Name of Fellow

    Dr Lydia Alvarez

    Institution

    Funder

    Parkinson's UK

    Contact information of fellow

    Country

    United Kingdom

    Title of project/programme

    Further development of a systemic gene therapy treatment for Parkinson's

    Source of funding information

    Parkinson's UK

    Total sum awarded (Euro)

    € 420,358

    Start date of award

    01/09/11

    Total duration of award in years

    5.5

    The project/programme is most relevant to:

    Parkinson's disease & PD-related disorders

    Keywords

    Neuroprotection | Gene therapy | Cell biology

    Research Abstract

    Gene therapy is one of the most promising tools for the treatment of Parkinson’s, however one of the major challenges facing this approach is the development of a gene therapy vehicle for widespread delivery to the brain. We have developed a gene therapy vehicle based on targeted exosomes which we have shown are capable of selectively targeting the delivery of siRNA to brain resulting in gene silencing after intravenous administration. Alpha-synuclein aggregation plays a central role in PD pathology and increased expression or decreased degradation may be key features in its mechanism. Consequently an obvious initial target is alpha-synuclein. The first aim is to evaluate the efficacy of normal and modified siRNA delivery by RVG-exosomes to silence alpha-synuclein expression in mice. The second aim is to develop this system for long-term silencing within the brain using minicircles expressing shRNA (shRNA MC). As a model system we will target the fluorescent EGFP protein. We will optimise the sequences, constructs and electroporation conditions in SH-SY5Y cells over-expressing EGFP. Subsequently, we will evaluate the efficacy of long-term silencing by shRNA MC delivery by RVG-exosomes to silence EGFP expression in the brain of transgenic EGFP-mice. Finally, we will silence the expression of human WT and phospho-mimic S129D alpha-synuclein expressed in mice using shRNA MC. Alpha-synuclein silencing will be evaluated by qPCR, western blot and immnuhistochemistry throughout the brain. These studies will allow us to continue to develop this gene delivery vehicle and identify its suitability for use in the treatment of Parkinson’s.

Types: Fellowships
Member States: United Kingdom
Diseases: Parkinson's disease & PD-related disorders
Years: 2016
Database Categories: N/A
Database Tags: N/A

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