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Towards physiological complexity with in vitro single-molecule biophysics

机译:利用体外单分子生物物理学解决生理复杂性

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摘要

Single-molecule biology has matured in recent years, driven to greater sophistication by the development of increasingly advanced experimental techniques. A progressive appreciation for its unique strengths is attracting research that spans an exceptionally broad swath of physiological phenomena—from the function of nucleosomes to protein diffusion in the cell membrane. Newfound enthusiasm notwithstanding, the single-molecule approach is limited to an intrinsically defined set of biological questions; such limitation applies to all experimental approaches, and an explicit statement of the boundaries delineating each set offers a guide to most fruitfully orienting in vitro single-molecule research in the future. Here, we briefly describe a simple conceptual framework to categorize how submolecular, molecular and intracellular processes are studied. We highlight the domain of single-molecule biology in this scheme, with an emphasis on its ability to probe various forms of heterogeneity inherent to populations of discrete biological macromolecules. We then give a general overview of our high-throughput DNA curtain methodology for studying protein–nucleic acid interactions, and by contextualizing it within this framework, we explore what might be the most enticing avenues of future research. We anticipate that a focus on single-molecule biology's unique strengths will suggest a new generation of experiments with greater complexity and more immediately translatable physiological relevance.
机译:近年来,随着越来越先进的实验技术的发展,单分子生物学已日趋成熟。人们逐渐意识到它的独特优势,从而吸引了广泛的生理现象研究,从核小体的功能到蛋白质在细胞膜中的扩散。尽管有新发现的热情,但单分子方法仅限于一组固有定义的生物学问题。这种局限性适用于所有实验方法,并且明确描述每组边界的方法为将来最有效地定向体外单分子研究提供了指南。在这里,我们简要描述一个简单的概念框架,以对如何研究亚分子,分子和细胞内过程进行分类。我们在此方案中重点介绍了单分子生物学的领域,重点是其探测离散生物大分子种群固有的各种形式的异质性的能力。然后,我们概述了用于研究蛋白质-核酸相互作用的高通量DNA幕布方法,并通过在此框架内对其进行了背景研究,探索了未来研究中最诱人的途径。我们预计,关注单分子生物学的独特优势将提示新一代实验,具有更高的复杂性和更直接的生理相关性。

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