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细菌中转录调控因子-DNA 相互作用的记忆效应。

Memory effects of transcription regulator-DNA interactions in bacteria.

机构信息

Department of Chemistry and Chemical Biology, Cornell University, Ithaca, NY 14853.

Department of Chemistry and Chemical Biology, Harvard University, Cambridge, MA 02138.

出版信息

Proc Natl Acad Sci U S A. 2024 Oct 8;121(41):e2407647121. doi: 10.1073/pnas.2407647121. Epub 2024 Oct 3.

Abstract

Memory effect refers to the phenomenon where past events influence a system's current and future states or behaviors. In biology, memory effects often arise from intra- or intermolecular interactions, leading to temporally correlated behaviors. Single-molecule studies have shown that enzymes and DNA-binding proteins can exhibit time-correlated behaviors of their activity. While memory effects are well documented and studied in vitro, no such examples exist in cells to our knowledge. Combining single-molecule tracking (SMT) and single-cell protein quantitation, we find in living cells distinct temporal correlations in the binding/unbinding events on DNA by MerR- and Fur-family metalloregulators, manifesting as memory effects with timescales of ~1 s. These memory effects persist irrespective of the type of the metalloregulators or their metallation states. Moreover, these temporal correlations of metalloregulator-DNA interactions are associated with spatial confinements of the metalloregulators near their DNA binding sites, suggesting microdomains of ~100 nm in size that possibly result from the spatial organizations of the bacterial chromosome without the involvement of membranes. These microdomains likely facilitate repeated binding events, enhancing regulator-DNA contact frequency and potentially gene regulation efficiency. These findings provide unique insights into the spatiotemporal dynamics of protein-DNA interactions in bacterial cells, introducing the concept of microdomains as a crucial player in memory effect-driven gene regulation.

摘要

记忆效应是指过去的事件影响系统当前和未来状态或行为的现象。在生物学中,记忆效应通常源于分子内或分子间的相互作用,导致时间相关的行为。单分子研究表明,酶和 DNA 结合蛋白可以表现出与其活性相关的时间相关性行为。虽然记忆效应在体外得到了很好的记录和研究,但据我们所知,在细胞中没有这样的例子。我们结合单分子追踪(SMT)和单细胞蛋白定量,在活细胞中发现 MerR 和 Fur 家族金属调控蛋白在 DNA 上的结合/解吸事件存在明显的时间相关性,表现为具有 ~1 s 时间尺度的记忆效应。这些记忆效应与金属调控蛋白的类型或其金属化状态无关。此外,这些金属调控蛋白-DNA 相互作用的时间相关性与金属调控蛋白在其 DNA 结合位点附近的空间限制有关,这表明存在大小约为 100nm 的微区,可能是由细菌染色体的空间组织而产生的,而不涉及膜。这些微区可能促进了重复的结合事件,增加了调控蛋白-DNA 的接触频率,并可能提高基因调控效率。这些发现为细菌细胞中蛋白质-DNA 相互作用的时空动态提供了独特的见解,引入了微区作为记忆效应驱动基因调控的关键因素的概念。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0ef7/11474097/0cc042b2194e/pnas.2407647121fig01.jpg

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