Functional characterization of an androgen response element in the first intron of the C3(1) gene of prostatic binding protein

Abstract

We demonstrate that the 204 bp intronic gene fragment of C3(1), which has a specific in vitro affinity for the androgen receptor, is able to confer androgen responsiveness to a heterologous promoter. This characteristic is completely destroyed by a single G → T substitution, affecting a 5′-TGTTCT-3′ element that closely resembles the consensus sequence of the glucocorticoid and progesterone response elements ( GRE PRE ). In fact we could show that this androgen response element (ARE) also acts as a similarly weak GRE or PRE in T-47D cells.