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TET enzymes: double agents in the transposable element–host genome conflict

机译:TET酶:转座因子与宿主基因组冲突中的双重作用

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摘要

The mouse genome is replete with retrotransposon sequences, from evolutionarily young elements with mutagenic potential that must be controlled, to inactive molecular fossils whose sequences can be domesticated over evolutionary time to benefit the host genome. In an exciting new study, de la Rica and colleagues have uncovered a complex relationship between ten-eleven translocation (TET) proteins and retrotransposons in mouse embryonic stem cells (ESCs), implicating TETs as enhancers in the exaptation and function of retroelement sequences. Furthermore, they have demonstrated that active demethylation of retrotransposons does not correlate with their increased expression in ESCs, calling into question long-held assumptions regarding the importance of DNA demethylation for retrotransposon expression, and revealing novel epigenetic players in retrotransposon control.
机译:小鼠基因组中充满了反转录转座子序列,从必须控制诱变潜力的进化年轻元件到无活性分子化石,其序列可以在进化时间内被驯化,从而使宿主基因组受益。在一项激动人心的新研究中,de la Rica及其同事发现了小鼠胚胎干细胞(ESC)中的11-11易位(TET)蛋白与逆转座子之间的复杂关系,暗示TET作为逆转录元件序列的增强和功能的增强子。此外,他们已经证明逆转座子的主动去甲基化与它们在ESC中的表达增加无关,这引起了人们对DNA脱甲基对逆转座子表达的重要性的长期存在的质疑,并揭示了逆转录转座子控制中新的表观遗传因素。

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