Abstract

Increased levels of serum ferritin in breast carcinoma is well known, however, its exact source has been disputed. Weinstein et al found six times the ferritin concentration in malignant tissue as compared to benign tissue. The anaplastic tumors had the highest ferritin concentrations, suggesting that the major site of the increased ferritin was the malignant epithelium. We found in a previous cytosolic and electron microscopic study of tissue ferritin in breast carcinoma that the malignant epithelium is almost certainly the source of the increased ferritin.To better define and expand this study and increase our knowledge of the role of transferrin receptors and iron metabolism in breast cancer, we began an immunocytochemical study of tissue ferritin to compliment our cytosol and ultrastructural observations. This was done with a mouse antihuman ferritin monoclonal antibody. To date 92 specimens have been examined by all three techniques. Immunocytochemical tissue slides showed intense staining of the cytoplasm with immunoperoxidase, and the intensity of the cytoplasmic staining correlated with the cytosolic concentrations and the electron microscopic findings.

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