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MODELLING DIFFUSION

"Mathematical models for diffusion controlled systems: diffusion on cell membrane, cluster formation and maintenance"

Coordinatore	VIB Organization address address: Rijvisschestraat 120 city: ZWIJNAARDE - GENT postcode: 9052 contact info Titolo: Mr. Nome: Rik Cognome: Audenaert Email: send email Telefono: +32 9 244 66 11 Fax: +32 9 244 66 11
Nazionalità Coordinatore	Belgium [BE]
Totale costo	161˙600 €
EC contributo	161˙600 €
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-2009-IIF
Funding Scheme	MC-IIF
Anno di inizio	2010
Periodo (anno-mese-giorno)	2010-08-01 - 2012-02-15

Partecipanti

#	participant	country	role	EC contrib. [€]
1	VIB Organization address address: Rijvisschestraat 120 city: ZWIJNAARDE - GENT postcode: 9052 contact info Titolo: Mr. Nome: Rik Cognome: Audenaert Email: send email Telefono: +32 9 244 66 11 Fax: +32 9 244 66 11	BE (ZWIJNAARDE - GENT)	coordinator	161˙600.00

Mappa

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protein lateral assembly clusters polarity diffusion signaling data inhomogeneous models proteins cell stable mathematical membrane microdomains assumptions

Obiettivo del progetto (Objective)

'Assembly of transient and stable signaling platforms in the plasma membrane of cells has been implicated in functions as varied as death and survival, polarity, differentiation, migration, cell-cell communication, virus entry, exocytosis, endocytosis. Naturally, the assembly of signaling microdomains requires the use of most complex molecular mechanisms capable of transducing intrinsic or extrinsic information into the actual making of the domain. Consensus exist that the lateral diffusion and heterogeneity of membrane proteins is absolutely necessary. However, more and more data indicate that the clustering of specific proteins to form a signaling platform involves as well the free lateral diffusion of stable assemblies of sphingoipids and cholesterol (rafts). Despite their fundamental relevance for cell function, the basic events responsible for the formation and dynamics of membrane microdomains is not well understood. Mathematical models are very useful tools for describing diffusion processes in an inhomogeneous medium with some anomalies as well as self-organized systems. Hence, it is my plan to use mathematical models to study the formation of protein-lipid clusters and how normal diffusion on an inhomogeneous membrane can be modified. The formation of protein clusters is a necessary condition for cell polarity and it could be related with the generation of pattern. I will propose a Turing-mechanism model to know if it is possible to generate stable spatial inhomogeneity on the cell surface. In order to formulate the equations it will be needed to make some assumptions about the biological system. Made assumptions will be refused or accepted according to the comparative analysis between theoretical results and experimental data. My background in physics make me feel suitable for undertaking the task of modelling these features. The validation experiments will be performed in the laboratory of Prof. Carlos Dotti where I have chosen to carry out this project.'