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AD SYNAPTIC DEFICITS

Functional and synaptic deficits in cerebral cortical neurons in Alzheimer’s Disease model mice

Coordinatore	BAR ILAN UNIVERSITY Organization address address: BAR ILAN UNIVERSITY CAMPUS city: RAMAT GAN postcode: 52900 contact info Titolo: Ms. Nome: Estelle Cognome: Waise Email: send email Telefono: +972 3 531 7439 Fax: +972 3 635 3277
Nazionalità Coordinatore	Israel [IL]
Totale costo	45˙000 €
EC contributo	45˙000 €
Programma	FP7-PEOPLE Specific programme "People" implementing the Seventh Framework Programme of the European Community for research, technological development and demonstration activities (2007 to 2013)
Code Call	FP7-PEOPLE-ERG-2008
Funding Scheme	MC-ERG
Anno di inizio	2008
Periodo (anno-mese-giorno)	2008-09-01 - 2011-08-31

Partecipanti

#	participant	country	role	EC contrib. [€]
1	BAR ILAN UNIVERSITY Organization address address: BAR ILAN UNIVERSITY CAMPUS city: RAMAT GAN postcode: 52900 contact info Titolo: Ms. Nome: Estelle Cognome: Waise Email: send email Telefono: +972 3 531 7439 Fax: +972 3 635 3277	IL (RAMAT GAN)	coordinator	0.00

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dynamics synapses cortical alzheimer calcium spines organization function disease effect insoluble soluble neurons beta single vivo mechanisms transgenic individual neuronal synaptic somatosensory neocortical ad dendritic plaques network receptive intact

Obiettivo del progetto (Objective)

'Alzheimer’s disease (AD) is the most common neurodegenerative disease, affecting millions of people worldwide and therefore it is fundamental to understand its underlying mechanisms. Although the neuropathologies involved in AD are well-described, the effect of those pathologies on neuronal function are poorly understood. Using a transgenic mouse model of AD that overexpresses human amyloid-beta (a-beta), we will study the effects of a-beta accumulation on neocortical synaptic function and receptive field organization using in vivo intracellular recording and in vivo 2-photon laser-scanning microscopy (2PLSM). We will measure the effect of soluble a-beta on individual synapses by imaging calcium dynamics in dendritic spines of somatosensory cortical neurons in response to whisker stimulation. Responses in transgenic animals will be compared to age-matched controls. This will measure the effects of a-beta on individual synapses in vivo. In addition, we will measure the neurotoxic effects of insoluble a-beta plaques on synaptic function by comparing the calcium dynamics in dendritic spines proximal to plaques to those distant from them. Finally, we will measure the effects of soluble a-beta and plaques on the receptive field organization of Layer II/III somatosensory cortical neurons to quantify the effects of the neuropathology on an intact neocortical network. This study will measure and differentiate between the effects of soluble a-beta and insoluble plaques on cortical function at several levels: at the level of the single synapse (calcium dynamics in dendritic spines), single neuron (electrophysiology of subthreshold inputs and spike outputs) and cortical network (receptive field organization) in the intact animal. This study will therefore fill a crucial gap between the molecular mechanisms of Alzheimer’s Disease and the symptoms of the disease, which are mediated by currently unknown neuronal events.'