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3'-5'外切核糖核酸酶Dis3L2在控制细胞增殖和组织生长中的新作用。

A novel role for the 3'-5' exoribonuclease Dis3L2 in controlling cell proliferation and tissue growth.

作者信息

Towler Benjamin P, Jones Christopher I, Harper Kirsty L, Waldron Joseph A, Newbury Sarah F

机构信息

a Brighton and Sussex Medical School, University of Sussex , Brighton , UK.

出版信息

RNA Biol. 2016 Dec;13(12):1286-1299. doi: 10.1080/15476286.2016.1232238. Epub 2016 Sep 14.

Abstract

In a complex organism, cell proliferation and apoptosis need to be precisely controlled in order for tissues to develop correctly. Excessive cell proliferation can lead to diseases such as cancer. We have shown that the exoribonuclease Dis3L2 is required for the correct regulation of proliferation in a natural tissue within the model organism Drosophila melanogaster. Dis3L2 is a member of a highly conserved family of exoribonucleases that degrade RNA in a 3'-5' direction. We show that knockdown of dis3L2 in the Drosophila wing imaginal discs results in substantial wing overgrowth due to increased cellular proliferation rather than an increase in cell size. Imaginal discs are specified in the embryo before proliferating and differentiating to form the adult structures of the fly. Using RNA-seq we identified a small set of mRNAs that are sensitive to Dis3L2 activity. Of the mRNAs which increase in levels and are therefore potential targets of Dis3L2, we identified 2 that change at the post-transcriptional level but not at the transcriptional level, namely CG2678 (a transcription factor) and pyrexia (a TRP cation channel). We also demonstrate a compensatory effect between Dis3L2 and the 5'-3' exoribonuclease Pacman demonstrating that these 2 exoribonucleases function to regulate opposing pathways within the developing tissue. This work provides the first description of the molecular and developmental consequences of Dis3L2 inactivation in a non-human animal model. The work is directly relevant to the understanding of human overgrowth syndromes such as Perlman syndrome.

摘要

在复杂生物体中,细胞增殖和凋亡需要精确调控,以便组织正常发育。细胞过度增殖会导致癌症等疾病。我们已经表明,外切核糖核酸酶Dis3L2是模式生物黑腹果蝇中自然组织增殖正确调控所必需的。Dis3L2是一个高度保守的外切核糖核酸酶家族的成员,该家族以3' - 5'方向降解RNA。我们发现,在果蝇翅成虫盘中介导Dis3L2基因敲低会导致翅显著过度生长,这是由于细胞增殖增加而非细胞大小增加所致。成虫盘在胚胎中被指定,然后进行增殖和分化以形成果蝇的成虫结构。使用RNA测序,我们鉴定出一小部分对Dis3L2活性敏感的mRNA。在那些水平升高因而可能是Dis3L2潜在靶标的mRNA中,我们鉴定出2种在转录后水平而非转录水平发生变化的mRNA,即CG2678(一种转录因子)和pyrexia(一种TRP阳离子通道)。我们还证明了Dis3L2与5' - 3'外切核糖核酸酶Pacman之间的补偿作用,表明这两种外切核糖核酸酶在发育中的组织内调节相反的途径。这项工作首次描述了在非人类动物模型中Dis3L2失活的分子和发育后果。这项工作与理解诸如佩尔曼综合征等人类过度生长综合征直接相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bce0/5207379/354c0ccc80bf/krnb-13-12-1232238-g001.jpg

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