Modeling and in vitro and in vivo characterization of a tissue engineered pancreatic substitute |
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| Authors: | C L Stabler C Fraker E Pedraza I Constantinidis A Sambanis |
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| Institution: | (1) Discipline of Marine Biotechnology &; Ecology, Central Salt and Marine Chemicals Research Institute, Gijubhai Badheka Marg, Bhavnagar, 364 002, Gujarat, India;(2) Department of Nano-structured &; Advanced Materials, Graduate School of Science and Engineering, Kagoshima University, 1–21–40 Korimoto, Kagoshima 890-0065, Japan; |
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| Abstract: | In designing appropriate devices for the development of a functional pancreatic substitute, computational models capable of
accurately predicting cellular behavior constitute a critical aspect. This study investigated the model-based design, fabrication
and in vitro and in vivo experimental characterization of a pancreatic substitute consisting of mouse insulinoma cells encapsulated in agarose in
a disk-shaped construct. Two construct prototypes were examined: (i) a single disk construct comprised of agarose and βTC3 cells; and (ii) a buffered disk construct, consisting of agarose and βTC3 cells, coated with an additional layer of pure agarose. Diffusional studies of glucose and insulin were performed to characterize
the transport properties of the material. Three dimensional oxygen diffusion-reaction models were used to predict the appropriate
cell loadings for the two construct prototypes under varying external oxygen tensions. In vitro and in vivo experiments found the overall viable cell number for each construct prototype plateaued to the same value, regardless of
the initial cell seeding number, when constructs were placed under identical environmental conditions. Furthermore, mathematical
model calculations correlated well with experimental in vitro and in vivo results of cell viability, indicating oxygen tension to be the dominating factor in establishing total viable cell number
in these constructs. These results indicate that the development of a computational model capable of accurately predicting
overall cell viability is useful for the development of tissue engineered constructs, when permissive matrices and continuous
cell lines are used. The applicability of this modeling and experimental methodology in the development of agarose-based constructs
for use as a bioartificial pancreas is discussed.
The authors would like to dedicate this paper to the memory of the colleague, friend, and mentor Professor Ioannis (Yanni)
Constantinidis, who died suddenly and untimely on April 16, 2006. |
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| Keywords: | Tissue construct modeling Pancreatic substitute Agarose Encapsulated cells β TC3 insulinoma cells |
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