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着丝粒卫星的转录特异性爆发是染色中心形成和早期小鼠发育所必需的。

A strand-specific burst in transcription of pericentric satellites is required for chromocenter formation and early mouse development.

机构信息

Laboratory of Nuclear Dynamics and Genome Plasticity, Unité Mixte de Recherche, 218 Centre National de la Recherche Scientifique/Institut Curie, 26, rue d'Ulm, 75248 Paris Cedex 05, France.

出版信息

Dev Cell. 2010 Oct 19;19(4):625-38. doi: 10.1016/j.devcel.2010.09.002.

Abstract

At the time of fertilization, the paternal genome lacks the typical configuration and marks characteristic of pericentric heterochromatin. It is thus essential to understand the dynamics of this region during early development, its importance during that time period and how a somatic configuration is attained. Here, we show that pericentric satellites undergo a transient peak in expression precisely at the time of chromocenter formation. This transcription is regulated in a strand-specific manner in time and space and is strongly biased by the parental asymmetry. The transcriptional upregulation follows a developmental clock, yet when replication is blocked chromocenter formation is impeded. Furthermore, interference with major satellite transcripts using locked nucleic acid (LNA)-DNA gapmers results in developmental arrest before completion of chromocenter formation. We conclude that the exquisite strand-specific expression dynamics at major satellites during the 2-cell stage, with both up and downregulation, are necessary events for proper chromocenter organization and developmental progression.

摘要

在受精时,父本基因组缺乏典型的着丝粒异染色质的结构和特征标记。因此,了解早期发育过程中该区域的动态、其在该时期的重要性以及如何获得体染色体结构是至关重要的。在这里,我们表明,着丝粒卫星在 precisely at the time of chromocenter formation 处经历了一个短暂的表达峰值。这种转录在时间和空间上以链特异性方式进行调控,并且受到亲本不对称性的强烈影响。转录的上调遵循发育时钟,但当复制被阻断时,着丝粒的形成就会受到阻碍。此外,使用锁核酸(LNA)-DNA 缺口嵌合体干扰主要卫星转录本会导致在完成着丝粒形成之前发生发育停滞。我们得出结论,在 2 细胞阶段,主要卫星的精确链特异性表达动态,包括上调和下调,是正确的着丝粒组织和发育进展所必需的事件。

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