A single d(GpG) cisplatin adduct on the estrogen response element decreases the binding of the estrogen receptor

Both cisplatin and the estrogen receptor (ER) are known to bend DNA. The in fluence of the bending of sequences by the d(GpC)cisPt adduct binding of ER to estrogen response element (ERE)-like sequences was examined, Three ERE- like oligonucleotides with different affinities for ER and which include a GG in the linker sequence mere designed in order to form a single central d (GpG)cisPt adduct, Using electrophoretic mobility shift assay and Scatchard analysis, it was shown that the presence of a single d(GpG)cisPt adduct in the linker sequence decreases the ER affinity for DNA. These results do no t support a critical role of a DNA bend in the initial recognition of ERE b y ER, Then, the platination of DNA outside of the ERE half-sites decreases the interaction of ER with ERE. (C) 2000 Federation of European Biochemical Societies.