RELATIONSHIP OF MONOCLONAL-ANTIBODY BINDING TO ESTROGEN AND PROGESTERONE-RECEPTOR CONTENT IN BREAST-CANCER

Abstract

Three monoclonal antibodies-H59, H71 and H72-which react with human breast cancer were developed using the estrogen-dependent human breast cancer cell line, ZR-75-1, as the immunogen. H59 bound only to estrogen receptor-positive, estrogen-regulated breast cancer cells in culture, whereas H71 and H72 bound breast cancer cells irrespective of the estrogen receptor content. Al 3 antibodies had minimal cross-reactivity with non-breast tissue culture cell lines. The 3 antigens appear to be glycoproteins located on the cell surface. H59 and H72 antigens bound preferentially to the apical surface of duct cells and may be secreted; H71 antigen demonstrated no evidence of an apical orientation or secretion. The binding of the antibodies to fixed cryosections from 152 breast cancer and 111 benign breast disease specimens was evaluated using a radioimmunoassay. Eight-five percent of breast cancer and almost 100% of benign disease specimens were bound by at least 1 antibody. H59 bound 39%, H71 bound 51% and H72 bound 65% of cancer specimens. Estrogen receptor and progesterone receptor analyses were obtained on 141 specimens. H59 bound almost exclusively to tumor specimens which contained estrogen and/or progesterone receptor, but not to all receptor-positive tumors. Therefore, the H59 antigen appeared to be present on a subset of estrogen receptor-positive tumors. Considering that it bound only to estrogen-regulated cells in culture, the antigen may be estrogen regulated and its presence may predict a response to hormone therapy. H71 and H72 recognized cell surface differentiation antigens but bound tumor specimens regardless of the receptor content. These antibodies may be useful as independent variables for predicting response to therapy and prognosis of patients with breast cancer.