Differential activity of conditional MYC and its variant MYC-S in human mortal fibroblasts

We have explored the effects of the conditional MYC-estrogen receptor fusion protein, MYC-ERT(TM), in human mortal fibroblasts, WI38, on cell-cycle entry, apoptosis and gene expression, The results indicate that activation of MYC-ER(TM) in WI38 cells is sufficient to cause S phase entry of quiescent cells, which is preceded by phosphorylation of Rb and activation of the Cdk2-associated kinase, We also analysed the MYC protein variant, MYC-S, which lacks part of the transcriptional activation domain but includes the conserved MYC box II and 26 amino acids N-terminal to it, MYC-S was previously shown to promote proliferation and apoptosis of immortalized rodent cell lines, The results indicate that MYC-S has undetectable activity as an inducer of S phase or apoptosis of quiescent WI38 cells. However, Myc-S stimulates proliferation of WI38 cells in the presence of 10% fetal calf serum, Surprisingly, we found that MYC-S, previously considered solely a repressor of specific reporter genes, is instead a weak transactivator of endogenous target genes both in mortal and immortalized cells. In addition, MYC-S exhibit a weak repressor activity upon an endogenous target gene only in immortalized cells, MYC-S transcriptional properties suggest that MYC box II and the adjacent N-terminal amino acids, while not sufficient for full repression function, participate in transactivation of endogenous target genes.