Ovarian epithelial cell lineage-specific gene expression using the promoter of a retrovirus-like element

We have isolated 462 bp of sequence termed ovarian-specific promoter 1 (OSP -1) that is part of a retrovirus-like element specifically expressed in the rat ovary. We have evaluated the ability of OSP-1 to activate gene express ion in normal and neoplastic cell lines derived from the ovaries of rats an d women. We have found that there was marked specificity in the ability of OSP-1 to drive reporter gene expression in an ovarian epithelial fell linea ge manner. The expression of herpes simplex virus thymidine kinase (HSV-TK) under OSP-1 control was sufficiently ovarian cancer cell line specific to render ganciclovir similar to 50-fold more toxic in the A2780 human ovarian cancer cell line compared with clones of the HCT-116 and HT-29 colon cance r cell lines. Furthermore, ganciclovir had marked antitumor efficacy in viv o in severe combined immunodeficient mice bearing A2780(OSP-1-HSV-TK) as a s.c. xenograft. We suggest that these data support the use of OSP-1 as a to ol to provide specificity to the gene therapy of ovarian cancer and to driv e ovarian-specific oncogene expression for the creation of transgenic mouse models of ovarian cancer.