增殖细胞表达的信使核糖核酸(mRNA)具有缩短的3'非翻译区和较少的微小RNA靶位点。
Proliferating cells express mRNAs with shortened 3' untranslated regions and fewer microRNA target sites.
作者信息
Sandberg Rickard, Neilson Joel R, Sarma Arup, Sharp Phillip A, Burge Christopher B
机构信息
Department of Biology, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.
出版信息
Science. 2008 Jun 20;320(5883):1643-7. doi: 10.1126/science.1155390.
Abstract
Messenger RNA (mRNA) stability, localization, and translation are largely determined by sequences in the 3' untranslated region (3'UTR). We found a conserved increase in expression of mRNAs terminating at upstream polyadenylation sites after activation of primary murine CD4+ T lymphocytes. This program, resulting in shorter 3'UTRs, is a characteristic of gene expression during immune cell activation and correlates with proliferation across diverse cell types and tissues. Forced expression of full-length 3'UTRs conferred reduced protein expression. In some cases the reduction in protein expression could be reversed by deletion of predicted microRNA target sites in the variably included region. Our data indicate that gene expression is coordinately regulated, such that states of increased proliferation are associated with widespread reductions in the 3'UTR-based regulatory capacity of mRNAs.
摘要
信使核糖核酸(mRNA)的稳定性、定位及翻译很大程度上由3'非翻译区(3'UTR)中的序列决定。我们发现,原代小鼠CD4+ T淋巴细胞激活后,在位于上游聚腺苷酸化位点处终止的mRNA表达出现保守性增加。该程序导致3'UTR缩短,是免疫细胞激活过程中基因表达的一个特征,并且与多种细胞类型和组织中的增殖相关。全长3'UTR的强制表达使蛋白质表达降低。在某些情况下,通过删除可变包含区域中预测的微小RNA靶位点,可以逆转蛋白质表达的降低。我们的数据表明,基因表达受到协同调控,因此增殖增加的状态与mRNA基于3'UTR的调控能力普遍降低相关。
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