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  5. Influence of Surface Groups on Poly(propylene imine) Dendrimers Antiprion Activity
 
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Influence of Surface Groups on Poly(propylene imine) Dendrimers Antiprion Activity

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Download Biomacromolecules.pdf2.9 MB
Author(s)
McCarthy, James M. 
Moreno, Beatriz Rasines 
Filippini, Damien 
Komber, Hartmut 
Maly, Marek 
Cernescu, Michaela 
Brutschy, Bernhard 
Appelhans, Dietmar 
Rogers, Mark S. 
Uri
http://hdl.handle.net/10197/4251
Date Issued
12 December 2012
Date Available
15T13:35:18Z April 2013
Abstract
Prion diseases are characterized by the accumulation of PrP(Sc), an aberrantly folded isoform of the host protein PrP(C). Specific forms of synthetic molecules known as dendrimers are able to eliminate protease-resistant PrP(Sc) in both an intracellular and in vitro setting. The properties of a dendrimer which govern this ability are unknown. We addressed the issue by comparing the in vitro antiprion ability of numerous modified poly(propylene-imine) dendrimers, which varied in size, structure, charge, and surface group composition. Several of the modified dendrimers, including an anionic glycodendrimer, reduced the level of protease resistant PrP(Sc) in a prion strain-dependent manner. This led to the formulation of a new working model for dendrimer/prion interactions which proposes dendrimers eliminate PrP(Sc) by destabilizing the protein and rendering it susceptible to proteolysis. This ability is not dependent on any particular charge of dendrimer, but does require a high density of reactive surface groups.
Type of Material
Journal Article
Publisher
American Chemical Society
Journal
Biomacromolecules
Volume
14
Issue
1
Start Page
27
End Page
37
Copyright (Published Version)
2012, American Chemical Society
Keywords
  • Dendrimers

  • PrPSc

  • Prions

DOI
10.1021/bm301165u
Language
English
Status of Item
Peer reviewed
This item is made available under a Creative Commons License
https://creativecommons.org/licenses/by-nc-nd/3.0/ie/
Owning collection
Biology & Environmental Science Research Collection
Scopus© citations
42
Acquisition Date
Feb 5, 2023
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1739
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