Cyclin D1 is necessary but not sufficient for anchorage-independent growth of rat mammary tumor cells and is associated with resistance of the Copenhagen rat to mammary carcinogenesis
To identify genes associated with the resistance of Copenhagen (Cop) rats to mammary carcinogenesis, we infused a retrovirus harboring v-Ha-ras directly into the main mammary ducts of resistant F1 rats from a cross between Cop and susceptible Wistar Furth (WIT) rats. Adenocarcinomas formed in approximately 50% of infused glands. Cell lines derived from these tumors were clonal, but did not share a common viral integration site, suggesting that a high level of v-Ha-ras expression was able to overcome resistance in the F1 rats. Some of the cell lines were able to grow in soft agar, but a significant number did not display anchorage-independent growth. These growth characteristics were independent of v-Ha-ras expression levels. The ability to grow in soft agar was associated with the size of tumors induced by injecting the cells into nude mice, and showed a striking positive association with the expression of cyclin D1. Furthermore, while resistance to anchorage-independent growth was fully overcome by transfection of cyclin D1 in some clones, in the others the effect was partial. A similar pattern of cyclin D1 upregulation and growth in soft agar was also observed when the cells were transfected with an active form of beta-catenin. Hybrid cells from the somatic fusion of an anchorage-dependent to an anchorage-independent clone did not grow in soft agar. These results suggest that while a high expression level of cyclin D1 is necessary for anchorage-independent growth in all clones, it is not sufficient for full growth capacity in soft agar, raising the possibility that the loss of a tumor suppressor gene in the cell lines is required to fully confer anchorage-independent growth. Our anchorage-dependent and independent rat mammary tumor-derived cell lines may recapitulate the resistance and susceptibility of Cop and WF rats, respectively, to mammary carcinogenesis that could facilitate the identification of breast cancer susceptibility genes.
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Department of Nutritional Sciences, Faculty of Medicine, 150 College St, TorontoDepartment of Nutritional Sciences, Faculty of Medicine, 150 College St, Toronto
Korkola J.E.
Wood G.A.
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Department of Nutritional Sciences, Faculty of Medicine, 150 College St, TorontoDepartment of Nutritional Sciences, Faculty of Medicine, 150 College St, Toronto
Wood G.A.
Archer M.C.
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Department of Nutritional Sciences, Faculty of Medicine, 150 College St, TorontoDepartment of Nutritional Sciences, Faculty of Medicine, 150 College St, Toronto
机构:
NYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USA
Fourth Mil Med Univ, Sch Publ Hlth, Dept Occupat & Environm Hlth, Xian 710032, Shannxi, Peoples R ChinaNYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USA
Cao, Zipeng
Li, Xueyong
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NYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USANYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USA
Li, Xueyong
Li, Jingxia
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NYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USANYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USA
Li, Jingxia
Kang, Beipei
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Fourth Mil Med Univ, Sch Publ Hlth, Dept Occupat & Environm Hlth, Xian 710032, Shannxi, Peoples R ChinaNYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USA
Kang, Beipei
Chen, Jingyuan
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Fourth Mil Med Univ, Sch Publ Hlth, Dept Occupat & Environm Hlth, Xian 710032, Shannxi, Peoples R ChinaNYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USA
Chen, Jingyuan
Luo, Wenjing
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Fourth Mil Med Univ, Sch Publ Hlth, Dept Occupat & Environm Hlth, Xian 710032, Shannxi, Peoples R ChinaNYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USA
Luo, Wenjing
Huang, Chuanshu
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NYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USANYU, Nelson Inst Environm Med, Sch Med, Tuxedo Pk, NY 10987 USA
机构:
Laboratory of Cancer Genomics, Hollings Cancer Center, Medical University of South Carolina, CharlestonLaboratory of Cancer Genomics, Hollings Cancer Center, Medical University of South Carolina, Charleston
Bowe D.B.
Kenney N.J.
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Department of Biological Sciences, Hampton University, HamptonLaboratory of Cancer Genomics, Hollings Cancer Center, Medical University of South Carolina, Charleston
Kenney N.J.
Adereth Y.
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Laboratory of Cancer Genomics, Hollings Cancer Center, Medical University of South Carolina, CharlestonLaboratory of Cancer Genomics, Hollings Cancer Center, Medical University of South Carolina, Charleston
Adereth Y.
Maroulakou I.G.
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Laboratory of Cancer Genomics, Hollings Cancer Center, Medical University of South Carolina, Charleston
Department of Medicine, Hollings Cancer Center, Medical University of South Carolina, CharlestonLaboratory of Cancer Genomics, Hollings Cancer Center, Medical University of South Carolina, Charleston