Histone acetylation-mediated chromatin compaction during mouse spermatogenesis.

J Govin, C Lestrat, C Caron, C Pivot-Pajot, S Rousseaux, S Khochbin
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引用次数: 56

Abstract

One of the most dramatic chromatin remodelling events takes place during mammalian spermatogenesis involving massive incorporation of somatic and testis-specific histone variants, as well as generalized histone modifications before their replacement by new DNA packaging proteins. Our data suggest that the induced histone acetylation occurring after meiosis may direct the first steps of genome compaction. Indeed, a double bromodomain-containing protein expressed in postmeiotic cells, Brdt, shows the extraordinary capacity to specifically condense acetylated chromatin in vivo and in vitro. In elongating spermatids, Brdt widely co-localizes with acetylated histones before accumulating in condensed chromatin domains. These domains preferentially maintain their acetylation status until late spermatogenesis. Based on these data, we propose that Brdt mediates a general histone acetylation-induced chromatin compaction and also maintains differential acetylation of specific regions, and is therefore involved in organizing the spermatozoon's genome.

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小鼠精子发生过程中组蛋白乙酰化介导的染色质压实。
最引人注目的染色质重塑事件之一发生在哺乳动物精子发生过程中,涉及体细胞和睾丸特异性组蛋白变异的大量合并,以及组蛋白在被新的DNA包装蛋白取代之前的普遍修饰。我们的数据表明,减数分裂后发生的诱导组蛋白乙酰化可能指导基因组压实的第一步。事实上,在减数分裂后细胞中表达的含有双溴结构域的蛋白Brdt,在体内和体外都显示出特异性浓缩乙酰化染色质的非凡能力。在伸长的精细胞中,Brdt广泛地与乙酰化组蛋白共定位,然后在浓缩的染色质结构域中积累。这些结构域优先维持其乙酰化状态,直到精子发生晚期。基于这些数据,我们提出Brdt介导组蛋白乙酰化诱导的染色质压实,并维持特定区域的差异乙酰化,因此参与了精子基因组的组织。
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