Abstract

Heterogeneity of cells in tumors appears to be a major obstacle in the successful treatment of cancer. It is also of importance in understanding the progression of cells to autonomous growth including metastasis. The highest estimates of the rate of variation responsible for heterogeneity have been on the order of one heritable alteration per 10?5? cell divisions. In the past year we were able to isolate five clones among the progeny of a Balb/3T3 cell which had just undergone spontaneous transformation and to characterize their properties. We found that each of the clones could be distinguished from the others by morphology, colony-forming efficiency in agar (CFEag), and rate of tumor formation in nude mice. The implication of this finding is that cultured cells are so unstable soon after transformation that essentially every cell may differ from the others in one or more characteristics, i.e., that there is a truly radical heterogeneity. We have also studied the evolution of further changes in these properties among the five clonal populations over a 6-month period and conclude that the type of variation which led to the initial differences among the clones could also be responsible for continuing change akin to tumor progression. Since the frequency of this type of variation is very high and involves several properties in a quantitative but uncoordinated way, it is unlikely to be caused by conventional genetic mutations. Rather, it is likely to be an epigenetic event. This type of variation is also likely to play a role in our second major finding, which is that some properties of transformed cells are altered during tumor formation in the nude mouse and again when the tumor cells are cultured. The former contradicts the generally accepted view that cells are not changed by passage through nude mice. We find our example, that a decrease in CFEag of more than 100-fold, is frequently observed during tumor formation. Cells from some tumors regain their original high CFEag after repeated passaging in culture but others do not. That is, there is a heterogeneity of response, some changes being stable and others unstable. The evidence to date indicates the alterations in cells during tumor formation and subsequent cultivation are basically epigenetic in nature and similar in type to those described above which occur after transformation. The results promise to provide new ground for understanding the origin and progression of cancer. (J)

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
3R01CA015744-11S1
Application #
3164257
Study Section
Cognition and Perception Study Section (CP)
Project Start
1979-08-01
Project End
1986-12-31
Budget Start
1985-05-01
Budget End
1986-12-31
Support Year
11
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of California Berkeley
Department
Type
Schools of Arts and Sciences
DUNS #
094878337
City
Berkeley
State
CA
Country
United States
Zip Code
94704

  Publications

Vidair, Charles; Rubin, Harry (2005) Mg2+ as activator of uridine phosphorylation in coordination with other cellular responses to growth factors. Proc Natl Acad Sci U S A 102:662-6
Rubin, A L; Sneade-Koenig, A; Rubin, H (1992) High rate of diversification and reversal among subclones of neoplastically transformed NIH 3T3 clones. Proc Natl Acad Sci U S A 89:4183-6
Ellison, B J; Rubin, H (1992) Individual transforming events in long-term cell culture of NIH 3T3 cells as products of epigenetic induction. Cancer Res 52:667-73
Yao, A; Rubin, H (1992) Sensitivity of transformation to small differences in population density during serial passage of NIH 3T3 cells. Proc Natl Acad Sci U S A 89:7486-90
Grundel, R; Rubin, H (1992) Adaptation and selection as factors in the spontaneous transformation of NIH-3T3 cells. Carcinogenesis 13:1873-7
Yao, A; Huang, W; Rubin, H (1991) Growth in high serum concentrations leads to rapid deadaptation of cells previously adapted to growth in an extremely low concentration of serum. Proc Natl Acad Sci U S A 88:9422-5
Rubin, H; Xu, K (1991) Epigenetic features of spontaneous transformation in the NIH 3T3 line of mouse cells. Basic Life Sci 57:301-12;discussion 312-3
Grundel, R; Rubin, H (1991) Effect of interclonal heterogeneity on the progressive, confluence-mediated acquisition of the focus-forming phenotype in NIH-3T3 populations. Cancer Res 51:1003-13
Farber, E; Rubin, H (1991) Cellular adaptation in the origin and development of cancer. Cancer Res 51:2751-61
Rubin, H (1990) On the nature of enduring modifications induced in cells and organisms. Am J Physiol 258:L19-24

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