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Proceedings of the National Academy of Sciences of the United States of America logoLink to Proceedings of the National Academy of Sciences of the United States of America
. 1980 Mar;77(3):1466–1470. doi: 10.1073/pnas.77.3.1466

Role of the degradation process in the mitogenic effect of epidermal growth factor

Naphtali Savion 1, Israel Vlodavsky 1, Denis Gospodarowicz 1
PMCID: PMC348516  PMID: 6966398

Abstract

The protease inhibitor leupeptin inhibits the degradation process of 125I-labeled epidermal growth factor (125I-EGF) by cultured bovine granulosa cells. At 80 μg/ml, leupeptin inhibited the appearance of degradation products of 125I-EGF in the medium by 95% during 1 hr of incubation and by 90% during 24 hr of incubation when the cells were exposed to 5 ng of 125I-EGF per ml. In contrast, cultures exposed to either saturating (10 ng/ml) or nonsaturating (0.1 ng/ml) concentrations of EGF in the presence of leupeptin (80 μg/ml) exhibited an increase in DNA synthesis that was 70-80% that of cultures exposed to EGF alone. Cultures responded to either EGF or fibroblast growth factor with a logarithmic increase in cell number and, over a period of 8 days, the number of cells increased 10- to 18-fold. Addition of leupeptin did not diminish the growth rate of the cultures. In the presence of leupeptin, 125I-EGF accumulated within the granulosa cells and was in a form that was precipitable with antiserum against EGF and that comigrated on isoelectric focusing with native 125I-EGF. That a full mitogenic response can be obtained despite a 90-95% inhibition of EGF degradation at either saturating or nonsaturating concentrations of the mitogen suggests that a proteolytic degradation of a given mitogen may not be involved in the induction of a proliferative response.

Keywords: mitogen degradation, leupeptin, granulosa cells, cell proliferation, DNA synthesis

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Selected References

These references are in PubMed. This may not be the complete list of references from this article.

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