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Efficient immortalization of luminal epithelial cells from human mammary gland by introduction of simian virus 40 large tumor antigen with a recombinant retrovirus
J Bartek, J Bartkova, N Kyprianou, EN Lalani, Z Staskova, M Shearer, S Chang, J Taylor-Papadimitriou
Language English Country United States
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Digital library NLK
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Free Medical Journals
from 1915 to 6 months ago
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from 1915 to 6 months ago
PubMed Central
from 1915 to 6 months ago
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from 1915 to 6 months ago
Open Access Digital Library
from 1915-01-01
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from 1915-01-15
PubMed
1708884
Knihovny.cz E-resources
- MeSH
- Antigens, Polyomavirus Transforming * genetics MeSH
- Cell Division MeSH
- Cell Line MeSH
- DNA, Viral genetics MeSH
- Epithelial Cells MeSH
- Fluorescent Antibody Technique MeSH
- Genetic Vectors MeSH
- Keratins metabolism MeSH
- Humans MeSH
- Milk, Human * cytology MeSH
- Mice, Nude MeSH
- Mice MeSH
- Oncogene Protein p21(ras) genetics MeSH
- Simian virus 40 genetics MeSH
- Breast * cytology MeSH
- Retroviridae genetics MeSH
- Blotting, Southern MeSH
- In Vitro Techniques MeSH
- Cell Transformation, Viral * MeSH
- Animals MeSH
- Check Tag
- Humans MeSH
- Mice MeSH
- Animals MeSH
When defined in terms of markers for normal cell lineages, most invasive breast cancer cells correspond to the phenotype of the common luminal epithelial cell found in the terminal ductal lobular units. Luminal epithelial cells cultured from milk, which have limited proliferative potential, have now been immortalized by introducing the gene encoding simian virus 40 large tumor (T) antigen. Infection with a recombinant retrovirus proved to be 50-100 times more efficient than calcium phosphate transfection, and of the 17 cell lines isolated, only 5 passed through a crisis period as characterized by cessation of growth. When characterized by immunohistochemical staining with monoclonal antibodies, 14 lines showed features of luminal epithelial cells and of these, 7 resembled the common luminal epithelial cell type in the profile of keratins expressed. These cells express keratins 7, 8, 18, and 19 homogeneously and do not express keratin 14 or vimentin; a polymorphic epithelial mucin produced in vivo by luminal cells is expressed heterogeneously and the pattern of fibronectin staining is punctate. Although the cell lines have a reduced requirement for added growth factors, they do not grow in agar or produce tumors in the nude mouse. When the v-Ha-ras oncogene was introduced into two of the cell lines by using a recombinant retrovirus, most of the selected clones senesced, but one entered crisis and emerged after 3 months as a tumorigenic cell line.
Department of Dental Sciences Royal College of Surgeons London United Kingdom
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- $a Efficient immortalization of luminal epithelial cells from human mammary gland by introduction of simian virus 40 large tumor antigen with a recombinant retrovirus / $c J Bartek, J Bartkova, N Kyprianou, EN Lalani, Z Staskova, M Shearer, S Chang, J Taylor-Papadimitriou
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- $a When defined in terms of markers for normal cell lineages, most invasive breast cancer cells correspond to the phenotype of the common luminal epithelial cell found in the terminal ductal lobular units. Luminal epithelial cells cultured from milk, which have limited proliferative potential, have now been immortalized by introducing the gene encoding simian virus 40 large tumor (T) antigen. Infection with a recombinant retrovirus proved to be 50-100 times more efficient than calcium phosphate transfection, and of the 17 cell lines isolated, only 5 passed through a crisis period as characterized by cessation of growth. When characterized by immunohistochemical staining with monoclonal antibodies, 14 lines showed features of luminal epithelial cells and of these, 7 resembled the common luminal epithelial cell type in the profile of keratins expressed. These cells express keratins 7, 8, 18, and 19 homogeneously and do not express keratin 14 or vimentin; a polymorphic epithelial mucin produced in vivo by luminal cells is expressed heterogeneously and the pattern of fibronectin staining is punctate. Although the cell lines have a reduced requirement for added growth factors, they do not grow in agar or produce tumors in the nude mouse. When the v-Ha-ras oncogene was introduced into two of the cell lines by using a recombinant retrovirus, most of the selected clones senesced, but one entered crisis and emerged after 3 months as a tumorigenic cell line.
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