2nd Department of Medicine, Klinikum rechts der Isar, Technical University Munich, Germany.
Cancer Cell. 2010 Aug 9;18(2):135-46. doi: 10.1016/j.ccr.2010.06.013.
Colonic cancers with a serrated morphology have been proposed to comprise a molecularly distinct tumor entity following an alternative pathway of genetic alterations independently of APC mutations. We demonstrate that intestinal epithelial cell specific expression of oncogenic K-ras(G12D) in mice induces serrated hyperplasia, which is characterized by p16(ink4a) overexpression and induction of senescence. Deletion of Ink4a/Arf in K-ras(G12D) expressing mice prevents senescence and leads to invasive, metastasizing carcinomas with morphological and molecular alterations comparable to human KRAS mutated serrated tumors. Thus, we suggest that oncogenic K-ras represents a key player during an alternative, serrated pathway to colorectal cancer and hence propose RAS-RAF-MEK signaling apart from APC as an additional gatekeeper in colorectal tumor development.
锯齿状形态的结肠癌被认为是一种分子上不同的肿瘤实体,其遗传改变途径不同于 APC 突变。我们证明,在小鼠中特异性表达致癌 K-ras(G12D)会诱导锯齿状增生,其特征是 p16(ink4a)过表达和衰老诱导。在表达 K-ras(G12D)的小鼠中删除 Ink4a/Arf 可防止衰老,并导致侵袭性、转移性癌,其形态和分子改变与人类 KRAS 突变的锯齿状肿瘤相似。因此,我们认为致癌 K-ras 代表结直肠癌另一种锯齿状途径中的关键参与者,因此除 APC 外,RAS-RAF-MEK 信号传导也被提议作为结直肠肿瘤发展的另一个守门员。
