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靶向基因修饰筛选将 SWI2/SNF2 蛋白级联与果蝇生长和自噬基因联系起来。

A targeted genetic modifier screen links the SWI2/SNF2 protein domino to growth and autophagy genes in Drosophila melanogaster.

机构信息

Biology Department, Emory University, Atlanta, Georgia 30322, USA.

出版信息

G3 (Bethesda). 2013 May 20;3(5):815-25. doi: 10.1534/g3.112.005496.

Abstract

Targeted genetic studies can facilitate phenotypic analyses and provide important insights into development and other complex processes. The SWI2/SNF2 DNA-dependent ATPase Domino (Dom) of Drosophila melanogaster, a component of the Tip60 acetyltransferase complex, has been associated with a wide spectrum of cellular processes at multiple developmental stages. These include hematopoiesis, cell proliferation, homeotic gene regulation, histone exchange during DNA repair, and Notch signaling. To explore the wider gene network associated with Dom action, we used RNAi directed against domino (dom) to mediate loss-of-function at the wing margin, a tissue that is readily scored for phenotypic changes. Dom RNAi driven through GAL4-UAS elicited dominant wing nicking that responded phenotypically to the dose of dom and other loci known to function with dom. We screened for phenotypic modifiers of this wing phenotype among 2500 transpositions of the EP P element and found both enhancers and suppressors. Several classes of modifier were obtained, including those encoding transcription factors, RNA regulatory proteins, and factors that regulate cell growth, proliferation and autophagy, a lysosomal degradation pathway that affects cell growth under conditions of starvation and stress. Our analysis is consistent with prior studies, suggesting that Dom acts pleiotropically as a positive effector of Notch signaling and a repressor of proliferation. This genetic system should facilitate screens for additional loci associated with Dom function, and complement biochemical approaches to their regulatory activity.

摘要

靶向基因研究可以促进表型分析,并为发育和其他复杂过程提供重要的见解。果蝇的 SWI2/SNF2 DNA 依赖性 ATP 酶 Domino(Dom)是 Tip60 乙酰转移酶复合物的一个组成部分,与多个发育阶段的多种细胞过程有关。这些过程包括造血、细胞增殖、同源基因调控、DNA 修复过程中的组蛋白交换以及 Notch 信号传导。为了探索与 Dom 作用相关的更广泛的基因网络,我们使用针对 domino(dom)的 RNAi 介导在翅膀边缘产生功能丧失,翅膀边缘是一个易于评分表型变化的组织。通过 GAL4-UAS 驱动的 Dom RNAi 引发显性翅膀缺口,该缺口对 dom 的剂量和其他已知与 dom 一起起作用的基因座表现出表型反应。我们在 EP P 元件的 2500 次转座中筛选了这种翅膀表型的表型修饰因子,发现了增强子和抑制剂。获得了几类修饰因子,包括编码转录因子、RNA 调节蛋白以及调节细胞生长、增殖和自噬的因子,自噬是一种溶酶体降解途径,在饥饿和应激条件下影响细胞生长。我们的分析与先前的研究一致,表明 Dom 作为 Notch 信号的正向效应子和增殖的抑制剂发挥多效性。这种遗传系统应该有助于筛选与 Dom 功能相关的其他基因座,并补充对其调节活性的生化方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/01e5/3656729/d8e75147db5f/815f1.jpg

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