AI Article Synopsis

  • Tissue engineering strategies for hepatocyte transplantation face challenges due to high cell death rates post-transplant.
  • Researchers modified a delivery system to include VEGF, EGF, and HGF to improve hepatocyte survival and monitored them in SCID mice for two weeks.
  • While a short-term increase in survival was noted due to VEGF, long-term survival remained unchanged, highlighting the complexity of the factors influencing hepatocyte engraftment.

Article Abstract

Tissue engineering approaches have been investigated as a strategy for hepatocyte transplantation; however the death of a majority of transplanted cells critically limits success of these approaches. In a previous study, a transient increase in hepatocyte survival was achieved through delivery of vascular endothelial growth factor (VEGF) from the porous polymer scaffold utilized for cell delivery. To enhance longer-term survival of the hepatocytes, this delivery system was modified to additionally deliver epidermal growth factor (EGF) and hepatocyte growth factor (HGF) in a sustained manner. Hepatocytes were subcutaneously implanted in SCID mice on scaffolds containing EGF and/or HGF, in addition to VEGF, and survival was monitored for two weeks. A short-term enhancement of hepatocyte survival was observed after one week and is attributed to VEGF-enhanced vascularization, which was not altered by EGF or HGF. Surprisingly, long-term hepatocyte engraftment was not improved, as survival declined to the level of control conditions for all growth factor combinations after two weeks. This investigation indicates that the survival of hepatocytes transplanted into heterotopic locations is dependent on multiple signals. The delivery system developed for the current study may be useful in elucidating the specific factors controlling this process, and bring therapeutic transplantation of hepatocytes closer to implementation.

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Source
http://dx.doi.org/10.1089/ten.2006.12.235DOI Listing

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