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

Protein Dynamics in Antiviral Processes

Descripción del proyecto

Desvelar los moduladores clave de la inmunidad antivírica

Provocar una respuesta inmunitaria frente a los virus tiene una importancia vital para la salud humana. El proyecto ProDAP, financiado con fondos europeos, está investigando las interacciones entre las proteínas derivadas del virus y del hospedador que regulan las respuestas de las células inmunitarias. Los investigadores han identificado, mediante espectrometría de masas y modelización estadística, las proteínas del hospedador que, ante la infección vírica, alteran su capacidad de interacción o tasa de rotación. Estas proteínas parecen ser vitales para la inmunidad antivírica y su caracterización detallada ayudará a analizar minuciosamente las complejas vías de la respuesta inmunitaria. Se espera que la información sobre la regulación de la interacción hospedador-patógeno conduzca a nuevas estrategias antivíricas.

Objetivo

The innate antiviral defense system is of central importance to protect from viral pathogens. Its ability to mitigate a detrimental outcome of an infectious event relies on interactions that happen between viral and host-derived proteins as well as on signalling cascades that regulate the cellular response. However, despite the importance of these interactions, the involved processes and proteins are not yet fully understood.

We established state of the art mass spectrometry techniques and statistical modelling to characterise protein-protein interactions that are affected by viruses. We identified a class of proteins we name “viral affected proteins changing their interaction” (iVAPs). In addition, we established protein turnover rates of >6900 proteins in virus infected cells and identified a group of “viral affected proteins changing turnover rates” (tVAPs). tVAPs are regulated on basis of protein stabilisation, degradation or translation. Preliminary experiments show critical importance of iVAPs and tVAPs in antiviral immunity, suggesting functional similarities to Interferon stimulated genes (ISGs). Alike ISGs, VAPs therefore represent a critical component of the immune system.

ProDAP will establish the function of iVAPs and tVAPs in the antiviral immune response. Systematic screens employing depletion and overexpression experiments, integration of these data in functional networks and mechanistic follow up studies will be performed. Already identified and new candidate proteins will be tested mechanistically for their immune-regulatory capacity and their influence on virus infections in vitro and in vivo.

ProDAP will allow insights in yet unstudied modulators of host-pathogen interplay and will influence our current understanding of immune regulation in general. It is well established that ISGs are of central importance to defend virus infections and we hypothesize that VAPs may fulfil a similarly important protective function that has yet not been elucid

Palabras clave

Régimen de financiación

ERC-COG - Consolidator Grant

Institución de acogida

TECHNISCHE UNIVERSITAET MUENCHEN
Aportación neta de la UEn
€ 2 169 555,00
Dirección
Arcisstrasse 21
80333 Muenchen
Alemania

Ver en el mapa

Región
Bayern Oberbayern München, Kreisfreie Stadt
Tipo de actividad
Higher or Secondary Education Establishments
Enlaces
Coste total
€ 2 169 555,00

Beneficiarios (1)