Publication:

Acrylic acid grafting and collagen immobilization on poly(ethylene terephthalate) surfaces for adherence and growth of human bladder smooth muscle cells

cris.lastimport.scopus

2024-08-08T08:50:09Z

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105000

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PH-SV

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ISIC

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SB

cris.virtual.parent-organization

EPFL

cris.virtual.sciperId

107554

cris.virtual.unitId

10180

cris.virtual.unitManager

Oates, Andrew Charles

cris.virtual.unitManager

Wurm, Florian Maria

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ed979eea-c2f0-4e70-afa3-e4871afb1fd1

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datacite.rights

metadata-only

dc.contributor.author

Bisson, I.

dc.contributor.author

Kosinski, M.

dc.contributor.author

Ruault, S.

dc.contributor.author

Gupta, B.

dc.contributor.author

Hilborn, J.

dc.contributor.author

Wurm, F.

dc.contributor.author

Frey, P.

dc.date.accessioned

2007-06-05T13:24:55

dc.date.available

2007-06-05T13:24:55

dc.date.created

2007-06-05

dc.date.issued

2002

dc.date.modified

2024-10-17T18:27:41.228960Z

dc.description.abstract

In tissue engineering, degradable or non-degradable polymer matrices can act as cell-carrier-scaffolds. Cell adhesion and growth on these scaffolds can be promoted by immobilizing extracellular matrix proteins. Therefore, in this study, polymer poly(ethylene terephthalate) (PET) films were surface modified by graft polymerization of acrylic acid, to subsequently allow collagen (types I and III) immobilization and human smooth muscle cell expansion. The surfaces of PET were activated by plasma, followed by acrylic acid graft polymerization, resulting in covalently bound brushes, containing an average of either 0.22+/-0.1 or 5.93+/-0.87 microg/cm2 of poly(acrylic acid) (PAA). Subsequent electrostatic adsorption of collagen gave a surface concentration of 4.96 and 17.2 microg/cm2, respectively, as determined using radiolabelled 125I collagen. Both PET films grafted with 0.22 microg/cm2 of PAA with or without adsorbed collagen were apt for smooth muscle cell adhesion and proliferation. However, films grafted with 5.93 microg/cm2 were not. PAA-grafted PET films, onto which serum proteins of the culture medium adsorbed spontaneously, proved to be better matrices than films on which collagen has been immobilized. It, therefore, can be speculated that other serum proteins are more important than collagen for the human smooth muscle cell adhesion and growth on surface-modified polymer matrices.

dc.description.notes

Centre Hospitalier Universitaire Vaudois, Department of Pediatric Surgery, Lausanne, Switzerland. isabisson@hotmail.com

dc.description.notes

Journal Article

dc.description.notes

Research Support, Non-U.S. Gov't

dc.description.notes

England

dc.description.sponsorship

LBTC

dc.identifier.doi

10.1016/S0142-9612(02)00061-3

dc.identifier.isi

WOS:000176268800010

dc.identifier.pmid

12102186

dc.identifier.uri

https://infoscience.epfl.ch/handle/20.500.14299/7626

dc.relation.issn

0142-9612

dc.relation.journal

Biomaterials

dc.subject

Acrylic Resins

dc.subject

*Biocompatible Materials

dc.subject

Cell Adhesion

dc.subject

Cell Division

dc.subject

Cells

dc.subject

Cultured

dc.subject

Cells

dc.subject

Immobilized

dc.subject

Collagen

dc.subject

Humans

dc.subject

Materials Testing

dc.subject

Microscopy

dc.subject

Electron

dc.subject

Scanning

dc.subject

Muscle

dc.subject

Smooth/*cytology

dc.subject

*Polyethylene Terephthalates

dc.subject

Surface Properties

dc.subject

Tissue Engineering

dc.subject

Urinary Bladder/*chemistry

dc.title

Acrylic acid grafting and collagen immobilization on poly(ethylene terephthalate) surfaces for adherence and growth of human bladder smooth muscle cells

dc.type

text::journal::journal article::research article

dspace.entity.type

Publication

dspace.legacy.oai-identifier

oai:infoscience.epfl.ch:105000

epfl.legacy.itemtype

Journal Articles

epfl.legacy.submissionform

ARTICLE

epfl.oai.currentset

OpenAIREv4

epfl.oai.currentset

SV

epfl.oai.currentset

article

epfl.peerreviewed

REVIEWED

epfl.publication.version

http://purl.org/coar/version/c_970fb48d4fbd8a85

epfl.writtenAt

EPFL

oaire.citation.endPage

58

oaire.citation.issue

15

oaire.citation.startPage

3149

oaire.citation.volume

23

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