Department of Pediatrics, University of Arizona Health Sciences Center, Tucson, Arizona.
Department of Pathology, University of Arizona Health Sciences Center, Tucson, Arizona.
Cell Mol Gastroenterol Hepatol. 2018 Aug 24;7(1):19-31. doi: 10.1016/j.jcmgh.2018.08.005. eCollection 2019.
BACKGROUND & AIMS: Lgr5 overexpression has been detected in colorectal cancers (CRCs), including some cases of colitis-associated CRCs. In colitis-associated CRCs, chronic inflammation is a contributing factor in carcinogenesis. We recently reported that intestinal Na/H exchanger isoform 8 (NHE8) plays an important role in intestinal mucosal protection and that loss of NHE8 expression results in an ulcerative colitis-like condition. Therefore, we hypothesized that NHE8 may be involved in the development of intestinal tumors.
We assessed NHE8 expression in human CRCs by immunohistochemistry and studied tumor burden in NHE8 knockout (KO) mice using an azoxymethane/dextran sodium sulfate colon cancer model. We also evaluated cell proliferation in HT29 cells and assessed tumor growth in NOD scid gamma (NSG) mice xenografted with HT29 cells. To verify if a relationship exists between Lgr5 and NHE8 expression, we analyzed Lgr5 expression in NHE8KO mice by polymerase chain reaction and in situ hybridization. Lgr5 expression and cell proliferation in the absence of NHE8 were confirmed in colonic organoid cultures. The expression of β-catenin and c-Myc also were analyzed to evaluate Wnt/β-catenin activation.
NHE8 was undetectable in human CRC tissues. Although only 9% of NHE8 wild-type mice showed tumorigenesis in the azoxymethane/dextran sodium sulfate colon cancer model, almost 10 times more NHE8KO mice (89%) developed tumors. In the absence of NHE8, a higher colony formation unit was discovered in HT29 cells. In NSG mice, larger tumors developed at the site where HT29 cells were injected compared with HT29 cells. Furthermore, NHE8 deficiency resulted in increased Lgr5 expression in the colon, in HT29-derived tumors, and in colonoids. The absence of NHE8 also increased Wnt/β-catenin activation.
NHE8 might be an intrinsic factor that regulates Wnt/β-catenin in the intestine.
Lgr5 在结直肠癌(CRC)中过表达,包括一些炎症相关性 CRC。在炎症相关性 CRC 中,慢性炎症是致癌的一个促成因素。我们最近报道,肠道钠离子/氢离子交换体 8(NHE8)在肠道黏膜保护中发挥重要作用,而 NHE8 表达缺失会导致溃疡性结肠炎样状态。因此,我们假设 NHE8 可能参与肠道肿瘤的发生。
我们通过免疫组织化学评估了人 CRC 中的 NHE8 表达,并使用氧化偶氮甲烷/葡聚糖硫酸钠结肠癌模型研究了 NHE8 敲除(KO)小鼠的肿瘤负担。我们还评估了 HT29 细胞中的细胞增殖,并在 NOD scid gamma(NSG)小鼠中评估了 HT29 细胞移植瘤的生长情况。为了验证 Lgr5 和 NHE8 表达之间是否存在关系,我们通过聚合酶链反应和原位杂交分析了 NHE8KO 小鼠中的 Lgr5 表达。在结肠类器官培养中证实了缺乏 NHE8 时 Lgr5 表达和细胞增殖。还分析了β-连环蛋白和 c-Myc 的表达,以评估 Wnt/β-连环蛋白的激活。
NHE8 在人 CRC 组织中无法检测到。虽然在氧化偶氮甲烷/葡聚糖硫酸钠结肠癌模型中,只有 9%的 NHE8 野生型小鼠发生肿瘤形成,但 NHE8KO 小鼠(89%)几乎有 10 倍的肿瘤形成。在缺乏 NHE8 的情况下,HT29 细胞中的集落形成单位更高。在 NSG 小鼠中,与 HT29 细胞相比,在注射 HT29 细胞的部位形成了更大的肿瘤。此外,NHE8 缺乏导致结肠、HT29 衍生肿瘤和类器官中 Lgr5 表达增加。NHE8 缺乏也增加了 Wnt/β-连环蛋白的激活。
NHE8 可能是调节肠道 Wnt/β-连环蛋白的内在因素。
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