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Mechanisms kinetics impurities and defects: consequences in macromolecular crystallization

机译:机理动力学杂质和缺陷:大分子结晶的后果

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摘要

The nucleation and growth of protein, nucleic acid and virus crystals from solution are functions of underlying kinetic and thermodynamic parameters that govern the process, and these are all supersaturation-dependent. While the mechanisms of macromolecular crystal growth are essentially the same as for conventional crystals, the underlying parameters are vastly different, in some cases orders of magnitude lower, and this produces very different crystallization processes. Numerous physical features of macromolecular crystals are of serious interest to X-ray diffractionists; the resolution limit and mosaicity, for example, reflect the degree of molecular and lattice order. The defect structure of crystals has an impact on their response to flash-cooling, and terminal crystal size is dependent on impurity absorption and incorporation. The variety and extent of these issues are further unique to crystals of biological macromolecules. All of these features are amenable to study using atomic force microscopy, which provides direct images at the nanoscale level. Some of those images are presented here.
机译:溶液中蛋白质,核酸和病毒晶体的成核和生长是控制该过程的基本动力学和热力学参数的函数,并且这些都是超饱和依赖性的。尽管大分子晶体生长的机理与常规晶体基本相同,但基本参数却大不相同,在某些情况下降低了几个数量级,从而产生了截然不同的结晶过程。大分子晶体的许多物理特征是X射线衍射学家们非常关注的。例如,分辨率极限和镶嵌度反映了分子和晶格有序的程度。晶体的缺陷结构会影响其对快速冷却的响应,并且最终晶体的大小取决于杂质的吸收和结合。这些问题的多样性和程度是生物大分子晶体所独有的。所有这些功能都适合使用原子力显微镜进行研究,该技术可提供纳米级的直接图像。这些图像中的一些在此处显示。

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