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Ice Growth Inhibition in Antifreeze Polypeptide Solution by Short-Time Solution Preheating

机译:短时溶液预热抑制防冻多肽溶液中的冰生长

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摘要

The objective of this study is to enhance the inhibition of ice growth in the aqueous solution of a polypeptide, which is inspired by winter flounder antifreeze protein. We carried out measurements on unidirectional freezing of the polypeptide solution. The thickness of the solution was 0.02 mm, and the concentration of polypeptide was varied from 0 to 2 mg/mL. We captured successive microscopic images of ice/solution interfaces, and measured the interface velocity from the locations of tips of the pectinate interface in the images. We also simultaneously measured the temperature by using a small thermocouple. The ice/solution interface temperature was defined by the temperature at the tips. It was found that the interface temperature was decreased with an increasing concentration of polypeptide. To try varying the activity of the polypeptide, we preheated the polypeptide solution and cooled it before carrying out the measurements. Preheating for 1–5 hours was found to cause a further decrease in the interface temperature. Furthermore, wider regions of solution and ice with inclined interfaces in the pectinate interface structure were observed, compared with the case where the solution was not preheated. Thus, the ice growth inhibition was enhanced by this preheating. To investigate the reason for this enhancement, we measured the conformation and aggregates of polypeptide in the solution. We also measured the local concentration of polypeptide. It was found that the polypeptide aggregates became larger as a result of preheating, although the polypeptide conformation was unchanged. These large aggregates caused both adsorption to the interface and the wide regions of supercooled solution in the pectinate interface structure.
机译:这项研究的目的是增强多肽水溶液中冰的抑制作用,这受冬季比目鱼抗冻蛋白的启发。我们对多肽溶液的单向冷冻进行了测量。溶液的厚度为0.02mm,并且多肽的浓度在0至2mg / mL之间变化。我们捕获了冰/溶液界面的连续显微图像,并从图像中果胶状界面的尖端位置测量了界面速度。我们还使用小型热电偶同时测量了温度。冰/溶液界面温度由尖端温度定义。已经发现,界面温度随着多肽浓度的增加而降低。为了尝试改变多肽的活性,我们在进行测量之前将多肽溶液预热并冷却。发现预热1-5小时会导致界面温度进一步降低。此外,与未预热溶液的情况相比,观察到了在果胶状界面结构中具有倾斜界面的溶液和冰的较宽区域。因此,通过该预热增强了冰的生长抑制。为了研究这种增强的原因,我们测量了溶液中多肽的构象和聚集体。我们还测量了多肽的局部浓度。发现多肽聚集体由于预热而变大,尽管多肽构象没有改变。这些大的聚集体引起对果胶酸盐界面结构中界面的吸附以及过冷溶液的宽区域。

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