Hematopoiesis-supportive function of growth-arrested human adipose-tissue stromal cells under physiological hypoxia

Ex vivo expansion of hematopoietic progenitors is considered as an attractive tool to increase the number of stem and progenitor cells (HSPCs) for cell therapy. The efficacy of ex vivo expansion is strongly depends on the feeder cell activity to mimic hematopoietic microenvironment. Here we demonstrated, that combination of mitomycin C-induced growth arrest and tissue-related O 2 (physiological hypoxia) modulated stromal capacity of adipose tissue derived stromal cells (ASCs). Growth arrest did not affect viability, stromal phenotype and multilineage potential of ASCs permanently expanded at tissue-related O 2 . Meanwhile, the PCR analysis revealed an up-regulation of genes, encoded molecules of cell–cell ( ICAM1 , HCAM/CD44 ) and cell–matrix adhesion ( ITGs ), extracellular matrix production ( COLs ) and remodeling ( MMPs , HAS1 ) in growth-arrested ASCs at physiological hypoxia in comparison with ambient O 2 (20%). The number of ICAM-1 positive ASCs was increased under low O 2 as well. These alterations contributed into the ex vivo expansion of cord blood HSPCs providing the preferential production of primitive HSPCs. The number of cobblestone area forming cell (CAFC) colonies was 1.5-fold higher at physiological hypoxia ( p in vivo . The presented data may be applicable in the development of upscale protocols of HSPC expansion.