Crissey Mary Ann S, Guo Rong-Jun, Fogt Franz, Li Hong, Katz Jonathan P, Silberg Debra G, Suh Eun Ran, Lynch John P
Division of Gastroenterology, Department of Medicine, University of Pennsylvania, 600 Clinical Research Building, 415 Curie Blvd., Philadelphia, PA 19104 USA.
Neoplasia. 2008 Jan;10(1):8-19. doi: 10.1593/neo.07703.
The Caudal-related homeobox genes Cdx1 and Cdx2 are intestine-specific transcription factors that regulate differentiation of intestinal cell types. Previously, we have shown Cdx1 to be antiproliferative and to promote cell differentiation. However, other studies have suggested that Cdx1 may be an oncogene. To test for oncogenic behavior, we used the murine villin promoter to ectopically express Cdx1 in the small intestinal villi and colonic surface epithelium. No changes in intestinal architecture, cell differentiation, or lineage selection were observed with expression of the transgene. Classic oncogenes enhance proliferation and induce tumors when ectopically expressed. However, the Cdx1 transgene neither altered intestinal proliferation nor induced spontaneous intestinal tumors. In a murine model for colitis-associated cancer, the Cdx1 transgene decreased, rather than increased, the number of adenomas that developed. In the polyps, the expression of the endogenous and the transgenic Cdx1 proteins was largely absent, whereas endogenous Villin expression was retained. This suggests that transgene silencing was specific and not due to a general Villin inactivation. In conclusion, neither the ectopic expression of Cdx1 was associated with changes in intestinal cell proliferation or differentiation nor was there increased intestinal cancer susceptibility. Our results therefore suggest that Cdx1 is not an oncogene in normal intestinal epithelium.
尾相关同源框基因Cdx1和Cdx2是肠道特异性转录因子,可调节肠道细胞类型的分化。此前,我们已表明Cdx1具有抗增殖作用并促进细胞分化。然而,其他研究表明Cdx1可能是一种癌基因。为了测试其致癌行为,我们使用小鼠绒毛蛋白启动子在小肠绒毛和结肠表面上皮中异位表达Cdx1。转基因表达后,未观察到肠道结构、细胞分化或谱系选择的变化。经典癌基因在异位表达时会增强增殖并诱导肿瘤。然而,Cdx1转基因既未改变肠道增殖,也未诱导自发性肠道肿瘤。在结肠炎相关癌症的小鼠模型中,Cdx1转基因减少而非增加了发生的腺瘤数量。在息肉中,内源性和转基因Cdx1蛋白的表达基本缺失,而内源性绒毛蛋白表达得以保留。这表明转基因沉默是特异性的,并非由于绒毛蛋白普遍失活所致。总之,Cdx1的异位表达既与肠道细胞增殖或分化的变化无关,也未增加肠道癌症易感性。因此,我们的结果表明Cdx1在正常肠道上皮中不是癌基因。