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Daxx maintains endogenous retroviral silencing and restricts cellular plasticity in vivo

机译:Daxx保持内源性逆转录病毒沉默并限制体内细胞塑性

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Tumor sequencing studies have emphasized the role of epigenetics and altered chromatin homeostasis in cancer. Mutations in DAXX , which encodes a chaperone for the histone 3.3 variant, occur in 25% of pancreatic neuroendocrine tumors (PanNETs). To advance our understanding of physiological functions of Daxx, we developed a conditional Daxx allele in mice. We demonstrate that Daxx loss is well tolerated in the pancreas but creates a permissive transcriptional state that cooperates with environmental stress (inflammation) and other genetic lesions ( Men1 loss) to alter gene expression and cell state, impairing pancreas recovery from inflammatory stress in vivo. The transcriptional changes are associated with dysregulation of endogenous retroviral elements (ERVs), and dysregulation of endogenous genes near ERVs is also observed in human PanNETs with DAXX mutations. Our results reveal a physiologic function of DAXX, provide a mechanism associated with impaired tissue regeneration and tumorigenesis, and expand our understanding of ERV regulation in somatic cells.
机译:肿瘤测序研究强调了表观遗传学和改变染色质稳态在癌症中的作用。 Daxx中的突变,其编码组蛋白3.3变体的伴侣,发生在25%的胰腺神经内分泌肿瘤(Pannets)中发生。为了推进我们对Daxx的生理功能的理解,我们在小鼠中开发了一种有条件的Daxx等位基因。我们证明Daxx损失在胰腺中耐受良好,但是产生与环境应激(炎症)和其他遗传病变(MEN1损失)配合以改变基因表达和细胞状态的允许转录状态,从体内损害胰腺恢复损害胰腺恢复。转录变化与内源性逆转录病毒元素(ERV)的失调相关,并且在具有Daxx突变的人培养中也观察到ERV附近的内源基因的失调。我们的结果揭示了Daxx的生理功能,提供了与组织再生和肿瘤患者有关的机制,并扩大了我们对体细胞中ERV调节的理解。

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