维甲酸
Wnt信号通路
维甲酸诱导孤儿G蛋白偶联受体
维甲酸受体
维甲酸受体γ
维甲酸受体β
生物
视黄醇X受体γ
维甲酸受体α
癌症研究
干瘪的
信号转导
细胞生物学
分子生物学
内分泌学
内科学
细胞培养
医学
遗传学
作者
Wayne Szeto,Wei Jiang,David A. Tice,Bonnee Rubinfeld,Philip G. Hollingshead,Sharon Fong,Debra L. Dugger,Truyen D. Pham,Daniel G. Yansura,T A Wong,J. Christopher Grimaldi,Racquel Corpuz,Jagdeep Singh,Gretchen Frantz,Bertrand Devaux,Craig Crowley,Ralph Schwall,David A. Eberhard,Luca Rastelli,Paul Polakis
出处
期刊:PubMed
[National Institutes of Health]
日期:2001-05-15
卷期号:61 (10): 4197-205
被引量:103
摘要
Genetic defects in the Wnt-1 signaling pathway contribute to human tumor progression and are especially prevalent in colorectal cancer. We screened mouse C57MG cells to isolate mRNAs induced by Wnt-1 and identified Stra6, an mRNA known to be up-regulated by retinoic acid. Up-regulation of Stra6 mRNA was also observed in hyperplastic mammary tissue and mammary gland tumors from transgenic mice expressing Wnt-1 and in human tumors that frequently harbor defects in Wnt-1 signaling. Stimulation of C57MG cells with retinoic acid plus Wnt-1 resulted in expression of Stra6 transcript to levels greatly exceeding that observed with either stimulus alone. This synergy could be explained in part by the up-regulation of retinoic acid receptor-gamma that was observed in response to Wnt-1 signaling. Accordingly, treatment of human colorectal cancer cell lines with retinoic acid resulted in the up-regulation of Stra6 mRNA and accumulation of Stra6 protein at the cell membrane. The data support a model in which Wnt-1 signaling synergizes with retinoids to activate retinoic acid receptor-gamma-responsive genes in human cancers.
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