Department of Pharmacology and Experimental Therapeutics, Division of Clinical Pharmacology, Thomas Jefferson University, Philadelphia, Pennsylvania, USA.
Gastroenterology. 2010 Jan;138(1):241-54. doi: 10.1053/j.gastro.2009.08.064. Epub 2009 Sep 6.
BACKGROUND & AIMS: GUCY2C is the intestinal receptor for the paracrine hormones guanylin and uroguanylin that converts guanosine-5'-triphosphate to cyclic guanosine monophosphate (cGMP). It functions as a tumor suppressor; its loss disrupts intestinal homeostasis and promotes tumorigenesis. We investigated the effects of GUCY2C loss on intestinal cell proliferation, metabolism, signaling, and tumorigenesis in mice.
Intestinal cell proliferation and metabolism were examined in Gucy2c(-/-) and colon cancer cells by microscopy, immunoblot, and functional analyses. Microarray analyses compared gene expression profiles of intestine cell from Gucy2c(-/-) and wild-type mice. v akt murine thymoma viral oncogene homolog (AKT) regulation and signaling were examined, and the role of AKT in GUCY2C-dependent tumorigenesis was defined in Gucy2c(-/-)Akt1(-/-) mice.
The size and number of intestinal crypts increased in Gucy2c(-/-) mice; the associated epithelial cells showed accelerated proliferation, increased glycolysis, and reduced oxidative phosphorylation, which was reversed by oral administration of cGMP. Conversely, activating guanylyl cyclase C in human colon cancer cells delayed cell-cycle progression, decreased DNA synthesis and colony formation, reduced glycolysis, and increased mitochondrial adenosine triphosphate production. AKT signaling pathways were activated in intestines of Gucy2c(-/-) mice, associated with increased AKT phosphorylation. Disruption of AKT activity, pharmacologically or genetically, reduced DNA synthesis, proliferation, and glycolysis, and increased mitochondrial biogenesis. Intestinal tumorigenesis increased after administration of azoxymethane to Gucy2c(-/-) mice, compared with wild-type mice, but was eliminated in Gucy2c(-/-)Akt1(-/-) mice.
GUCY2C is a tumor suppressor that controls proliferation and metabolism of intestinal epithelial cells by inactivating AKT signaling. This receptor and its ligands, which are paracrine hormones, might be novel candidates for anticolorectal cancer therapy.
GUCY2C 是旁分泌激素——鸟苷酸环化酶 C(guanylin 和 uroguanylin)的肠道受体,可将鸟苷-5'-三磷酸转化为环鸟苷单磷酸(cGMP)。它作为一种肿瘤抑制因子发挥作用;其缺失会破坏肠道内稳态并促进肿瘤发生。我们研究了 GUCY2C 缺失对小鼠肠道细胞增殖、代谢、信号转导和肿瘤发生的影响。
通过显微镜、免疫印迹和功能分析检查 Gucy2c(-/-) 和结肠癌细胞中的肠细胞增殖和代谢。比较 Gucy2c(-/-) 和野生型小鼠肠细胞的基因表达谱。研究了 v akt 鼠胸腺瘤病毒癌基因同源物(AKT)的调节和信号转导,并在 Gucy2c(-/-)Akt1(-/-) 小鼠中定义了 AKT 在 GUCY2C 依赖性肿瘤发生中的作用。
Gucy2c(-/-) 小鼠的肠道隐窝大小和数量增加;相关的上皮细胞表现出加速增殖、增加糖酵解和减少氧化磷酸化,这些变化可通过口服 cGMP 逆转。相反,激活人结肠癌细胞中的鸟苷酸环化酶 C 会延迟细胞周期进程,减少 DNA 合成和集落形成,减少糖酵解并增加线粒体三磷酸腺苷的产生。Gucy2c(-/-) 小鼠的 AKT 信号通路被激活,与 AKT 磷酸化增加有关。药理学或遗传学上破坏 AKT 活性可减少 DNA 合成、增殖和糖酵解,并增加线粒体生物发生。与野生型小鼠相比,给予 Gucy2c(-/-) 小鼠氧化偶氮甲烷后,肠道肿瘤发生增加,但在 Gucy2c(-/-)Akt1(-/-) 小鼠中消除。
GUCY2C 是一种肿瘤抑制因子,通过失活 AKT 信号来控制肠道上皮细胞的增殖和代谢。该受体及其配体作为旁分泌激素,可能是抗结直肠癌治疗的新候选物。
