Centre for Genomic Regulation, Dr Aiguader 88, 08003 Barcelona, Spain.
Nucleic Acids Res. 2013 Jan 7;41(1):e31. doi: 10.1093/nar/gks968. Epub 2012 Oct 22.
The transcriptional silencing of one of the female X-chromosomes is a finely regulated process that requires accumulation in cis of the long non-coding RNA X-inactive-specific transcript (Xist) followed by a series of epigenetic modifications. Little is known about the molecular machinery regulating initiation and maintenance of chromosomal silencing. Here, we introduce a new version of our algorithm catRAPID to investigate Xist associations with a number of proteins involved in epigenetic regulation, nuclear scaffolding, transcription and splicing processes. Our method correctly identifies binding regions and affinities of protein interactions, providing a powerful theoretical framework for the study of X-chromosome inactivation and other events mediated by ribonucleoprotein associations.
X 染色体失活过程中,一条 X 染色体上的转录沉默是一个精细调控的过程,需要在顺式位置积累长非编码 RNA X 失活特异性转录本(Xist),然后进行一系列表观遗传修饰。然而,关于调控染色体沉默起始和维持的分子机制知之甚少。在这里,我们引入了我们的算法 catRAPID 的新版本,用于研究 Xist 与许多参与表观遗传调控、核支架、转录和剪接过程的蛋白质之间的关联。我们的方法可以正确识别蛋白质相互作用的结合区域和亲和力,为研究 X 染色体失活和其他由核糖核蛋白相关介导的事件提供了强大的理论框架。
Zotero 插件