DocumentCode :
386570
Title :
Cardiac cell networks on elastic microgrooved scaffolds
Author :
Bien, H. ; Yin, L. ; Entcheva, E.
Author_Institution :
Dept. of Biomed. Eng., State Univ. of New York, Stony Brook, NY, USA
Volume :
1
fYear :
2002
fDate :
2002
Firstpage :
788
Abstract :
We tested the potential of elastic topographically-modified (EM) scaffolds to serve as an atrophy countermeasure for engineered cardiac cell constructs. We compared the structural and electromechanical characteristics of cardiac syncytia on flat rigid and elastic microgrooved scaffolds, cultured and tested under identical conditions. Our paired test analysis demonstrated a significant increase (with respect to control) in sustained synchronous contractile activity, diastolic Ca2+ (>115%), systolic Ca2+ levels (>200%), maximum upstroke velocity (>440%) and maximum recovery velocity (>600%) in the EM-grown cell constructs (n=9 pairs, p<0.005 for all parameters). 3D reconstructions of confocal immunocy-to-chemistry images of cell cytoskeleton and gap junctional proteins (Connexin 43) confirmed a more mature in vivo-like intra- and inter-cellular organization for the EM case. Our results suggest that self-organized cell activity in response to the supporting matrix might effectively mimic anti-atrophy effects reported for external electrical or mechanical stimulation. We conclude, that topographically-modified elastic scaffolds might serve as strong positive inotropic effectors, can promote self-organized synchronous mechanical and electrical activity, and therefore produce structurally and functionally superior cardiac tissue equivalents with improved viability.
Keywords :
biochemistry; bioelectric potentials; biological specimen preparation; biological tissues; biomechanics; biomembrane transport; cardiology; cellular biophysics; 3D reconstructions; Ca; Connexin 43; anti-atrophy effects; atrophy countermeasure; cardiac cell networks; cardiac syncytia; cell cytoskeleton; confocal immunocytochemistry images; diastolic Ca2+ levels; elastic microgrooved scaffolds; elastic topographically-modified scaffolds; electrical activity; electromechanical characteristics; engineered cardiac cell constructs; external electrical stimulation; flat rigid scaffolds; functionally superior cardiac tissue equivalents; gap junctional proteins; identical conditions; inter-cellular organization; intra-cellular organization; maximum recovery velocity; maximum upstroke velocity; mechanical activity; mechanical stimulation; paired test analysis; self-organized cell activity; self-organized synchronous activity; strong positive inotropic effectors; structural characteristics; structurally superior cardiac tissue equivalents; supporting matrix; sustained synchronous contractile activity; systolic Ca2+ levels; topographically-modified elastic scaffolds; Atrophy; Biomedical engineering; Calcium; Cells (biology); Image analysis; Image reconstruction; Immune system; Proteins; Testing; Velocity control;
fLanguage :
English
Publisher :
ieee
Conference_Titel :
Engineering in Medicine and Biology, 2002. 24th Annual Conference and the Annual Fall Meeting of the Biomedical Engineering Society EMBS/BMES Conference, 2002. Proceedings of the Second Joint
ISSN :
1094-687X
Print_ISBN :
0-7803-7612-9
Type :
conf
DOI :
10.1109/IEMBS.2002.1137073
Filename :
1137073
Link To Document :
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