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research article

Protein delivery from materials formed by self-selective conjugate addition reactions

Elbert, D. L.
•
Pratt, A. B.
•
Lutolf, M. P.  
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2001
Journal of Controlled Release

A new chem. crosslinking scheme was utilized for the formation of degradable poly(ethylene glycol) hydrogels suitable for the delivery of protein drugs. An aq. soln. contg. a PEG-multiacrylate and solid particles of albumin was mixed with an aq. soln. contg. a PEG-dithiol, rapidly producing a cross-linked hydrogel through a Michael-type addn. reaction. For some formulations, it was obsd. that about 65% of the incorporated protein was released with zero-order kinetics over a period of about 4 days. By changing the functionality of the cross-linker, the release of protein could even be delayed for about 4 days, followed by zero-order release. The mechanism for release appeared to be a combination of slow dissoln. of protein in the presence of PEG and hindered diffusion of protein through the gel. The crosslinking of the gels was studied rheometrically, and the hydrolytic degrdn. of the gels was characterized by measuring the swelling of the gels. Biochem. anal. of the released proteins demonstrated that the polymers reacted with each other, but not with proteins. Utilizing the Flory-Rehner and Peppas-Merrill equations, a framework for modeling the protein release from the gels is described. [on SciFinder (R)]

  • Details
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Type
research article
DOI
10.1016/S0168-3659(01)00398-4
Author(s)
Elbert, D. L.
Pratt, A. B.
Lutolf, M. P.  
Halstenberg, S.
Hubbell, J. A.  
Date Issued

2001

Published in
Journal of Controlled Release
Volume

76

Issue

1-2

Start page

11

End page

25

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LMRP  
UPLUT  
Available on Infoscience
February 27, 2006
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/226564
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