AI Article Synopsis

  • NSCs show potential for treating central nervous system disorders but face significant challenges with survival rates after transplantation, as only a small fraction remain viable long-term.
  • Initial studies reveal that up to 80% of grafted NSCs may die within the first 24 hours due to a hypoxic environment, leading to strong immune system responses in the brain.
  • The survival of NSCs worsens over time, dropping to about 1% of the initial number, highlighting the need for a better understanding of these early post-transplantation processes to improve therapeutic outcomes.

Article Abstract

Introduction: Transplantation of neural stem cells (NSCs) is increasingly suggested to become part of future therapeutic approaches to improve functional outcome of various central nervous system disorders. However, recently it has become clear that only a small fraction of grafted NSCs display long-term survival in the (injured) adult mouse brain. Given the clinical invasiveness of NSC grafting into brain tissue, profound characterisation and understanding of early post-transplantation events is imperative to claim safety and efficacy of cell-based interventions.

Methods: Here, we applied in vivo bioluminescence imaging (BLI) and post-mortem quantitative histological analysis to determine the localisation and survival of grafted NSCs at early time points post-transplantation.

Results: An initial dramatic cell loss (up to 80% of grafted cells) due to apoptosis could be observed within the first 24 hours post-implantation, coinciding with a highly hypoxic NSC graft environment. Subsequently, strong spatiotemporal microglial and astroglial cell responses were initiated, which stabilised by day 5 post-implantation and remained present during the whole observation period. Moreover, the increase in astrocyte density was associated with a high degree of astroglial scarring within and surrounding the graft site. During the two-week follow up in this study, the NSC graft site underwent extensive remodelling with NSC graft survival further declining to around 1% of the initial number of grafted cells.

Conclusions: The present study quantitatively describes the early post-transplantation events following NSC grafting in the adult mouse brain and warrants that such intervention is directly associated with a high degree of cell loss, subsequently followed by strong glial cell responses.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3580486PMC
http://dx.doi.org/10.1186/scrt147DOI Listing

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