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利用活性液滴调控核酸催化。

Regulating Nucleic Acid Catalysis Using Active Droplets.

机构信息

Department of Bioscience, School of Natural Sciences, Technical University of Munich, Lichtenbergstrasse 4, 85748, Garching, Germany.

Department of Chemistry and Chemical Biology, TU Dortmund University, Otto-Hahn-Strasse 4a, 44227, Dortmund, Germany.

出版信息

Angew Chem Int Ed Engl. 2024 Nov 18;63(47):e202412534. doi: 10.1002/anie.202412534. Epub 2024 Oct 15.

Abstract

Cells use transient membraneless organelles to regulate biological reaction networks. For example, stress granules selectively store mRNA to downregulate protein expression in response to heat or oxidative stress. Models mimicking this active behavior should be established to better understand in vivo regulation involving compartmentalization. Here we use active, complex coacervate droplets as a model for membraneless organelles to spatiotemporally control the activity of a catalytic DNA (DNAzyme). Upon partitioning into these peptide-RNA droplets, the DNAzyme unfolds and loses its ability to catalyze the cleavage of a nucleic acid strand. We can transiently pause the DNAzyme activity upon inducing droplet formation with fuel. After fuel consumption, the DNAzyme activity autonomously restarts. We envision this system could be used to up and downregulate multiple reactions in a network, helping understand the complexity of a cell's pathways. By creating a network where the DNAzyme could reciprocally regulate the droplet properties, we would have a powerful tool for engineering synthetic cells.

摘要

细胞利用瞬时无膜细胞器来调节生物反应网络。例如,应激颗粒选择性地储存 mRNA,以响应热或氧化应激下调蛋白质表达。应该建立模拟这种主动行为的模型,以更好地理解涉及区隔化的体内调控。在这里,我们使用活性的、复杂的凝聚液滴作为无膜细胞器的模型,来时空控制催化 DNA(DNA 酶)的活性。在分配到这些肽-RNA 液滴后,DNA 酶展开并失去催化核酸链切割的能力。我们可以通过用燃料诱导液滴形成来暂时暂停 DNA 酶的活性。燃料消耗后,DNA 酶活性会自动重新开始。我们设想这个系统可以用于上调和下调网络中的多个反应,帮助理解细胞途径的复杂性。通过创建一个 DNA 酶可以相互调节液滴特性的网络,我们将拥有一个用于工程合成细胞的强大工具。

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