4.6 Article

Enhancing In Vivo Survival of Adipose-Derived Stromal Cells Through BcI-2 Overexpression Using a Minicircle Vector

Journal

STEM CELLS TRANSLATIONAL MEDICINE
Volume 2, Issue 9, Pages 690-702

Publisher

WILEY
DOI: 10.5966/sctm.2013-0035

Keywords

Apoptosis; Adult stem cells; Cellular therapy; Gene delivery systems in vivo or in vitro

Funding

  1. NIH [1 R21 DE019274-01, RC2 DE020771, RC1 HL100490, 5U011-IL099776, R01-HL058770]
  2. Oak Foundation
  3. California Institute for Regenerative Medicine Grant [RL1-00662]
  4. Hagey Laboratory for Pediatric Regenerative Medicine

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Tissue regeneration using progenitor cell-based therapy has the potential to aid in the healing of a diverse range of pathologies, ranging from short-gut syndrome to spinal cord lesions. However, there are numerous hurdles to be overcome prior to the widespread application of these cells in the clinical setting. One of the primary barriers to effective stem cell therapy is the hostile environment that progenitor cells encounter in the clinical injury wound setting. In order to promote cellular survival, stem cell differentiation, and participation in tissue regeneration, relevant cells and delivery scaffolds must be paired with strategies to prevent cell death to ensure that these cells can survive to form de novo tissue. The BcI-2 protein is a prosurvival member of a family of proteins that regulate the mitochondrial pathway of apoptosis. Using several strategies to overexpress the BcI-2 protein, we demonstrated a decrease in the mediators of apoptosis in vitro and in vivo. This was shown through the use of two different clinical tissue repair models. Cells overexpressing BcI-2 not only survived within the wound environment at a statistically significantly higher rate than control cells, but also increased tissue regeneration. Finally, we used a nonintegrating minicircle technology to achieve this in a potentially clinically applicable strategy for stem cell therapy.

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