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利用分子精度监测相变来观察经典成核理论的实际应用。

Observing classical nucleation theory at work by monitoring phase transitions with molecular precision.

机构信息

Structural Biology Brussels, Vrije Universiteit Brussel, Pleinlaan 2, 1050 Elsene, Belgium.

Center for Nonlinear Phenomena and Complex Systems, Université Libre de Bruxelles, Blvd. du Triomphe, 1050 Brussels, Belgium.

出版信息

Nat Commun. 2014 Dec 3;5:5598. doi: 10.1038/ncomms6598.

Abstract

It is widely accepted that many phase transitions do not follow nucleation pathways as envisaged by the classical nucleation theory. Many substances can traverse intermediate states before arriving at the stable phase. The apparent ubiquity of multi-step nucleation has made the inverse question relevant: does multistep nucleation always dominate single-step pathways? Here we provide an explicit example of the classical nucleation mechanism for a system known to exhibit the characteristics of multi-step nucleation. Molecular resolution atomic force microscopy imaging of the two-dimensional nucleation of the protein glucose isomerase demonstrates that the interior of subcritical clusters is in the same state as the crystalline bulk phase. Our data show that despite having all the characteristics typically associated with rich phase behaviour, glucose isomerase 2D crystals are formed classically. These observations illustrate the resurfacing importance of the classical nucleation theory by re-validating some of the key assumptions that have been recently questioned.

摘要

人们普遍认为,许多相变并不遵循经典成核理论所设想的成核途径。许多物质在到达稳定相之前可以穿过中间状态。多步成核的明显普遍性使得反向问题变得相关:多步成核是否总是主导单步途径?在这里,我们提供了一个已知表现出多步成核特征的系统的经典成核机制的明确示例。通过分子分辨率原子力显微镜对蛋白质葡萄糖异构酶二维成核的成像表明,亚临界团簇的内部与晶体块状相处于相同状态。我们的数据表明,尽管具有与丰富的相行为相关的所有特征,但葡萄糖异构酶二维晶体仍以经典方式形成。这些观察结果通过重新验证最近受到质疑的一些关键假设,说明了经典成核理论的重新出现的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f800/4268696/dc057bf1e289/ncomms6598-f1.jpg

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