be selective and sensitive diagnostic indicators for Parkinson’s disease. The focus of this project is to...

  • Rapid Response Innovation Awards, 2010
    The Role of Alpha-synuclein in the Pathogenesis of Parkinson's Disease in a Pre-clinical Model

    Objective/Rationale: 
    We hypothesized that alpha-synuclein increased level and accumulation within the target neurons in the affected model acts as a trigger mechanism for activation of additional...

  • Target Validation, 2010
    Validation of FKBP Inhibitors to Target Alpha-synuclein Pathology in Pre-clinical Model Brain

    Objective/Rationale: 
    FK506 Binding Proteins (FKBPs) are enzymes that play a role in protein folding. FKBPs are highly expressed in human brain and are thought to be involved in neurodegenerative...

  • Therapeutics Development Initiative, 2010
    Evaluation of the Neuroprotectivity Ability of Zymes' Water-soluble CoQ10 (WS-CoQ10) in Pre-clinical Models of PD; Preclinical Validation and Dose Optimization for Clinical Study

    Objective/Rationale:
    Coenzyme Q10 is a lipid soluble naturally occurring compound essential for energy production and defence against oxidative stress.  Recent clinical studies indicate that it may...

  • Alpha-Synuclein Therapeutics, 2010
    Use of the Orally Administered Pharmacological Chaperone AT3375 to Reduce Alpha-synuclein Levels in the Brain of Thy-1 Alpha-synuclein Small Models

    Objective/Rationale: 
    Mutations in the GBA1 gene increase the risk of Parkinson’s. These mutations reduce the activity of the enzyme glucocerebrosidase (GCase), which is deficient in the lysosomal...

  • Target Validation, 2010
    Kynurenine 3-monooxygenase (KMO) as a Target to Develop Drugs to Block Progression of Parkinson's Disease

    Objective/Rationale:
    These studies will validate the enzyme kynurenine 3-monooxygenase (KMO) as a target to develop drugs to treat PD (PD). KMO is expressed in cells involved in inflammation, which is...

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