用于果蝇 TGF-β/BMP 信号研究的基因组工程工具集。

IF 3.7 2区生物学 Q1 DEVELOPMENTAL BIOLOGY

Development Pub Date : 2024-11-04 DOI:10.1242/dev.204222

Clara-Maria Ell, Abu Safyan, Mrinal Chayengia, Manuela M M Kustermann, Jennifer Lorenz, Melanie Schächtle, George Pyrowolakis

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引用次数: 0

摘要

TGF-β/BMP 超家族配体在生长、模式化和器官形成的调控中发挥着关键作用，并可作为长程形态发生因子。要了解 TGF-β/BMP 信号动态和调控，关键是要有能监测和操纵以生理水平和内源性时空模式表达的通路成分的工具。我们利用基因组工程生成了一个全面的内源表位或荧光标记的受体、共受体、转录因子以及果蝇 BMP 和 Activin 信号通路的关键反馈调节因子库。我们证明所生成的等位基因具有生物活性，可用于评估相应蛋白质的组织和亚细胞分布。此外，我们还展示了基因组平台可用于基因座结构-功能和顺式调控分析。最后，我们还介绍了一套基于蛋白质粘合剂的补充工具，它可以对表位标记蛋白质的稳定性和亚细胞定位进行可视化操作，为 BMP 信号转导及其他分析提供了新的工具。

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A genome engineered tool set for Drosophila TGF-β/BMP signaling studies.

Ligands of the TGF-β/BMP superfamily are critically involved in the regulation of growth, patterning and organogenesis and can act as long-range morphogens. Essential for understanding TGF-β/BMP signaling dynamics and regulation are tools that allow monitoring and manipulating pathway components expressed at physiological levels and endogenous spatiotemporal patterns. We used genome engineering to generate a comprehensive library of endogenously epitope- or fluorescently-tagged versions of receptors, co-receptors, transcription factors and key feedback regulators of the Drosophila BMP and Activin signaling pathways. We demonstrate that the generated alleles are biologically active and can be utilized for assessing tissue and subcellular distribution of the corresponding proteins. Further, we show that the genomic platforms can be used for in locus structure-function and cis-regulatory analyses. Finally, we present a complementary set of protein binder-based tools, which allow visualization as well as manipulation of the stability and subcellular localization of epitope-tagged proteins, providing new tools for the analysis of BMP signaling and beyond.

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来源期刊

Development 生物-发育生物学

CiteScore

6.70

自引率

4.30%

发文量

433

审稿时长

3 months

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