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Improved angiogenic cell penetration in vitro and in vivo in collagen scaffolds with internal channels

Abstract:
Porous scaffolds are limited in volume due to diffusion constraint and delay of vascular network formation. Channels have the potential to speed up cellular penetration. Their effectiveness in improving angiogenic cell penetration was assessed in vitro and in vivo in 3-D collagen scaffolds. In vitro, channelled and non-channelled scaffolds were seeded with vascular smooth muscle cells. Results demonstrated that the scaffolds supported angiogenic cell ingrowth in culture and the channels improved the depth of cell penetration into the scaffold (P < 0.05). The cells reside mainly around and migrate along the channels. In vivo, channels increased cell migration into the scaffolds (P < 0.05) particularly angiogenic cells (P < 0.05) resulting in a clear branched vascular network of microvessels after 2 weeks in the channelled samples which was not apparent in the non-channelled samples. Channels could aid production of tissue engineered constructs by offering the possibility of rapid blood vessel infiltration into collagen scaffolds. © 2013 Springer Science+Business Media New York.

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Publisher copy:
10.1007/s10856-013-4912-7

Authors


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Institution:
University of Oxford
Division:
MPLS
Department:
Materials
Role:
Author


Journal:
Journal of Materials Science: Materials in Medicine More from this journal
Volume:
24
Issue:
6
Pages:
1571-1580
Publication date:
2013-06-01
DOI:
EISSN:
1573-4838
ISSN:
0957-4530


Language:
English
Pubs id:
pubs:410053
UUID:
uuid:c05fa890-1d66-46f4-8762-536bce6e0181
Local pid:
pubs:410053
Source identifiers:
410053
Deposit date:
2013-11-16

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