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  4. Core-Shell Structure of Organic Crystalline Nanoparticles Determined by Relayed Dynamic Nuclear Polarization NMR
 
research article

Core-Shell Structure of Organic Crystalline Nanoparticles Determined by Relayed Dynamic Nuclear Polarization NMR

Pinon, Arthur C.  
•
Skantze, Urban
•
Viger-Gravel, Jasmine
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November 8, 2018
The Journal of Physical Chemistry A

The structure of crystalline nanoparticles (CNPs) is determined using dynamic nuclear polarization (DNP) enhanced NMR spectroscopy experiments. The CNPs are composed of a crystalline core containing an active pharmaceutical ingredient (compound P), coated with a layer of PEG (DSPE-PEG 5000) located at the crystal surface, in a D2O suspension. Relayed DNP experiments are performed to study H-1-H-1 spin diffusion and to determine the size of the crystalline core as well as the thickness of the PEG overlayer. This is achieved through selective doping to create a heterogeneous system in which the D2O contains glycerol and organic radicals, which act as polarization sources, and the CNPs are exempt of radical molecules. We observe features that are characteristic of a core-shell system: high and constant DNP enhancement for components located in the surrounding radical solution, short build-up times for the PEG layer, and longer build-up times and time dependent enhancements for compound P. By comparing numerical simulations and experimental data, we propose a structural model for the CNPs with a core-shell organization and a high affinity between the radical and the PEG molecules.

  • Details
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Type
research article
DOI
10.1021/acs.jpca.8b08630
Web of Science ID

WOS:000449889100011

Author(s)
Pinon, Arthur C.  
Skantze, Urban
Viger-Gravel, Jasmine
Schantz, Staffan
Emsley, Lyndon  
Date Issued

2018-11-08

Publisher

AMER CHEMICAL SOC

Published in
The Journal of Physical Chemistry A
Volume

122

Issue

44

Start page

8802

End page

8807

Subjects

Chemistry, Physical

•

Physics, Atomic, Molecular & Chemical

•

Chemistry

•

Physics

•

nanocrystal formulations

•

drug

•

size

•

spectroscopy

•

diffusion

•

efficient

•

polymers

•

delivery

•

surface

•

peg

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LRM  
ISIC-GE  
Available on Infoscience
December 13, 2018
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/152147
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