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上游RNA加工对μS与μM聚腺苷酸化位点选择的影响。

Effect of upstream RNA processing on selection of mu S versus mu M poly(A) sites.

作者信息

Abuodeh R, Wei H, Yuan D

机构信息

Laboratory of Molecular Pathology, Department of Pathology, University of Texas Southwestern Medical Center,5323 Harry Hines Boulevard, Dallas, TX 75235, USA.

出版信息

Nucleic Acids Res. 1998 Dec 1;26(23):5417-24. doi: 10.1093/nar/26.23.5417.

Abstract

All of the regulatory factors responsible for augmenting microseconds mRNA levels preceding the dramatic increase in secretory IgM production upon B cell activation has not been totally elucidated. Whereas previous experiments have centered on the region of the gene specifying the choice between splicing to mu M exons versus selection of the mu S poly(A) site, we have found that upstream sequences within the Cmu gene, specifically the Cmu 4 acceptor splice site together with intronic sequences between the Cmu 3++ and Cmu 4 exons, play an important role in dictating the precision or the extent of splicing to the mu M exons even under conditions in which functional polyadenylation factors should be in excess. Therefore, splicing of upstream exons can affect remotely located downstream exons. These findings suggest that regulation of differential mu S/mu M mRNA expression may involve general processing enzymes that recognize specific cis -regulatory sequences residing within the body of the mu gene and account for the unique ability of activated B cells to secrete copious amounts of IgM.

摘要

在B细胞活化后分泌性IgM产量急剧增加之前,所有负责提高微秒级mRNA水平的调节因子尚未完全阐明。尽管先前的实验集中在基因区域,该区域决定了剪接至μM外显子与选择μS聚腺苷酸化位点之间的选择,但我们发现Cμ基因内的上游序列,特别是Cμ4受体剪接位点以及Cμ3++和Cμ4外显子之间的内含子序列,即使在功能性聚腺苷酸化因子应该过量的条件下,在决定剪接至μM外显子的精确性或程度方面也起着重要作用。因此,上游外显子的剪接可以远程影响位于下游的外显子。这些发现表明,μS/μM mRNA差异表达的调节可能涉及识别位于μ基因体内特定顺式调节序列的一般加工酶,并解释了活化B细胞分泌大量IgM的独特能力。

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