胃泌素前体靶向治疗后抑制β-连环蛋白/Tcf-4可降低肠道肿瘤的生长并促进其分化。
Beta-catenin/Tcf-4 inhibition after progastrin targeting reduces growth and drives differentiation of intestinal tumors.
作者信息
Pannequin Julie, Delaunay Nathalie, Buchert Michael, Surrel Fanny, Bourgaux Jean-François, Ryan Joanne, Boireau Stéphanie, Coelho Jessica, Pélegrin André, Singh Pomila, Shulkes Arthur, Yim Mildred, Baldwin Graham S, Pignodel Christine, Lambeau Gérard, Jay Philippe, Joubert Dominique, Hollande Frédéric
机构信息
CNRS UMR5203, Montpellier, France.
出版信息
Gastroenterology. 2007 Nov;133(5):1554-68. doi: 10.1053/j.gastro.2007.08.023. Epub 2007 Oct 24.
BACKGROUND & AIMS: Aberrant activation of the beta-catenin/Tcf-4 transcriptional complex represents an initiating event for colorectal carcinogenesis, shifting the balance from differentiation toward proliferation in colonic crypts. Here, we assessed whether endogenous progastrin, encoded by a target gene of this complex, was in turn able to regulate beta-catenin/Tcf-4 activity in adenomatous polyposis coli (APC)-mutated cells, and we analyzed the impact of topical progastrin depletion on intestinal tumor growth in vivo.
METHODS
Stable or transient RNA silencing of the GAST gene was induced in human tumor cells and in mice carrying a heterozygous Apc mutation (APCDelta14), which overexpress progastrin but not amidated or glycine-extended gastrin.
RESULTS
Depletion of endogenous progastrin production strongly decreased intestinal tumor growth in vivo through a marked inhibition of constitutive beta-catenin/Tcf-4 activity in tumor cells. This effect was mediated by the de novo expression of the inhibitor of beta-catenin and Tcf-4 (ICAT), resulting from a down-regulation of integrin-linked kinase in progastrin-depleted cells. Accordingly, ICAT down-regulation was correlated with progastrin overexpression and Tcf-4 target gene activation in human colorectal tumors, and ICAT repression was detected in the colon epithelium of tumor-prone, progastrin-overexpressing mice. In APCDelta14 mice, small interfering RNA-mediated progastrin depletion not only reduced intestinal tumor size and numbers, but also increased goblet cell lineage differentiation and cell apoptosis in the remaining adenomas.
CONCLUSIONS
Thus, depletion of endogenous progastrin inhibits the tumorigenicity of APC-mutated colorectal cancer cells in vivo by promoting ICAT expression, thereby counteracting Tcf-4 activity. Progastrin targeting strategies should provide an exciting prospect for the differentiation therapy of colorectal cancer.
背景与目的
β-连环蛋白/Tcf-4转录复合体的异常激活是结直肠癌发生的起始事件,它改变了结肠隐窝中从分化向增殖的平衡。在此,我们评估了由该复合体的一个靶基因编码的内源性胃泌素原是否能够反过来调节腺瘤性息肉病(APC)突变细胞中的β-连环蛋白/Tcf-4活性,并分析了局部胃泌素原缺失对体内肠道肿瘤生长的影响。
方法
在人肿瘤细胞和携带杂合Apc突变(APCDelta14)的小鼠中诱导GAST基因的稳定或瞬时RNA沉默,这些小鼠过度表达胃泌素原但不表达酰胺化或甘氨酸延伸型胃泌素。
结果
内源性胃泌素原产生的缺失通过显著抑制肿瘤细胞中组成型β-连环蛋白/Tcf-4活性,在体内强烈降低了肠道肿瘤生长。这种效应是由β-连环蛋白和Tcf-4抑制剂(ICAT)的从头表达介导的,这是由于胃泌素原缺失细胞中整合素连接激酶的下调所致。相应地,ICAT下调与人类结直肠癌中胃泌素原过表达和Tcf-4靶基因激活相关,并且在易患肿瘤、胃泌素原过表达的小鼠的结肠上皮中检测到ICAT抑制。在APCDelta14小鼠中,小干扰RNA介导的胃泌素原缺失不仅减少了肠道肿瘤的大小和数量,还增加了剩余腺瘤中杯状细胞谱系分化和细胞凋亡。
结论
因此,内源性胃泌素原的缺失通过促进ICAT表达在体内抑制APC突变的结直肠癌细胞的致瘤性,从而抵消Tcf-4活性。靶向胃泌素原的策略应为结直肠癌的分化治疗提供令人兴奋的前景。
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