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rSAMs-NANO SIGNED

Nanoparticles with switchable shells for virus sensing and inhibition

Total Cost €

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EC-Contrib. €

0

Partnership

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 rSAMs-NANO project word cloud

Explore the words cloud of the rSAMs-NANO project. It provides you a very rough idea of what is the project "rSAMs-NANO" about.

saccharide    binding    free    surface    receptor    model    drugs    self    layer    multivalency    ligands    explored    biointerfacial    strategy    viruses    thiol    lipid    reversible    infection    inhibitors    influenza    sensing    nanoplasmonic    assemblies    tunable    density    fixed    strains    affinity    stages    antibody    sams    multivalent    shell    generation    sensors    validated    rapid    nature    biological    bilayers    biointerfaces    assays    assembled    select    antiviral    dendritic    weak    receptors    ebola    pathogens    entry    diagnostics    interactions    first    respect    particles    series    ligand    composition    human    contrast    nanoparticles    benchmark    nanoparticle    selectivity    group    prepare    multiple    interacting    versions    architectures    dynamic    detection    exploring    shells    efficiency    monolayers    particle    amidines    terminated    ultrasensitive    inhibition    animal    prevents    ph    enhanced    simultaneously    virus    affinities    subtyping    capability    responsiveness    stability    covalently    artificial    head    inhibit    situ    relying    featuring    decorated    switchable    saccharides    blocking    compromises    rsams    relies    drug   

Project "rSAMs-NANO" data sheet

The following table provides information about the project.

Coordinator
MALMO UNIVERSITET 

Organization address
address: NORDENSKIOLDSGATAN 1
city: MALMOE
postcode: 205 06
website: www.mah.se

contact info
title: n.a.
name: n.a.
surname: n.a.
function: n.a.
email: n.a.
telephone: n.a.
fax: n.a.

 Coordinator Country Sweden [SE]
 Total cost 185˙857 €
 EC max contribution 185˙857 € (100%)
 Programme 1. H2020-EU.1.3.2. (Nurturing excellence by means of cross-border and cross-sector mobility)
 Code Call H2020-MSCA-IF-2017
 Funding Scheme MSCA-IF-EF-CAR
 Starting year 2018
 Duration (year-month-day) from 2018-09-03   to  2020-09-02

 Partnership

Take a look of project's partnership.

# participants  country  role  EC contrib. [€] 
1    MALMO UNIVERSITET SE (MALMOE) coordinator 185˙857.00

Map

 Project objective

This proposal concerns Reversible Self-assembled Monolayers (rSAMs) as dynamic nanoparticle shells for multivalent interactions at biointerfaces. Current drug design and diagnostics are exploring the multivalency concept, i.e. binding of biological targets via multiple weak interactions. In contrast to classical drug design relying on high-affinity inhibitors, this relies on dendritic architectures featuring a high density of ligands, e.g. saccharides, capable of simultaneously interacting with biointerfacial receptors. This strategy can be used to inhibit the virus entry by blocking the receptor at the early stages of infection and the concept is being explored as antiviral drugs and in virus sensing. However, in current systems ligands are covalently fixed on the particle surface. This prevents control over the ligand distribution and composition which compromises selectivity and affinity of the interactions. rSAMs are pH-switchable versions of thiol-SAMs. They are tunable with respect to the nature of the head group and layer order and stability while featuring pH responsiveness and the dynamic nature of non-covalently build assemblies e.g. lipid bilayers. Ligand decorated rSAMs therefore feature strongly enhanced affinities for multivalent targets. The main aims of this proposal are: 1) to investigate the use of rSAMs as dynamic nanoparticle shells for multivalent inhibition of viruses and 2) to assess such systems as nanoplasmonic sensors for antibody-free ultrasensitive, robust and rapid in situ virus detection. Under 1) we will select model pathogens, e.g. Ebola and prepare a series of saccharide terminated amidines for the first generation dynamic shell nanoparticles.Their efficiency will be assessed in infection assays using artificial virus particles Under 2) we will develop influenza virus sensors with subtyping capability within human and animal virus strains. The sensors will be validated with respect to benchmark assays.

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