Modelling human neuroinflammatory and demyelinating disease in transgenic and mutant animals

Ziel

In human demyelinating diseases like multiple sclerosis (MS), inflammatory reactions are the primary cause of myelin damage. While experimentally-induced animal models for MS have provided much insight into the involvement of myelin- specific T-cells in the early phases of disease, the peripheral immune response alone is unable to account for the widespread and selective destruction of myelin that occurs in MS and that leads to impairment of neurological function.
A critical additional pathogenic factor, for which characterised animal models have not yet been developed, relates to disturbances of the cellular and molecular environment within the central nervous system (CNS) itself, for example by the deregulated production of pro-inflammatory molecules by activated glia. Tumour necrosis factor a(TNF)is a major effector molecule of the immune- system, and is now believed to play a critical role in the pathogenesis of MS and several other neuroinflammatory and neurodegenerative CNS diseases such as AIDS dementia and Alzheimer's disease. We have recently demonstrated that TNF overexpression in the CNS of transgenic mice, can indeed trigger a spontaneous inflammatory demyelinating disease with many of the clinical and histopathological hallmarks of MS. To further develop this phenotype as a model for human CNS inflammation and demyelination, major questions concerning the molecular and cellular mechanisms by which TNF triggers disease need to be addressed. The core of the present proposal centres around the development and application of state-of-the-art techniques in transgenic and conditional gene targeting methodology, to introduce specific disturbances into the micro- environment of the CNS, as an approach to generate animal models of human CNS disease with precise genetically determined characteristics. As well as specifically addressing questions about TNF biology, such as the source and context of deregulated TNF production, the cellular distribution of the two high affinity TNF receptors (pSSTNFR & p75TNFR) and the results of their respective signalling, this approach will also be used to study the contribution of additional factors that might predispose the CNS to inflammation and demyelination, particularly metabolic disturbances in myelin, and disturbances in the function of the blood-brain barrier.
The goals of this proposal are:
1. To develop new predictive animal models of human inflammatory, demyelinating and neurodegenerative diseases of the CNS, by the use of gene addition, gene deletion and conditional gene targeting protocols, to create specific perturbances in cellular homeostasis (i.e. disruption of the blood-bra barrier), cytokine balances (i.e. TNF and TNF-R production) and/or the molecular composition of myelin (i.e. PLP protein).
2. To exploit the molecular and cellular phenotypes of these in-vivo systems and of the pathologies induced, to gain further insight into the biology of CNS immune response, and into the pathogenic mechanisms leading to the development of the relevant human diseases.
3. To use the transgenic animal models to identify key mechanisms as potential targets for therapeutical intervention, and to design and test, in-vivo, new therapies and pharmacological approaches aiming to control the induction and perpetuation of destructive inflammatory phenomena in the CNS (many of these will be provided by Industry).

Wissenschaftliches Gebiet (EuroSciVoc)

CORDIS klassifiziert Projekte mit EuroSciVoc, einer mehrsprachigen Taxonomie der Wissenschaftsbereiche, durch einen halbautomatischen Prozess, der auf Verfahren der Verarbeitung natürlicher Sprache beruht. Siehe: Das European Science Vocabulary.

• Medizin- und Gesundheitswissenschaften Grundlagenmedizin Neurologie Demenz Alzheimer
• Medizin- und Gesundheitswissenschaften Grundlagenmedizin Neurologie Multiple Sklerose
• Medizin- und Gesundheitswissenschaften Grundlagenmedizin Immunologie
• Medizin- und Gesundheitswissenschaften Gesundheitswissenschaften Infektionskrankheit RNS-Virus HIV
• Medizin- und Gesundheitswissenschaften Grundlagenmedizin Physiologie Homöostase

Programm/Programme

Mehrjährige Finanzierungsprogramme, in denen die Prioritäten der EU für Forschung und Innovation festgelegt sind.

• FP4-BIOTECH 2 - Specific research, technological development and demonstration programme in the field of biotechnology, 1994-1998

Thema/Themen

Aufforderungen zur Einreichung von Vorschlägen sind nach Themen gegliedert. Ein Thema definiert einen bestimmten Bereich oder ein Gebiet, zu dem Vorschläge eingereicht werden können. Die Beschreibung eines Themas umfasst seinen spezifischen Umfang und die erwarteten Auswirkungen des finanzierten Projekts.

• 030202 - Animal models

Aufforderung zur Vorschlagseinreichung

Verfahren zur Aufforderung zur Einreichung von Projektvorschlägen mit dem Ziel, eine EU-Finanzierung zu erhalten.

Finanzierungsplan

Finanzierungsregelung (oder „Art der Maßnahme“) innerhalb eines Programms mit gemeinsamen Merkmalen. Sieht folgendes vor: den Umfang der finanzierten Maßnahmen, den Erstattungssatz, spezifische Bewertungskriterien für die Finanzierung und die Verwendung vereinfachter Kostenformen wie Pauschalbeträge.

CSC - Cost-sharing contracts

Koordinator

Beteiligte (7)