囊性纤维化跨膜传导调节因子是小鼠和人类肠道癌中的一种肿瘤抑制基因。
CFTR is a tumor suppressor gene in murine and human intestinal cancer.
作者信息
Than B L N, Linnekamp J F, Starr T K, Largaespada D A, Rod A, Zhang Y, Bruner V, Abrahante J, Schumann A, Luczak T, Walter J, Niemczyk A, O'Sullivan M G, Medema J P, Fijneman R J A, Meijer G A, Van den Broek E, Hodges C A, Scott P M, Vermeulen L, Cormier R T
机构信息
Department of Biomedical Sciences, University of Minnesota Medical School, Duluth, MN, USA.
Laboratory of Experimental Oncology and Radiobiology, Center for Experimental Molecular Medicine, Academic Medical Center, Amsterdam, the Netherlands.
出版信息
Oncogene. 2016 Aug 11;35(32):4179-87. doi: 10.1038/onc.2015.483. Epub 2016 Jan 11.
CFTR, the cystic fibrosis (CF) gene, encodes for the CFTR protein that plays an essential role in anion regulation and tissue homeostasis of various epithelia. In the gastrointestinal (GI) tract CFTR promotes chloride and bicarbonate secretion, playing an essential role in ion and acid-base homeostasis. Cftr has been identified as a candidate driver gene for colorectal cancer (CRC) in several Sleeping Beauty DNA transposon-based forward genetic screens in mice. Further, recent epidemiological and clinical studies indicate that CF patients are at high risk for developing tumors in the colon. To investigate the effects of CFTR dysregulation on GI cancer, we generated Apc(Min) mice that carried an intestinal-specific knockout of Cftr. Our results indicate that Cftr is a tumor suppressor gene in the intestinal tract as Cftr mutant mice developed significantly more tumors in the colon and the entire small intestine. In Apc(+/+) mice aged to ~1 year, Cftr deficiency alone caused the development of intestinal tumors in >60% of mice. Colon organoid formation was significantly increased in organoids created from Cftr mutant mice compared with wild-type controls, suggesting a potential role of Cftr in regulating the intestinal stem cell compartment. Microarray data from the Cftr-deficient colon and the small intestine identified dysregulated genes that belong to groups of immune response, ion channel, intestinal stem cell and other growth signaling regulators. These associated clusters of genes were confirmed by pathway analysis using Ingenuity Pathway Analysis and gene set enrichment analysis (GSEA). We also conducted RNA Seq analysis of tumors from Apc(+/+) Cftr knockout mice and identified sets of genes dysregulated in tumors including altered Wnt β-catenin target genes. Finally we analyzed expression of CFTR in early stage human CRC patients stratified by risk of recurrence and found that loss of expression of CFTR was significantly associated with poor disease-free survival.
囊性纤维化(CF)基因CFTR编码CFTR蛋白,该蛋白在各种上皮细胞的阴离子调节和组织稳态中起着至关重要的作用。在胃肠道中,CFTR促进氯离子和碳酸氢根分泌,在离子和酸碱平衡中起关键作用。在几项基于睡美人DNA转座子的小鼠正向遗传筛选中,Cftr已被确定为结直肠癌(CRC)的候选驱动基因。此外,最近的流行病学和临床研究表明,CF患者患结肠癌的风险很高。为了研究CFTR失调对胃肠道癌症的影响,我们构建了肠道特异性敲除Cftr的Apc(Min)小鼠。我们的结果表明,Cftr是肠道中的肿瘤抑制基因,因为Cftr突变小鼠在结肠和整个小肠中发生的肿瘤明显更多。在年龄约为1岁的Apc(+/+)小鼠中,仅Cftr缺陷就导致超过60%的小鼠发生肠道肿瘤。与野生型对照相比,Cftr突变小鼠来源的类器官中结肠类器官的形成显著增加,这表明Cftr在调节肠道干细胞区室中可能发挥作用。来自Cftr缺陷结肠和小肠的微阵列数据确定了属于免疫反应、离子通道、肠道干细胞和其他生长信号调节因子组的失调基因。使用 Ingenuity Pathway Analysis和基因集富集分析(GSEA)通过通路分析证实了这些相关的基因簇。我们还对Apc(+/+) Cftr敲除小鼠的肿瘤进行了RNA测序分析,并确定了肿瘤中失调的基因集,包括Wntβ-连环蛋白靶基因的改变。最后,我们分析了按复发风险分层的早期人类CRC患者中CFTR的表达,发现CFTR表达缺失与无病生存期差显著相关。
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