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Wnt3a-dependent and -independent protein interaction networks of chromatin-bound β-catenin in mouse embryonic stem cells

机译:小鼠胚胎干细胞中与染色质结合的β-catenin的Wnt3a依赖性和非依赖性蛋白相互作用网络

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Canonical Wnt signaling is repeatedly used during development to control cell fate, and it is often implicated in human cancer. β-catenin, the effector of Wnt signaling, has a dual function in the cell and is involved in both cell adhesion and transcription. Nuclear β-catenin controls transcription through association with transcription factors of the TCF family and the recruitment of epigenetic modifiers. In this study, we used a strategy combining the genetic manipulation of mouse embryonic stem cells with affinity purification and quantitative mass spectroscopy utilizing stable isotope labeling with amino acids in cell culture to study the interactome of chromatin-bound β-catenin with and without Wnt3a stimulation. We uncovered previously unknown interactions of β-catenin with transcription factors and chromatin-modifying complexes. Our proof-of-principle experiments show that β-catenin can recruit the H3K4me2/1 demethylase LSD1 to regulate the expression of the tumor suppressor Lefty1 in mouse embryonic stem cells. The mRNA levels of LSD1 and β-catenin are inversely correlated with the levels of Lefty1 in pancreas and breast tumors, implying that this mechanism is common to mouse embryonic stem cells and cancer cells.
机译:规范Wnt信号在发育过程中被反复使用以控制细胞命运,并且经常与人类癌症有关。 Wnt信号的效应子β-catenin在细胞中具有双重功能,并参与细胞粘附和转录。 β-catenin核通过与TCF家族的转录因子缔合和表观遗传修饰子的募集来控制转录。在这项研究中,我们采用了将小鼠胚胎干细胞的基因操作与亲和纯化相结合的策略,并利用稳定的同位素标记和细胞培养中的氨基酸进行了定量质谱分析,研究了有无Wnt3a刺激的染色质结合β-catenin的相互作用。我们发现了以前未知的β-catenin与转录因子和染色质修饰复合物的相互作用。我们的原理验证实验表明,β-连环蛋白可以募集H3K4me2 / 1脱甲基酶LSD1来调节小鼠胚胎干细胞中抑癌基因Lefty1的表达。 LSD1和β-catenin的mRNA水平与胰腺和乳腺肿瘤中Lefty1的水平呈负相关,这表明这种机制在小鼠胚胎干细胞和癌细胞中很常见。

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