Monoclonal antibodies to early pregnancy factor perturb tumour cell growth
Corresponding Author
K. A. QUINN
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
K. A. Quinn, Department of Surgery, University of Queensland, Clinical Sciences Building, Royal Brisbane Hospital, Herston Qld 4029, Brisbane, Australia.Search for more papers by this authorS. ATHANASAS-PLATSIS
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorT.-Y. WONG
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorB.E. ROLFE
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorA. C. CAVANAGH
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorH. MORTON
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorCorresponding Author
K. A. QUINN
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
K. A. Quinn, Department of Surgery, University of Queensland, Clinical Sciences Building, Royal Brisbane Hospital, Herston Qld 4029, Brisbane, Australia.Search for more papers by this authorS. ATHANASAS-PLATSIS
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorT.-Y. WONG
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorB.E. ROLFE
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorA. C. CAVANAGH
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorH. MORTON
Department of Surgery, University of Queensland, Royal Brisbane Hospital, Brisbane, Australia
Search for more papers by this authorSUMMARY
The pregnancy-associated substance early pregnancy factor (EPF) has previously been reported as a product of tumours of germ cell origin. More recently EPF (or an EPF-related substance, tEPF) has also been detected in the serum of patients bearing tumours of non-germ cell origin. We report here the production of tEPF by a variety of cultured transformed and tumour cell lines, of both germ and non-germ cell origin. Antibodies specific for EPF remove all tEPF activity from tumour cell conditioned medium, tEPF production is found to be associated with cell division; tEPF is no longer detected after growth arrest or differentiation. Co-culture of tumour cells with increasing doses of anti-EPF monoclonal antibodies resulted in a significant, dose-dependent decrease in rate of cell growth and viability. Similar anti-EPF concentrations had no effect on the concanavalin A induced proliferation of mouse spleen cells. These studies suggest, therefore, that tEPF is a growth-regulated product of cultured tumour and transformed cells. These cells are also dependent upon tEPF for continued growth, i.e. tEPF is acting in the autocrine mode.
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