Abstract

The nm23 gene family encodes nucleoside diphosphate kinases (NDPKs) which supply the cell with (d)NTPs. The human NDPKB, also known as the PuF protein, binds the c- myc promoter and transactivates the c- myc protooncogene. We have now studied the effects of mouse NDPKA and NDPKB overexpression on endogenous c- myc transactivation in the mouse BAF3 and the rat PC12 cell lines. c- myc transcripts were found to be up-regulated by NDPKB only in the BAF3 line. This suggests that c- myc transcriptional control via NDPKB depends on the presence of cell-specific co-factors. Unexpectedly, NDPKB also induced NDPKA expression. This new effect was found in both cell lines, suggesting that NDPKB-dependent nm23-M1 gene transactivation requires cis and/or trans elements different from those involved in c- myc transactivation. Moreover, the BAF3 cell proliferation capacities were found to be independent of NDPKA or B cell contents. Interestingly, cell death induced by c- myc overexpression or H 2O 2 exposure was decreased in nm23-transfected compared to control BAF3 cells. These data collectively suggest that NDPKs might improve cell survival by a mechanism coupling DNA repair and transcriptional regulation of genes involved in DNA damage response.

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