AI Article Synopsis

  • Researchers are exploring stem cell-derived insulin producing cells (IPCs) as a potential alternative to traditional islet transplantation for treating diabetes.
  • Current methods to differentiate stem cells into IPCs are lengthy and complex, but this study shows that bone marrow nucleated cells (BMNCs) can be converted into IPCs more efficiently using conditioned media from stressed pancreatic β-cells.
  • This method produced IPCs that expressed key insulin-producing markers, improved diabetic conditions in mice, and suggests that differentiating factors are contained within micro particles rather than being released as soluble substances.

Article Abstract

Transplantation of stem cell-derived insulin producing cells (IPCs) has been proposed as an alternative to islet transplantation for the treatment of diabetes mellitus. However, current IPC differentiation protocols are focused on generating functional cells from the pluripotent stem cells and tend to rely on multistep, long-term exposure to various exogenous factors. In this study, we addressed the observation that under stress, pancreatic β-cells release essential components that direct the differentiation of the bone marrow nucleated cells (BMNCs) into IPCs. Without any supplementation with known differentiation-inducing factors, IPCs can be generated from BMNCs by in vitro priming for 6 days with conditioned media (CM) from the β-cells. In vitro primed BMNCs expressed the β-cell-specific transcription factors, as well as insulin, and improved hyperglycemia and glucose intolerance after transplantation into the streptozotocin-induced diabetic mice. Furthermore, we have found that components of the CM which trigger the differentiation were enclosed by or integrated into micro particles (MPs), rather than being secreted as soluble factors. Identification of these differentiation-directing factors might enable us to develop novel technologies required for the production of clinically applicable IPCs.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6441031PMC
http://dx.doi.org/10.1038/s41598-019-41823-9DOI Listing

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