CELL-CYCLE VARIATION IN I-125-LABELED EPIDERMAL GROWTH-FACTOR BINDING IN CHEMICALLY TRANSFORMED-CELLS
- 1 January 1982
- journal article
- research article
- Vol. 42 (7), 2633-2638
Abstract
The nontransformed mouse fibroblast AKR-2B cells when arrested in G1 phase of the cell cycle due to low-MW nutrient (amino acid) deficiency exhibit a 5- to 10-fold lower level of epidermal growth factor (EGF) receptor activity than do the same cells in the rapidly growing state or arrested in G1 due to growth factor deficiency. The chemically transformed AKR-MCA and C3H/MCA-58 cell lines spontaneously arrest growth in G1 due to nutrient deficiency when grown to saturation density in medium with 10% fetal bovine serum. An examination of 125I-labeled EGF binding in rapidly growing and G1-arrested AKR-MCA and C3H/MCA-58 cells showed that the G1-arrested chemically transformed cells also have a 10- to 20-fold reduction in the amount of 125I-labeled EGF binding relative to the same cells in the rapidly growing state. Stimulation of DNA synthesis in the arrested cells by the addition of serum-free medium caused a 6- to 10-fold increase in 125I-labeled EGF binding. This recovery of receptor activity was inhibited by actinomycin D and cycloheximide, suggesting that new mRNA synthesis and increased protein synthesis is necessary for the recovery of EGF binding. A comparison of EGF binding in C3H/MCA-58 cells and the nontransformed parent line (C3H/10T1/2) in the rapidly growing state showed the same approximate level of receptor activity. However, the rapidly growing AKR-MCA cells had .apprx. 1/10 the amount of EGF binding as did the rapidly growing nontransformed parent line (AKR-2B). Scatchard analysis of binding data showed a 10-fold greater number of receptors in the AKR-2B cells relative to the AKR-MCA cells with a lesser difference in apparent receptor affinity. The chemically transformed BP-3T3, like the other 2 chemically transformed lines, was also demonstrated to arrest growth spontaneously due to nutrient deficiency with an associated 100-fold decrease in EGF binding. Rapidly growing BP-3T3 cells had only slightly less 125I-labeled EGF binding than did the nontransformed parent line (BALB-3T3) in the rapidly growing state. One mechanism for reduction of EGF binding in chemically transformed cells is the propensity of these cells to arrest growth in G1 at saturation density due to low MW nutrient deficiency, a state associated with decreased EGF binding.This publication has 19 references indexed in Scilit:
- Epidermal growth factor and the control of proliferation of Balb 3T3 and benzo[a]pyrene-transformed Balb 3T3 cellsJournal of Cellular Physiology, 1979
- Regulation of epidermal growth factor (EGF) receptor activity during the modulation of protein synthesisJournal of Cellular Physiology, 1979
- DIFFERENT RESPONSES TO DRUGS AND SERUM OF CELLS TRANSFORMED BY VARIOUS MEANS1979
- An ordered sequence of events is required before BALB/c-3T3 cells become committed to DNA synthesisProceedings of the National Academy of Sciences, 1978
- MECHANISM OF GROWTH ARREST OF CHEMICALLY TRANSFORMED-CELLS IN CULTURE1978
- Gene expression in chemically transformed mouse embryo cells: Selective enhancement of the expression of C type RNA tumor virus genesCell, 1977
- Nuclear RNA polymerase activities and poly(A)-containing mRNA accumulation in cultured AKR mouse embryo cells stimulated to proliferateExperimental Cell Research, 1977
- In situ detection of mycoplasma contamination in cell cultures by fluorescent Hoechst 33258 stainExperimental Cell Research, 1977
- Transformation by murine and feline sarcoma viruses specifically blocks binding of epidermal growth factor to cellsNature, 1976
- A study of the conditions and mechanism of the diphenylamine reaction for the colorimetric estimation of deoxyribonucleic acidBiochemical Journal, 1956