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Reversion of uroepithelial cell tumorigenesis by the ectopic expression of human wnt-5a.

作者信息

Olson D J, Gibo D M, Saggers G, Debinski W, Kumar R

机构信息

Department of Surgery, College of Medicine, Milton S. Hershey Medical Center, Pennsylvania State University, Hershey 17033, USA.

出版信息

Cell Growth Differ. 1997 Apr;8(4):417-23.

PMID:9101087
Abstract

Wnt gene family members are thought to play an important role in cell growth and differentiation. When normal wnt gene expression is disrupted, there is the potential for cell transformation. We have found previously that a strong correlation exists between the loss of normal wnt-5a gene expression and cell transformation (Olson and Papkoff, Cell Growth & Differ., 5: 197-206, 1994). Recently, this has been tested directly using antisense wnt-5a, which, when expressed in mouse mammary cells, results in cell transformation (Olson and Gibo, Antisense wnt-5a transforms C57MG mouse mammary epithelial cells, manuscript in preparation). We hypothesize that wnt-5a is a growth-regulating gene, the disruption of which could result in tumorigenesis. The multistage progression of many human cancers involves the loss of normal tumor suppressor gene(s) activity. Several tumor suppressor genes are thought to map to chromosome 3p11-p25. We have studied the ectopic expression of human wnt-5a (3p14-p21) in a tumorigenic uroepithelial cell line with deletion of chromosome 3p13-p21.2. This results in loss of tumorigenicity in athymic nude mice and suppresses anchorage-independent cell growth in soft agar. This suggests that human wnt-5a is a novel tumor suppressor gene in uroepithelial cell carcinoma and may be one of the suppressor genes deleted or rearranged on chromosome 3p.

摘要

相似文献

1
Reversion of uroepithelial cell tumorigenesis by the ectopic expression of human wnt-5a.
Cell Growth Differ. 1997 Apr;8(4):417-23.
2
Antisense wnt-5a mimics wnt-1-mediated C57MG mammary epithelial cell transformation.反义Wnt-5a模拟Wnt-1介导的C57MG乳腺上皮细胞转化。
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3
Regulated expression of Wnt family members during proliferation of C57mg mammary cells.C57mg乳腺细胞增殖过程中Wnt家族成员的调控表达。
Cell Growth Differ. 1994 Feb;5(2):197-206.
4
Loss of 3p13----p21.2 in tumorigenic reversion of a hybrid between isogeneic nontumorigenic and tumorigenic human uroepithelial cells.在同基因非致瘤性和致瘤性人尿道上皮细胞杂交瘤的致瘤性逆转中3p13----p21.2的缺失
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Chromosome losses in tumorigenic revertants of EJ/ras-expressing somatic cell hybrids.表达EJ/ras的体细胞杂种致瘤性回复突变体中的染色体丢失
Cancer Genet Cytogenet. 1992 Apr;59(2):180-90. doi: 10.1016/0165-4608(92)90213-r.
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Molecular cloning of the human proto-oncogene Wnt-5A and mapping of the gene (WNT5A) to chromosome 3p14-p21.人类原癌基因Wnt-5A的分子克隆及该基因(WNT5A)在染色体3p14-p21上的定位。
Genomics. 1993 Nov;18(2):249-60. doi: 10.1006/geno.1993.1463.
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Ectopic expression of wnt-5a in human renal cell carcinoma cells suppresses in vitro growth and telomerase activity.Wnt-5a在人肾癌细胞中的异位表达抑制体外生长和端粒酶活性。
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Neoplastic progression by EJ/ras at different steps of transformation in vitro of human uroepithelial cells.EJ/ras在人尿道上皮细胞体外转化不同阶段的肿瘤进展。
Cancer Res. 1992 Feb 1;52(3):688-95.
10
Wnt-1 and int-2 mammary oncogene effects on the beta-catenin pathway in immortalized mouse mammary epithelial cells are not sufficient for tumorigenesis.Wnt-1和int-2乳腺癌基因对永生化小鼠乳腺上皮细胞中β-连环蛋白信号通路的影响不足以引发肿瘤形成。
Oncogene. 2001 Nov 15;20(52):7645-57. doi: 10.1038/sj.onc.1204980.

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