Abstract:
:The effects of a ligand regulated neu tyrosine kinase were examined in NIH 3T3 cells. A chimeric construct encoding the human EGF receptor extracellular domain fused to the tyrosine kinase domain of the rat neu cDNA was expressed under the transcriptional control of the Moloney murine leukemia virus LTR promoter. This resulted in higher levels of expression of the chimeric receptor than were previously obtained from the SV40 virus early promoter in the same cells. The chimeric receptor showed strict ligand-dependent tyrosine kinase and signal transducing activities for the induction of growth-regulated biochemical activities and DNA synthesis in resting cells. The ligand-activated cells became morphologically transformed and grew in agar in the presence of EGF and TGF beta as efficiently as did the ligand-independent neu oncogene-transformed cells. Our results establish similarities between the signal pathways of the EGF receptor and the neu tyrosine kinase.
journal_name
J Cell Biochemjournal_title
Journal of cellular biochemistryauthors
Lehväslaiho H,Sistonen L,diRenzo F,Partanen J,Comoglio P,Hölttä E,Alitalo Kdoi
10.1002/jcb.240420303subject
Has Abstractpub_date
1990-03-01 00:00:00pages
123-33issue
3eissn
0730-2312issn
1097-4644journal_volume
42pub_type
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