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Genetic screens reveal mechanisms for the transcriptional regulation of tissue-specific genes in normal cells and tumors

机译:遗传筛选揭示正常细胞和肿瘤中组织特异性基因转录调控的机制

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摘要

The proper tissue-specific regulation of gene expression is essential for development and homeostasis in metazoans. However, the illegitimate expression of normally tissue-restricted genes—like testis- or placenta-specific genes—is frequently observed in tumors; this promotes transformation, but also allows immunotherapy. Two important questions are: how is the expression of these genes controlled in healthy cells? And how is this altered in cancer? To address these questions, we used an unbiased approach to test the ability of 350 distinct genetic or epigenetic perturbations to induce the illegitimate expression of over 40 tissue-restricted genes in primary human cells. We find that almost all of these genes are remarkably resistant to reactivation by a single alteration in signaling pathways or chromatin regulation. However, a few genes differ and are more readily activated; one is the placenta-expressed gene ADAM12, which promotes invasion. Using cellular systems, an animal model, and bioinformatics, we find that a non-canonical but druggable TGF-β/KAT2A/TAK1 axis controls ADAM12 induction in normal and cancer cells. More broadly, our data show that illegitimate gene expression in cancer is an heterogeneous phenomenon, with a few genes activatable by simple events, and most genes likely requiring a combination of events to become reactivated.
机译:基因表达的适当组织特异性调节对于后生动物的发育和体内平衡至关重要。然而,通常在肿瘤中观察到正常组织限制性基因(如睾丸或胎盘特异性基因)的非法表达。这可以促进转化,但也可以进行免疫治疗。两个重要的问题是:如何在健康细胞中控制这些基因的表达?癌症如何改变?为了解决这些问题,我们使用了一种无偏方法来测试350种不同的遗传或表观遗传扰动在原代人类细胞中诱导40多种组织受限基因的非法表达的能力。我们发现,几乎所有这些基因都对信号通路或染色质调节的单个改变具有明显的抵抗再激活作用。但是,一些基因不同并且更容易被激活。一种是胎盘表达的基因ADAM12,它促进侵袭。使用细胞系统,动物模型和生物信息学,我们发现非规范但可药物化的TGF-β/ KAT2A / TAK1轴控制正常细胞和癌细胞中的ADAM12诱导。更广泛地说,我们的数据表明,癌症中非法基因的表达是一种异质现象,其中一些基因可以通过简单事件激活,而大多数基因可能需要事件的组合才能重新激活。

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