Differential regulation of the proteome and phosphoproteome along the dorso-ventral axis of the early Drosophila embryo.

IF 6.4 1区 生物学 Q1 BIOLOGY eLife Pub Date : 2024-09-02 DOI:10.7554/eLife.99263
Juan Manuel Gomez, Hendrik Nolte, Elisabeth Vogelsang, Bipasha Dey, Michiko Takeda, Girolamo Giudice, Miriam Faxel, Theresa Haunold, Alina Cepraga, Robert P Zinzen, Marcus Krüger, Evangelia Petsalaki, Yu-Chiun Wang, Maria Leptin
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Abstract

The initially homogeneous epithelium of the early Drosophila embryo differentiates into regional subpopulations with different behaviours and physical properties that are needed for morphogenesis. The factors at top of the genetic hierarchy that control these behaviours are known, but many of their targets are not. To understand how proteins work together to mediate differential cellular activities, we studied in an unbiased manner the proteomes and phosphoproteomes of the three main cell populations along the dorso-ventral axis during gastrulation using mutant embryos that represent the different populations. We detected 6111 protein groups and 6259 phosphosites of which 3398 and 3433 were differentially regulated, respectively. The changes in phosphosite abundance did not correlate with changes in host protein abundance, showing phosphorylation to be a regulatory step during gastrulation. Hierarchical clustering of protein groups and phosphosites identified clusters that contain known fate determinants such as Doc1, Sog, Snail, and Twist. The recovery of the appropriate known marker proteins in each of the different mutants we used validated the approach, but also revealed that two mutations that both interfere with the dorsal fate pathway, Toll10B and serpin27aex do this in very different manners. Diffused network analyses within each cluster point to microtubule components as one of the main groups of regulated proteins. Functional studies on the role of microtubules provide the proof of principle that microtubules have different functions in different domains along the DV axis of the embryo.

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果蝇早期胚胎背腹轴蛋白质组和磷酸蛋白组的差异调控。
果蝇早期胚胎的上皮细胞最初是均质的,后来分化成具有不同行为和物理性质的区域亚群,这些行为和物理性质是形态发生所必需的。控制这些行为的遗传层次结构顶层因子是已知的,但它们的许多靶标并不清楚。为了了解蛋白质如何共同介导不同的细胞活动,我们使用代表不同细胞群的突变体胚胎,以无偏见的方式研究了胃形成过程中沿背腹轴三个主要细胞群的蛋白质组和磷酸化蛋白质组。我们检测到 6111 个蛋白质组和 6259 个磷酸位点,其中分别有 3398 个和 3433 个位点受到差异调控。磷酸化位点丰度的变化与宿主蛋白质丰度的变化并不相关,这表明磷酸化是胃形成过程中的一个调控步骤。蛋白质组和磷酸化位点的分层聚类确定了包含已知命运决定因子(如 Doc1、Sog、Snail 和 Twist)的聚类。在我们使用的每种不同突变体中都恢复了适当的已知标记蛋白,这验证了我们的方法,同时也揭示了两个都干扰背侧命运途径的突变体--Toll10B 和 serpin27aex--的作用方式截然不同。每个群组内的扩散网络分析表明,微管成分是受调控蛋白质的主要群组之一。对微管作用的功能研究证明,微管在胚胎 DV 轴的不同区域具有不同的功能。
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来源期刊
eLife
eLife BIOLOGY-
CiteScore
12.90
自引率
3.90%
发文量
3122
审稿时长
17 weeks
期刊介绍: eLife is a distinguished, not-for-profit, peer-reviewed open access scientific journal that specializes in the fields of biomedical and life sciences. eLife is known for its selective publication process, which includes a variety of article types such as: Research Articles: Detailed reports of original research findings. Short Reports: Concise presentations of significant findings that do not warrant a full-length research article. Tools and Resources: Descriptions of new tools, technologies, or resources that facilitate scientific research. Research Advances: Brief reports on significant scientific advancements that have immediate implications for the field. Scientific Correspondence: Short communications that comment on or provide additional information related to published articles. Review Articles: Comprehensive overviews of a specific topic or field within the life sciences.
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