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Literature DB >> 2813423

Role of a tumor-suppressor gene in the negative control of anchorage-independent growth of Syrian hamster cells.

M Koi¹, C A Afshari, L A Annab, J C Barrett.

Abstract

Tumor-suppressor genes control the neoplastic phenotype of tumor cells, but the function of these genes in normal cells is unknown. In this report we show that the loss of a tumor-suppressor gene function releases negative controls on the growth of cells in agar. This conclusion is based on observations of cell hybrids and studies of cell variants that have retained or lost a tumor-suppressor gene function. Nontumorigenic cell hybrids between normal Syrian hamster embryo cells and a benzo[a]pyrene-transformed tumor-cell line (BP6T) continued to secrete autocrine and/or paracrine growth factors produced by the tumor cells but failed to respond to these factors by growing in agar. Normal diploid cells also failed to grow in agar in response to the growth factors produced by the tumor cells. Clonal variants of nontumorigenic, immortal Syrian hamster cell lines were isolated that either retained (termed supB+) or had lost (termed supB-) the ability to suppress tumorigenicity of BP6T tumor cells after cell hybridization. Neither supB+ nor supB- variants grew in agar under conditions that allowed efficient growth of the tumor cells. However, supB- cells were reversibly induced to grow in agar with high colony-forming efficiencies in the presence of tumor cell-conditioned medium or by supplementation of the medium with a combination of growth factors. Under the same conditions, the supB+ cells failed to grow in agar. This enhanced growth-factor responsiveness in agar was used to select for supB- variants existing at a low frequency in the supB+ population. These two phenotypes, loss of tumor-suppressor function and enhanced growth-factor responsiveness in agar, were seen to cosegregate. These results indicate the tumor-suppressor gene function in these cells negatively regulates the growth response of cells in agar to mitogenic stimuli. This growth regulation may depend on cell shape or adhesion because supB+ and supB- cells grown attached to plastic responded similarly to growth factors.

Entities: Chemical Disease Species

Mesh：

Substances：
Growth Substances

Year: 1989 PMID： 2813423 PMCID： PMC298372 DOI： 10.1073/pnas.86.22.8773

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

44 in total

1. Members of the src and ras oncogene families supplant the epidermal growth factor requirement of BALB/MK-2 keratinocytes and induce distinct alterations in their terminal differentiation program.

Authors: B Weissman; S A Aaronson
Journal: Mol Cell Biol Date: 1985-12 Impact factor: 4.272

Review 2. Growth factors and cancer.

Authors: A S Goustin; E B Leof; G D Shipley; H L Moses
Journal: Cancer Res Date: 1986-03 Impact factor: 12.701

Review 3. Early signals in the mitogenic response.

Authors: E Rozengurt
Journal: Science Date: 1986-10-10 Impact factor: 47.728

4. Loss of tumor-suppressive function during chemically induced neoplastic progression of Syrian hamster embryo cells.

Authors: M Koi; J C Barrett
Journal: Proc Natl Acad Sci U S A Date: 1986-08 Impact factor: 11.205

5. Potentiation of growth factor activity by exogenous c-myc expression.

Authors: V Sorrentino; V Drozdoff; M D McKinney; L Zeitz; E Fleissner
Journal: Proc Natl Acad Sci U S A Date: 1986-11 Impact factor: 11.205

6. Differential responsiveness of myc- and ras-transfected cells to growth factors: selective stimulation of myc-transfected cells by epidermal growth factor.

Authors: D F Stern; A B Roberts; N S Roche; M B Sporn; R A Weinberg
Journal: Mol Cell Biol Date: 1986-03 Impact factor: 4.272

7. Suppression of tumorigenicity with continued expression of the c-Ha-ras oncogene in EJ bladder carcinoma-human fibroblast hybrid cells.

Authors: A G Geiser; C J Der; C J Marshall; E J Stanbridge
Journal: Proc Natl Acad Sci U S A Date: 1986-07 Impact factor: 11.205

Review 8. Genetic suppression of tumor formation: a new frontier in cancer research.

Authors: R Sager
Journal: Cancer Res Date: 1986-04 Impact factor: 12.701

9. Human retinoblastoma susceptibility gene: cloning, identification, and sequence.

Authors: W H Lee; R Bookstein; F Hong; L J Young; J Y Shew; E Y Lee
Journal: Science Date: 1987-03-13 Impact factor: 47.728

10. A human DNA segment with properties of the gene that predisposes to retinoblastoma and osteosarcoma.

Authors: S H Friend; R Bernards; S Rogelj; R A Weinberg; J M Rapaport; D M Albert; T P Dryja
Journal: Nature Date: 1986 Oct 16-22 Impact factor: 49.962

7 in total

1. Imatinib mesylate inhibits proliferation of rheumatoid synovial fibroblast-like cells and phosphorylation of Gab adapter proteins activated by platelet-derived growth factor.

Authors: H Kameda; H Ishigami; M Suzuki; T Abe; T Takeuchi
Journal: Clin Exp Immunol Date: 2006-05 Impact factor: 4.330

Role of a tumor-suppressor gene in the negative control of anchorage-independent growth of Syrian hamster cells.

1. Members of the src and ras oncogene families supplant the epidermal growth factor requirement of BALB/MK-2 keratinocytes and induce distinct alterations in their terminal differentiation program.

Review 2. Growth factors and cancer.

Review 3. Early signals in the mitogenic response.

4. Loss of tumor-suppressive function during chemically induced neoplastic progression of Syrian hamster embryo cells.

5. Potentiation of growth factor activity by exogenous c-myc expression.

6. Differential responsiveness of myc- and ras-transfected cells to growth factors: selective stimulation of myc-transfected cells by epidermal growth factor.

7. Suppression of tumorigenicity with continued expression of the c-Ha-ras oncogene in EJ bladder carcinoma-human fibroblast hybrid cells.

Review 8. Genetic suppression of tumor formation: a new frontier in cancer research.

9. Human retinoblastoma susceptibility gene: cloning, identification, and sequence.

10. A human DNA segment with properties of the gene that predisposes to retinoblastoma and osteosarcoma.

1. Imatinib mesylate inhibits proliferation of rheumatoid synovial fibroblast-like cells and phosphorylation of Gab adapter proteins activated by platelet-derived growth factor.

2. Expression of Gab1 lacking the pleckstrin homology domain is associated with neoplastic progression.

3. Induction of apoptosis by c-Fos protein.

4. Regulation of microfilament organization and anchorage-independent growth by tropomyosin 1.

5. Evidence for a potential tumor suppressor role for the Na,K-ATPase beta1-subunit.

6. Suppression of anchorage-independent growth after gene transfection.

Review 7. Identification of genes associated with tumor suppression in Syrian hamster embryo cells.