Restoration of C/EBPα in dedifferentiated liposarcoma induces G2/M cell cycle arrest and apoptosis.

[dedifferentiated liposarcoma]

Well-differentiated liposarcoma (WDLS ) and dedifferentiated liposarcoma (DDLS ) represent the most common biological group of liposarcoma , and there is a pressing need to develop targeted therapies for patients with advanced disease . To identify potential therapeutic targets , we sought to identify differences in the adipogenic pathways between DDLS , WDLS , and normal adipose tissue . In a microarray analysis of DDLS (n = 84 ), WDLS (n = 79 ), and normal fat (n = 23 ), C /EBPα , a transcription factor involved in cell cycle regulation and differentiation , was underexpressed in DDLS when compared to both WDLS and normal fat (15 .2 - and 27 .8 -fold , respectively ). In normal adipose-derived stem cells , C /EBPα expression was strongly induced when cells were cultured in differentiation media , but in three DDLS cell lines , this induction was nearly absent . We restored C /EBPα expression in one of the cell lines (DDLS 8817 ) by transfection of an inducible C /EBPα expression vector . Inducing C /EBPα expression reduced proliferation and caused cells to accumulate in G 2 /M . Under differentiation conditions , the cell proliferation was reduced further , and 66 % of the DDLS cells containing the inducible C /EBPα expression vector underwent apoptosis as demonstrated by annexin V staining . These cells in differentiation conditions expressed early adipocyte-specific mRNAs such as LPL and FABP 4 , but they failed to accumulate intracellular lipid droplets , a characteristic of mature adipocytes . These results demonstrate that loss of C /EBP α is an important factor in suppressing apoptosis and maintaining the dedifferentiated state in DDLS . Restoring C /EBPα may be a useful therapeutic approach for DDLS .