Type β Transforming Growth Factor: A Bifunctional Regulator of Cellular Growth

Type β transforming growth factor (TGF-β ) is a two-chain polypeptide of 25,000 daltons isolated from many tissues, including bovine kidney, human placenta, and human platelets. It has been characterized by its ability to stimulate reversible transformation of nonneoplastic murine fibroblasts, as me...

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Published inProceedings of the National Academy of Sciences - PNAS Vol. 82; no. 1; pp. 119 - 123
Main Authors Roberts, Anita B., Anzano, Mario A., Wakefield, Lalage M., Roche, Nanette S., Stern, David F., Sporn, Michael B.
Format Journal Article
LanguageEnglish
Published Washington, DC National Academy of Sciences of the United States of America 01.01.1985
National Acad Sciences
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Abstract Type β transforming growth factor (TGF-β ) is a two-chain polypeptide of 25,000 daltons isolated from many tissues, including bovine kidney, human placenta, and human platelets. It has been characterized by its ability to stimulate reversible transformation of nonneoplastic murine fibroblasts, as measured by the formation of colonies of these cells in soft agar (ED50= 4 pM TGF-β for NRK fibroblasts). We now show that the response of cells to TGF-β is bifunctional, in that TGF-β inhibits the anchorage-dependent growth of NRK fibroblasts and of human tumor cells by increasing cell cycle time. Moreover, the anchorage-independent growth of many human melanoma, lung carcinoma, and breast carcinoma cell lines is inhibited by TGF-β at concentrations in the same range as those that stimulate colony formation of NRK fibroblasts (average ED50= 10-30 pM TGF-β for inhibition). Whereas epidermal growth factor and TGF-β synergize to induce anchorage-independent growth of NRK fibroblasts, their effects on the growth of A-549 human lung carcinoma cells are antagonistic. The bifunctional response of cells to TGF-β is further demonstrated in Fischer rat 3T3 fibroblasts transfected with a cellular myc gene. In these cells TGF-β synergizes with platelet-derived growth factor to stimulate colony formation but inhibits the colony formation induced by epidermal growth factor. The data indicate that the effects of TGF-β on cells are not a function of the peptide itself, but rather of the total set of growth factors and their receptors that is operant in the cell at a given time.
AbstractList Type beta transforming growth factor (TGF-beta) is a two-chain polypeptide of 25,000 daltons isolated from many tissues, including bovine kidney, human placenta, and human platelets. It has been characterized by its ability to stimulate reversible transformation of nonneoplastic murine fibroblasts, as measured by the formation of colonies of these cells in soft agar (ED50 = 4 pM TGF-beta for NRK fibroblasts). We now show that the response of cells to TGF-beta is bifunctional, in that TGF-beta inhibits the anchorage-dependent growth of NRK fibroblasts and of human tumor cells by increasing cell cycle time. Moreover, the anchorage-independent growth of many human melanoma, lung carcinoma, and breast carcinoma cell lines is inhibited by TGF-beta at concentrations in the same range as those that stimulate colony formation of NRK fibroblasts (average ED50 = 10-30 pM TGF-beta for inhibition). Whereas epidermal growth factor and TGF-beta synergize to induce anchorage-independent growth of NRK fibroblasts, their effects on the growth of A-549 human lung carcinoma cells are antagonistic. The bifunctional response of cells to TGF-beta is further demonstrated in Fischer rat 3T3 fibroblasts transfected with a cellular myc gene. In these cells TGF-beta synergizes with platelet-derived growth factor to stimulate colony formation but inhibits the colony formation induced by epidermal growth factor. The data indicate that the effects of TGF-beta on cells are not a function of the peptide itself, but rather of the total set of growth factors and their receptors that is operant in the cell at a given time.
Type β transforming growth factor (TGF-β ) is a two-chain polypeptide of 25,000 daltons isolated from many tissues, including bovine kidney, human placenta, and human platelets. It has been characterized by its ability to stimulate reversible transformation of nonneoplastic murine fibroblasts, as measured by the formation of colonies of these cells in soft agar (ED50= 4 pM TGF-β for NRK fibroblasts). We now show that the response of cells to TGF-β is bifunctional, in that TGF-β inhibits the anchorage-dependent growth of NRK fibroblasts and of human tumor cells by increasing cell cycle time. Moreover, the anchorage-independent growth of many human melanoma, lung carcinoma, and breast carcinoma cell lines is inhibited by TGF-β at concentrations in the same range as those that stimulate colony formation of NRK fibroblasts (average ED50= 10-30 pM TGF-β for inhibition). Whereas epidermal growth factor and TGF-β synergize to induce anchorage-independent growth of NRK fibroblasts, their effects on the growth of A-549 human lung carcinoma cells are antagonistic. The bifunctional response of cells to TGF-β is further demonstrated in Fischer rat 3T3 fibroblasts transfected with a cellular myc gene. In these cells TGF-β synergizes with platelet-derived growth factor to stimulate colony formation but inhibits the colony formation induced by epidermal growth factor. The data indicate that the effects of TGF-β on cells are not a function of the peptide itself, but rather of the total set of growth factors and their receptors that is operant in the cell at a given time.
Author Wakefield, Lalage M.
Roche, Nanette S.
Anzano, Mario A.
Sporn, Michael B.
Roberts, Anita B.
Stern, David F.
Author_xml – sequence: 1
  givenname: Anita B.
  surname: Roberts
  fullname: Roberts, Anita B.
– sequence: 2
  givenname: Mario A.
  surname: Anzano
  fullname: Anzano, Mario A.
– sequence: 3
  givenname: Lalage M.
  surname: Wakefield
  fullname: Wakefield, Lalage M.
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  givenname: Nanette S.
  surname: Roche
  fullname: Roche, Nanette S.
– sequence: 5
  givenname: David F.
  surname: Stern
  fullname: Stern, David F.
– sequence: 6
  givenname: Michael B.
  surname: Sporn
  fullname: Sporn, Michael B.
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https://www.ncbi.nlm.nih.gov/pubmed/3871521$$D View this record in MEDLINE/PubMed
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Mammalia
Animal
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Snippet Type β transforming growth factor (TGF-β ) is a two-chain polypeptide of 25,000 daltons isolated from many tissues, including bovine kidney, human placenta,...
Type beta transforming growth factor (TGF-beta) is a two-chain polypeptide of 25,000 daltons isolated from many tissues, including bovine kidney, human...
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pnas
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StartPage 119
SubjectTerms Animals
Biological and medical sciences
Cell Adhesion
Cell Cycle - drug effects
Cell growth
Cell Line
Cell lines
Cell physiology
Cell Transformation, Viral
Cells, Cultured
Cultured cells
Drug Interactions
Epidermal Growth Factor - pharmacology
Epithelial cells
Fibroblasts
Fibroblasts - cytology
Fundamental and applied biological sciences. Psychology
Growth Inhibitors - pharmacology
Growth Substances - pharmacology
Human growth
Kidney cells
Lungs
Melanoma
Molecular and cellular biology
Oncogenes
Peptides - pharmacology
Rats
Responses to growth factors, tumor promotors, other factors
Transforming Growth Factors
Tumor cell line
Title Type β Transforming Growth Factor: A Bifunctional Regulator of Cellular Growth
URI https://www.jstor.org/stable/24501
http://www.pnas.org/content/82/1/119.abstract
https://www.ncbi.nlm.nih.gov/pubmed/3871521
https://pubmed.ncbi.nlm.nih.gov/PMC396983
Volume 82
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