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J. Biol. Chem., Vol. 260, Issue 6, 3360-3367, Mar, 1985
LP Chandler, CE Chandler, M Hosang and EM Shooter
An epidermal growth factor (EGF) receptor-interactive monoclonal antibody
(151-IgG) that inhibits EGF binding to PC12 rat pheochromocytoma cells and
to various other cell types has been produced. The hybridoma clone was
obtained by fusing Sp2/O-Ag14 myeloma cells with splenocytes from Balb/C
mice which had been immunized with n- octyl glucoside-solubilized protein
from isolated PC12 cell plasma membranes. The antibody is an IgG which
binds to protein A. 151-IgG did not bind EGF. At 0.5 degrees C 151-IgG was
directly competitive for EGF binding to PC12 cells. It also inhibited EGF
binding to bovine corneal endothelial cells, rabbit corneal fibroblasts,
human foreskin fibroblasts, and normal rat kidney cells, and it slightly
enchanced EGF binding to SW 3T3 cells. PC12 cells have the same number of
binding sites for 151-IgG as for EGF (approximately 27,000 sites/cell).
151-IgG inhibited the photoactivatable cross-linking of EGF to a protein of
Mr 170,000 in PC12 cells. 151-IgG inhibited the EGF-stimulated
incorporation of [3H]thymidine into quiescent bovine corneal endothelial
cells, rabbit corneal endothelial cells, epithelial normal rat kidney
cells, and SW 3T3 cells while it enhanced the EGF-stimulated [3H]thymidine
incorporation into quiescent human foreskin fibroblasts. 151-IgG by itself
possessed intrinsic EGF-like activity for human fibroblasts but not for the
other cells tested. This suggests that there is a difference in EGF
receptors and/or processing in these normal cell types.
A monoclonal antibody which inhibits epidermal growth factor binding has opposite effects on the biological action of epidermal growth factor in different cells
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