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REDOX

Reporter models for the Evaluation of Diseases involving OXidative stress

Coordinatore	UNIVERSITY OF DUNDEE Spiacenti, non ci sono informazioni su questo coordinatore. Contattare Fabio per maggiori infomrazioni, grazie.
Nazionalità Coordinatore	United Kingdom [UK]
Totale costo	2˙486˙524 €
EC contributo	2˙486˙524 €
Programma	FP7-IDEAS-ERC Specific programme: "Ideas" implementing the Seventh Framework Programme of the European Community for research, technological development and demonstration activities (2007 to 2013)
Code Call	ERC-2011-ADG_20110310
Funding Scheme	ERC-AG
Anno di inizio	2012
Periodo (anno-mese-giorno)	2012-03-01 - 2017-02-28

Partecipanti

#	participant	country	role	EC contrib. [€]
1	UNIVERSITY OF DUNDEE Organization address address: Nethergate city: DUNDEE postcode: DD1 4HN contact info Titolo: Dr. Nome: Kathryn Cognome: Williamson Email: send email Telefono: +44 1382 388340	UK (DUNDEE)	hostInstitution	2˙486˙524.00
2	UNIVERSITY OF DUNDEE Organization address address: Nethergate city: DUNDEE postcode: DD1 4HN contact info Titolo: Prof. Nome: Charles Roland Cognome: Wolf Email: send email Telefono: +44 1382 232621	UK (DUNDEE)	hostInstitution	2˙486˙524.00

Mappa

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experimental regulated reporter sophisticated ros oxidative vivo redox endogenous models aetiology create stress human technologies diseases disease reporters types

Obiettivo del progetto (Objective)

'Perturbations in cellular redox status are implicated in many human diseases, yet there is an extreme lack of knowledge about the effects of oxidative stress in vivo, mainly due to difficulties in measuring reactive oxygen species (ROS) in vivo and the absence of experimental models. REDOX will use novel transgenic technologies to develop mouse models that report on ROS in vivo, allowing spatio-temporal monitoring of different types of oxidative stress, ultimately simultaneously in a complex reporter line, and clarifying its role in the aetiology of disease and pathways of drug & chemical toxicity. These models will reveal oxidative stress as a primary cause, or a consequence, of the disease process. Reporters will be driven by endogenous genes regulated by different forms of oxidative stress and, uniquely, we will exploit the sophisticated redox sensing systems in bacteria to discern different types of ROS. In a sophisticated system we will express 3 reporters from the same stress regulated promotor, generating a polycistronic mRNA by use of the FMDV 2A sequence, which cleaves the nascent polypeptide to yield the endogenous gene product and individual reporters. LacZ will be used as an in situ reporter, luciferase for imaging, and a secreted protein, eg hCG, as a non-invasive biomarker in blood or urine. The in vivo role of oxidative stress in disease aetiology, and the potential of novel anti-oxidants to prevent such diseases, will be evaluated in these models. A further novel aspect will be to generate ES cells from the reporter lines, and create genetically-driven disease models which reflect inherited human diseases. REDOX combines ambitious experimental systems with sophisticated novel technologies to create models to define the role of oxidative stress in human disease, offering a new approach in defining and testing of disease prevention and therapeutic interventions while reducing the number of animals required.'