Skip to main content
European Commission logo
español español
CORDIS - Resultados de investigaciones de la UE
CORDIS
CORDIS Web 30th anniversary CORDIS Web 30th anniversary

A novel multi-functional nanocomposites against Parkinson’s disease for the protection and regeneration of dopamine neurons with anti alpha-Synuclein aggregation properties.

Descripción del proyecto

Nanopartículas multifuncionales para el tratamiento de la enfermedad de Parkinson

La enfermedad de Parkinson (EP) es un trastorno neurodegenerativo asociado con la pérdida de neuronas dopaminérgicas y la acumulación intraneuronal de α-sinucleína (α-S). El transporte de determinados factores neurotróficos (FNT) al encéfalo detiene y revierte la neurodegeneración en modelos animales, pero estos FNT no atraviesan la barrera hematoencefálica y deben administrarse mediante microcirugía. La estrategia para curar la EP se basa en la eliminación de la α-S y la prevención de su agregación patológica. Los resultados preliminares mostraron que las nanopartículas de oro recubiertas de beta-caseína reducen la agregación de α-S y pueden utilizarse para transportar FNT al encéfalo. El proyecto financiado con fondos europeos NEUROCURE busca desarrollar un tratamiento multifuncional basado en nanopartículas de oro para la EP que ralentice la progresión de la enfermedad asociada con la α-S y promueva la supervivencia de las neuronas dopaminérgicas, transportando los FNT al encéfalo.

Objetivo

Parkinson’s disease (PD) is the second most common neurodegenerative disorder that is characterised by progressive loss of dopamine neurons and abnormal intra-neuronal accumulation of protein α-synuclein (αS). None of the available treatments have shown ability to slow down the progression of the neurodegeneration. One of the therapeutically potent approaches to combat PD is neurotrophic factor (NTF)-based therapies. Delivery of NTFs to the brain shows a notable therapeutic potential due to the ability to stop and reverse neurodegeneration in animal models. The most potent NTFs for PD therapy so far are CDNF and GDNF that have been recently studied in clinical trials on PD patients. Despite of the promising results, CDNF and GDNF does not pass through the blood brain barrier (BBB) and should be delivered to the brain through a risky microsurgery. Thus, there is a great need for an effective method that can deliver CDNF/GDNF through the BBB avoiding intracranial surgery. Another promising strategy for curing PD is based on αS clearance and control of its pathological aggregation and propagation. Our preliminary results showed that beta-casein coated AuNPs have great capacity to reduce αS aggregation and can be used to deliver NTFs to the brain. This proposal combines nanomedicine and molecular neurobiology to develop multi-functional AuNP-based medicine against PD that will positively impact the disease progression through mitigation of the parthenogenesis associated with αS and support the survival of dopamine neurons by CDNF/GDNF delivery to the brain. The applicant will get training needed for his future independent research career through hands-on training in the top scientific laboratories and by managing the highly innovative research at the interface of different disciplines connecting two excellent scientists: Prof. Saarma, a world leading molecular neurobiologist and Prof. Teesalu, an expert in homing peptides.

Coordinador

HELSINGIN YLIOPISTO
Aportación neta de la UEn
€ 190 680,96
Dirección
FABIANINKATU 33
00014 HELSINGIN YLIOPISTO
Finlandia

Ver en el mapa

Región
Manner-Suomi Helsinki-Uusimaa Helsinki-Uusimaa
Tipo de actividad
Higher or Secondary Education Establishments
Enlaces
Coste total
€ 190 680,96