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初生 RNA 支架有助于染色体域结构并对抗染色质的紧缩。

Nascent RNA scaffolds contribute to chromosome territory architecture and counter chromatin compaction.

机构信息

Department of Neurology and Pediatrics, University of Massachusetts Medical School, 55 Lake Avenue North, Worcester, MA 01655, USA.

Department of Neurology and Pediatrics, University of Massachusetts Medical School, 55 Lake Avenue North, Worcester, MA 01655, USA.

出版信息

Mol Cell. 2021 Sep 2;81(17):3509-3525.e5. doi: 10.1016/j.molcel.2021.07.004. Epub 2021 Jul 27.

Abstract

Nuclear chromosomes transcribe far more RNA than required to encode protein. Here we investigate whether non-coding RNA broadly contributes to cytological-scale chromosome territory architecture. We develop a procedure that depletes soluble proteins, chromatin, and most nuclear RNA from the nucleus but does not delocalize XIST, a known architectural RNA, from an insoluble chromosome "scaffold." RNA-seq analysis reveals that most RNA in the nuclear scaffold is repeat-rich, non-coding, and derived predominantly from introns of nascent transcripts. Insoluble, repeat-rich (CT-1) RNA co-distributes with known scaffold proteins including scaffold attachment factor A (SAF-A), and distribution of these components inversely correlates with chromatin compaction in normal and experimentally manipulated nuclei. We further show that RNA is required for SAF-A to interact with chromatin and for enrichment of structurally embedded "scaffold attachment regions" prevalent in euchromatin. Collectively, the results indicate that long nascent transcripts contribute a dynamic structural role that promotes the open architecture of active chromosome territories.

摘要

核染色体转录的 RNA 远远超过编码蛋白质所需的 RNA。在这里,我们研究了非编码 RNA 是否广泛有助于细胞尺度染色体领域结构。我们开发了一种程序,该程序可从细胞核中除去可溶性蛋白质、染色质和大多数核 RNA,但不会使已知结构 RNA XIST 从不溶性染色体“支架”上解聚。RNA-seq 分析表明,核支架中的大多数 RNA 富含重复序列、非编码且主要来源于新生转录本的内含子。不溶性、富含重复序列(CT-1)的 RNA 与已知的支架蛋白共分布,包括支架附着因子 A(SAF-A),这些成分的分布与正常和实验操作核中染色质的紧缩呈负相关。我们进一步表明,RNA 是 SAF-A 与染色质相互作用以及富含结构嵌入的“支架附着区”所必需的,这些区在常染色质中普遍存在。总的来说,这些结果表明,长的新生转录本发挥了动态结构作用,促进了活性染色体领域的开放结构。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2db0/8419111/2e45e97e6f67/nihms-1728258-f0002.jpg

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