MODULATION OF EPIDERMAL GROWTH-FACTOR RECEPTOR-BINDING AND ACTION BY N-ACETYL-TGF-ALPHA(34-43) METHYL-ESTER

Controversial data have been reported concerning the ability of N-acet yl-TGF alpha(34-43) methyl ester (TGF alpha A) to antagonize the mitog enic effect or the receptor binding of TGF alpha and EGF. We reinvesti gated the effect of TGF alpha A on various EGF-sensitive cell lines an d in reaggregate and monolayer cell cultures of rat anterior pituitary . In reaggregate pituitary cell cultures, EGF dose-dependently increas ed [H-3]thymidine ([H-3]T) incorporation in lactotrophs and decreased [H-3]T incorporation in somatotrophs. TGF alpha A (5 mu M) completely blocked the effect of 0.1 nM EGF on both lactotrophs and somatotrophs. It had no intrinsic effect on its own. However, depending on the batc h of[I-125]EGF used, a dose of 5-10 mu M TGF alpha A did not or only p artially inhibited the binding of 3 X 10(-10) M [I-125]EGF to pituitar y monolayer cell cultures. In the EGF-sensitive cell lines A-43 1, BS- C-1, NRK-52E, and pituitary GH3 cells, none of the EGF effects were an tagonized by TGF alpha A. On the contrary, the EGF effect was slightly augmented in A-431 cells. In GH3 cells TGF alpha A was clearly mitoge nic on its own. It is concluded that, although TGF alpha A negatively interacts with EGF action and binding in normal pituitary, this is mos t likely not due to a direct competition with the binding of EGF.