PROTEINLOCALIZATION

Finding New Mechanisms for Protein Localization in Bacteria

 Coordinatore INSTITUTO DE TECNOLOGIA QUIMICA E BIOLOGICA - UNIVERSIDADE NOVA DE LISBOA 

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 Nazionalità Coordinatore Portugal [PT]
 Totale costo 1˙656˙960 €
 EC contributo 1˙656˙960 €
 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-2012-StG_20111109
 Funding Scheme ERC-SG
 Anno di inizio 2013
 Periodo (anno-mese-giorno) 2013-03-01   -   2018-02-28

 Partecipanti

# participant  country  role  EC contrib. [€] 
1    INSTITUTO DE TECNOLOGIA QUIMICA E BIOLOGICA - UNIVERSIDADE NOVA DE LISBOA

 Organization address address: "Avenida da Republica, Estacao Agronomica Nacional"
city: OEIRAS
postcode: 2784-505

contact info
Titolo: Dr.
Nome: Maria Lurdes
Cognome: Conceição
Email: send email
Telefono: +351 214469229
Fax: +351 214469314

PT (OEIRAS) hostInstitution 1˙656˙960.00
2    INSTITUTO DE TECNOLOGIA QUIMICA E BIOLOGICA - UNIVERSIDADE NOVA DE LISBOA

 Organization address address: "Avenida da Republica, Estacao Agronomica Nacional"
city: OEIRAS
postcode: 2784-505

contact info
Titolo: Dr.
Nome: Mariana Luisa
Cognome: Tomàs Gomes De Pinho
Email: send email
Telefono: +351 214469527
Fax: 0

PT (OEIRAS) hostInstitution 1˙656˙960.00

Mappa


 Word cloud

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inflammatory    components    protein    enzymes    peptidoglycan    recognition    surface    cell    acids    assembly    localization    metabolic    responsible    host    synthesis    bacterial   

 Obiettivo del progetto (Objective)

'During infection, the host immune system interacts with the bacterial cell surface, a complex structure made of peptidoglycan, wall teichoic acids, lipoteichoic acids, capsule polysaccharide and peptidoglycan-attached proteins. A lot is known about the metabolic pathways for the synthesis of each individual cell surface component. Almost nothing is known about the coordination between the synthesis of the peptidoglycan, the major structural component of the cell surface and the main inflammatory component of gram-positive bacteria, and the synthesis of the other molecules present at the surface. However, this coordination is essential for the construction of a surface capable not only of performing its biological functions in cell protection and morphology, but also of masking its inflammatory components for evasion from host recognition.

Using the clinical pathogen Staphylococcus aureus as a model organism, we propose to investigate the temporal and spatial regulation of the enzymes responsible for the synthesis of the cell surface components, as well as their dependence on the underlying divisome.

We will (i) use state-of –the art fluorescence microscopy to localize fluorescent derivatives of enzymes required for cell surface synthesis; (ii) use libraries of antibiotics, of antisense RNA expression plasmids, and of transposon mutants to identify the order of assembly and requirements for the localization of cell surface synthesis enzymes; (iii) identify the exact metabolic compound/protein/geometric cue responsible for the localization of key enzymes; (iv) determine if cells with impaired surface synthesis due to protein delocalization are more susceptible to host recognition and therefore less capable of causing infections.

This project will result in the identification of new mechanisms of protein localization, a fundamental question in cell biology, and in a better understanding of the assembly of the bacterial cell surface of successful bacterial pathogens'

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