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Karyotype evolution in a simian virus 40-transformed tumorigenic human cell line.

作者信息

Goolsby C L, Wiley J E, Steiner M, Bartholdi M F, Cram L S, Kraemer P M

机构信息

Department of Pathology, Northwestern University Medical School/VA Lakeside Medical Center, Chicago, Illinois 60611.

出版信息

Cancer Genet Cytogenet. 1990 Dec;50(2):231-48. doi: 10.1016/0165-4608(90)90183-b.

DOI:10.1016/0165-4608(90)90183-b
PMID:2176127
Abstract

Normal human foreskin fibroblasts (HSF4) were transfected using the pSV3-neo plasmid. A pool of 10 G418-resistant colonies, HSF4-T12, showed a progressive increase in the expression of a number of in vitro transformation markers with passage in culture and became immortalized. Although no tumors were formed when cells were injected subcutaneously into nude mice, this cell line produced progressive tumors when cells were injected into preimplanted Gelfoam sponges in the mice. When these tumors were cultured in vitro and subsequently injected subcutaneously, progressive tumors were produced with median latency periods as short as 4 weeks. Three phases of cytogenetic change could be distinguished. At early passages after transfection. HSF4-T12 exhibited many random chromosomal changes. At a time just after immortalization, both flow karyotype and G-banded analyses showed the appearance of balanced clonal rearrangements. These included t(2;4), t(2;14), t(3;?), 6p-, i(6p), 8p-, t(14;15), i(15), and t(18;?). These clonal rearrangements were stable with passage in culture, and less variability from cell to cell was noted. The only consistent chromosomal loss observed was -Y. Analysis of three independent tumors showed characteristic loss of chromosomal material rather than balanced chromosomal rearrangements. Frequent loss of 6q and chromosomes #13, 15, 20, and Y was noted.

摘要

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