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Epidermal growth factor ligand-independent, unregulated, cell-transforming potential of a naturally occurring human mutant EGFRvIII gene.

Publication ,  Journal Article
Batra, SK; Castelino-Prabhu, S; Wikstrand, CJ; Zhu, X; Humphrey, PA; Friedman, HS; Bigner, DD
Published in: Cell Growth Differ
October 1995

The type III deletion-mutant gene for the epidermal growth factor receptor (EGFRvIII) is frequently expressed in glioblastomas and in breast and non-small cell lung carcinomas. To understand its contribution to the malignant phenotype in humans, we transfected NR6 cells with the mammalian vector pH beta APr-1-neo containing cDNA for either EGFRvIII or wild-type EGFR. Western blot analyses showed that NR6 transfected with wild-type EGFR (NR6W) contained a normal-sized protein (170 kilodaltons); cells transfected with EGFRvIII (NR6M) contained a truncated protein (145 kilodaltons). NR6W cells demonstrated a saturation binding curve with 125I-labeled EGF (affinity, 1.8 x 10(8); r2 = 0.96). NR6M cells, however, showed a low but consistent level of 125I-labeled EGF binding (affinity, 4 x 10(7); r2 = 0.99) compared with NR6, which lacked binding. The population doubling time was shorter for NR6M (0.64 days) than for NR6W (1.1 days) and NR6V (2.27 days). Soft agar focus formation assay by NR6M was 4- to 5-fold higher than that by NR6W. In nude mice, NR6M (1 x 10(7) cells), without exogenous ligand, formed tumors within 12 days; no tumors were observed over 90 days in mice receiving identical doses of NR6W, NR6V, or NR6 cells. EGF stimulated autophosphorylation of receptor in NR6W (4- to 9-fold) but caused only slight (1.8- to 1.9-fold) to no enhancement in NR6M. Further, there was no difference in constitutive tyrosine kinase activity between NR6M and NR6W. Our results clearly indicate that EGFRvIII functions as an oncoprotein, but its intrinsic tyrosine kinase activity may not be responsible for its biological function.

Duke Scholars

Published In

Cell Growth Differ

ISSN

1044-9523

Publication Date

October 1995

Volume

6

Issue

10

Start / End Page

1251 / 1259

Location

United States

Related Subject Headings

  • Transfection
  • Sequence Deletion
  • RNA, Messenger
  • Protein-Tyrosine Kinases
  • Phosphorylation
  • Oncology & Carcinogenesis
  • Oncogene Proteins
  • Mice, Nude
  • Mice
  • Kinetics
 

Citation

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MLA
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Batra, S. K., Castelino-Prabhu, S., Wikstrand, C. J., Zhu, X., Humphrey, P. A., Friedman, H. S., & Bigner, D. D. (1995). Epidermal growth factor ligand-independent, unregulated, cell-transforming potential of a naturally occurring human mutant EGFRvIII gene. Cell Growth Differ, 6(10), 1251–1259.
Batra, S. K., S. Castelino-Prabhu, C. J. Wikstrand, X. Zhu, P. A. Humphrey, H. S. Friedman, and D. D. Bigner. “Epidermal growth factor ligand-independent, unregulated, cell-transforming potential of a naturally occurring human mutant EGFRvIII gene.Cell Growth Differ 6, no. 10 (October 1995): 1251–59.
Batra SK, Castelino-Prabhu S, Wikstrand CJ, Zhu X, Humphrey PA, Friedman HS, et al. Epidermal growth factor ligand-independent, unregulated, cell-transforming potential of a naturally occurring human mutant EGFRvIII gene. Cell Growth Differ. 1995 Oct;6(10):1251–9.
Batra SK, Castelino-Prabhu S, Wikstrand CJ, Zhu X, Humphrey PA, Friedman HS, Bigner DD. Epidermal growth factor ligand-independent, unregulated, cell-transforming potential of a naturally occurring human mutant EGFRvIII gene. Cell Growth Differ. 1995 Oct;6(10):1251–1259.

Published In

Cell Growth Differ

ISSN

1044-9523

Publication Date

October 1995

Volume

6

Issue

10

Start / End Page

1251 / 1259

Location

United States

Related Subject Headings

  • Transfection
  • Sequence Deletion
  • RNA, Messenger
  • Protein-Tyrosine Kinases
  • Phosphorylation
  • Oncology & Carcinogenesis
  • Oncogene Proteins
  • Mice, Nude
  • Mice
  • Kinetics