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Binary control of enzymatic cleavage of DNA origami by structural antideterminants

机译:结构反术治疗DNA折聚物的酶促切割的二元控制

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Controlling DNA nanostructure interaction with protein is essential in developing nanodevices with programmable function, reactivity, and stability for biological and medical applications. Here, we show that the sequence-specific action of restriction endonucleases towards sharp triangular or rectangular DNA origami exhibits a novel, binary 'on/off' behaviour, as canonical recognition sites are either essentially fully reactive, or strongly resistant to enzymatic cutting. Moreover, introduction of structural defects in the sharp triangle can activate an otherwise unreactive site, with a site-to-defect distance of similar to 50 nm. We argue that site reactivity is dependent upon programmable, mechanical coupling in the two-dimensional DNA origami, with specific structural elements, including DNA nicks and branches proximal to the sites that can function as negative(anti) determinants of reactivity. Empirically modelling the constraints to DNA degrees of freedom associated with each recognition site in the sharp triangle can rationalize the pattern of suppressed reactivity towards nine restriction endonucleases, in substantial agreement with the experimental results. These results provide a basis for a predictive understanding of structure-reactivity correlates of specific DNA nanostructures, which will allow a better understanding of the behaviour of nucleic acids under nanoscale confinement, as well as in the rational design of func-tional nanodevices based on self-assembling nucleic acids.
机译:控制与蛋白质的DNA纳米结构相互作用在开发具有可编程功能,反应性和生物和医疗应用稳定性的纳米型中是必需的。在这里,我们表明,朝向尖锐三角形或矩形DNA折纸的限制性内切核酸酶的序列特异性作用表现出一种新颖的二进制'ON / OFF'行为,因为规范识别位点是基本完全反应的,或强烈耐酶切割。此外,尖锐三角形中的结构缺陷引入可以激活否则不合适的部位,其位点缺陷距离与50nm相似。我们认为,现场反应性取决于二维DNA折纸中的可编程机械耦合,具有特定的结构元素,包括近端的DNA缺口和分支,该位点可以用作反应性的负(抗)决定簇。经验模拟与夏始三角形中的每个识别部位相关的DNA自由度的约束可以使抑制反应性的模式与九个限制性内切核酸酶的模式合理化,以实际协议与实验结果很重要。这些结果为特定DNA纳米结构的结构反应性相关的预测理解提供了基础,这将允许更好地理解纳米级限制下的核酸的行为,以及基于自我的核心纳米纳米型的合理设计 - 合理的核酸。

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