Mao Junhao, Ligon Keith L, Rakhlin Elena Y, Thayer Sarah P, Bronson Roderick T, Rowitch David, McMahon Andrew P
Department of Molecular and Cellular Biology, Harvard University, Cambridge, Massachusetts 02138, USA.
Cancer Res. 2006 Oct 15;66(20):10171-8. doi: 10.1158/0008-5472.CAN-06-0657.
We report a novel mouse model for the generation of sporadic tumors and show the efficiency of this approach by surveying Hedgehog (Hh)-related tumors. Up-regulation of the Hh pathway is achieved by conditionally regulated expression of an activated allele of Smoothened (R26-SmoM2) using either sporadic leakage or global postnatal induction of a ubiquitously expressed inducible Cre transgene (CAGGS-CreER). Following postnatal tamoxifen induction, CAGGS-CreER; R26-SmoM2 mice developed tumors with short latency and high penetrance. All mice exhibited rhabdomyosarcoma and basal cell carcinoma; 40% also developed medulloblastoma. In addition, mice showed a novel pancreatic lesion resembling low-grade mucinous cystic neoplasms in humans. In contrast, widespread activation of SmoM2 in the postnatal prostate epithelium results in no detectable morphologic outcome in 12-month-old mice. Comparison of gene expression profiles among diverse tumors identified several signature genes, including components of platelet-derived growth factor and insulin-like growth factor pathways, which may provide a common mechanistic link to the Hh-related malignancies. This experimental model provides a robust tool for exploring the process of Hh-dependent tumorigenesis and the treatment of such tumors. More generally, this approach provides a genetic platform for identifying tumorigenic potential in putative oncogenes and tumor suppressors and for more effective modeling of sporadic cancers in mice.
我们报告了一种用于生成散发性肿瘤的新型小鼠模型,并通过研究刺猬信号通路(Hh)相关肿瘤展示了该方法的有效性。通过使用散发性渗漏或在出生后全身性诱导普遍表达的可诱导性Cre转基因(CAGGS-CreER)来条件性调控激活型平滑受体(R26-SmoM2)等位基因的表达,从而实现Hh信号通路的上调。在出生后给予他莫昔芬诱导后,CAGGS-CreER; R26-SmoM2小鼠在短时间内且高频率地发生肿瘤。所有小鼠均出现横纹肌肉瘤和基底细胞癌;40%还发生了髓母细胞瘤。此外,小鼠出现了一种类似于人类低度黏液性囊性肿瘤的新型胰腺病变。相比之下,出生后前列腺上皮中SmoM2的广泛激活在12月龄小鼠中未导致可检测到的形态学变化。对不同肿瘤之间基因表达谱的比较鉴定出了几个特征基因,包括血小板衍生生长因子和胰岛素样生长因子通路的成分,这可能为与Hh相关的恶性肿瘤提供一个共同的机制联系。该实验模型为探索Hh依赖性肿瘤发生过程以及此类肿瘤的治疗提供了一个强大的工具。更普遍地说,这种方法为鉴定假定的癌基因和肿瘤抑制基因中的致瘤潜力以及在小鼠中更有效地模拟散发性癌症提供了一个遗传平台。