Zhao Y L, Piao C Q, Hei T K
Center for Radiological Research, College of Physicians and Surgeons of Columbia University, VC 11-218, 630 West 168th Street, New York, NY 10032, USA.
Br J Cancer. 2002 Jun 17;86(12):1923-8. doi: 10.1038/sj.bjc.6600304.
Interaction between cell and extracellular matrix plays a crucial role in tumour invasion and metastasis. Using an immortalised human bronchial epithelial (BEP2D) cell model, the study here shows that expression of Betaig-h3 gene, which encodes a secreted adhesion molecule induced by transforming growth factor-beta, is markedly decreased in several independently generated, radiation-induced tumour cell lines (TL1-TL5) relative to parental BEP2D cells. Transfection of Betaig-h3 gene into tumour cells resulted in a significant reduction in tumour growth. While integrin receptor alpha5beta1 was overexpressed in tumour cells, its expression was corrected to the level found in control BEP2D cells after Betaig-h3 transfection. These data suggest that Betaig-h3 gene is involved in tumour progression by regulating integrin receptor alpha5beta1. The findings provide strong evidence that the Betaig-h3 gene has tumour suppressor function in human BEP2D cell model and suggest a potential target for interventional therapy.
细胞与细胞外基质之间的相互作用在肿瘤侵袭和转移中起着关键作用。利用永生化人支气管上皮(BEP2D)细胞模型,本研究表明,编码一种由转化生长因子-β诱导的分泌型粘附分子的Betaig-h3基因,在几个独立产生的辐射诱导肿瘤细胞系(TL1-TL5)中的表达相对于亲代BEP2D细胞显著降低。将Betaig-h3基因转染到肿瘤细胞中导致肿瘤生长显著减少。虽然整合素受体α5β1在肿瘤细胞中过表达,但在转染Betaig-h3后其表达恢复到对照BEP2D细胞中的水平。这些数据表明,Betaig-h3基因通过调节整合素受体α5β1参与肿瘤进展。这些发现提供了强有力的证据,证明Betaig-h3基因在人BEP2D细胞模型中具有肿瘤抑制功能,并提示了一个潜在的介入治疗靶点。
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