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在温度可控的冷冻容器中分析蛋白质冷冻浓缩和微观偏析。

Protein freeze concentration and micro-segregation analysed in a temperature-controlled freeze container.

作者信息

Roessl Ulrich, Leitgeb Stefan, Nidetzky Bernd

机构信息

Research Center Pharmaceutical Engineering GmbH, Inffeldgasse 13, A-8010 Graz, Austria.

Institute of Biotechnology and Biochemical Engineering, Graz University of Technology, Petersgasse 12, A-8010 Graz, Austria.

出版信息

Biotechnol Rep (Amst). 2015 Mar 26;6:108-111. doi: 10.1016/j.btre.2015.03.004. eCollection 2015 Jun.

Abstract

To examine effects of varied freezing conditions on the development of spatial heterogeneity in the frozen protein solution, macroscopic freeze concentration and micro-segregation of bovine serum albumin (BSA) were investigated in a temperature-controlled 200-ml freeze container. Freezing to -40 °C promoted formation of protein concentration gradients (69-114 μg ml) in frozen samples taken from 12 different freezer positions, whereby slow freezing in 4 h or longer facilitated the evolution of strong spatial heterogeneities and caused local concentration increases by 1.15-fold relative to the initial protein concentration (100 μg ml). To visualize protein micro-segregation during phase separation, BSA was conjugated with fluorescein isothiocyanate and confocal laser scanning fluorescence microscopy was used to localize and size the freeze-concentrated protein regions. Slow freezing resulted in distinctly fewer and larger protein domains in the frozen bulk than fast freezing. Surface stress on the protein during freezing would therefore be minimized at low cooling rates; microscopic freeze concentration would however be highest under these conditions, potentially favoring protein aggregation.

摘要

为研究不同冷冻条件对冷冻蛋白质溶液中空间异质性发展的影响,在一个温度可控的200毫升冷冻容器中研究了牛血清白蛋白(BSA)的宏观冷冻浓缩和微观偏析。将样品冷冻至-40°C,促进了从12个不同冷冻位置取出的冷冻样品中蛋白质浓度梯度(69-114μg/ml)的形成,4小时或更长时间的缓慢冷冻促进了强烈空间异质性的演变,并导致局部浓度相对于初始蛋白质浓度(100μg/ml)增加1.15倍。为了观察相分离过程中的蛋白质微观偏析,将BSA与异硫氰酸荧光素偶联,并使用共聚焦激光扫描荧光显微镜对冷冻浓缩的蛋白质区域进行定位和测量。与快速冷冻相比,缓慢冷冻导致冷冻块体中蛋白质结构域明显更少、更大。因此,在低冷却速率下,冷冻过程中蛋白质上的表面应力将降至最低;然而,在这些条件下微观冷冻浓缩将最高,这可能有利于蛋白质聚集。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e91a/5466265/6343d975a6d1/gr1.jpg

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