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毛细管等电聚焦——重现性与蛋白质吸附

Capillary isoelectric focusing--reproducibility and protein adsorption.

作者信息

Graf Michael, Wätzig Hermann

机构信息

Institute of Pharmacy, TU Braunschweig, Braunschweig, Germany.

出版信息

Electrophoresis. 2004 Sep;25(17):2959-64. doi: 10.1002/elps.200305978.

Abstract

Capillary isoelectric focusing (CIEF) is an important tool for the quality assurance of biotechnologically maintained drugs and for proteome analysis. The critical performance parameters of this technique are the precisions of isoelectric point (pI) values and peak areas. Compared to capillary zone electrophoresis (CZE), where precise results can be obtained (e.g., 0.5% relative standard deviation (RSD) for peak areas, n = 60), only few data are available for CIEF experiments. So far, reproducible data of pI values (RSD = 0.5%) have been acquired, but peak areas show inferior results (about 3-15% RSD). Nonstable capillary coatings and protein adsorption have been discussed as possible reasons. Recent work of Righetti et al. [25, 27] has proven that the use of coated capillaries can reduce the adsorption of proteins by 50% but cannot prevent it. In our CIEF experiments irregular and poorly reproducible peak patterns have been observed. In a long-time experiment of 106 repeated runs, an overall RSD of 10% was obtained for peak areas, RSD of 2% only in series of about 10 consecutive replicates. Especially at higher concentrations the reproducibility deteriorates. This seems to be the result of a self-amplifying process, induced by adsorbed protein molecules, leading to further agglomerations. CZE control experiments in linear polyacrylamide (LPA)-coated capillaries proved a strong pH dependency of these effects within a small range. Compared to bare fused-silica surfaces, adsorption effects are reduced but not inhibited. An enhancement of reproducibility in CIEF experiments can be achieved only by controlling the interactions of proteins and capillary walls.

摘要

毛细管等电聚焦(CIEF)是用于生物技术维持药物质量保证和蛋白质组分析的重要工具。该技术的关键性能参数是等电点(pI)值和峰面积的精密度。与毛细管区带电泳(CZE)相比,CZE能获得精确的结果(例如,峰面积的相对标准偏差(RSD)为0.5%,n = 60),而关于CIEF实验的数据却很少。到目前为止,已获得了可重复的pI值数据(RSD = 0.5%),但峰面积的结果较差(约3 - 15% RSD)。不稳定的毛细管涂层和蛋白质吸附被认为是可能的原因。里盖蒂等人[25, 27]最近的研究证明,使用涂层毛细管可使蛋白质吸附减少50%,但无法防止吸附。在我们的CIEF实验中,观察到了不规则且重现性差的峰形。在106次重复运行的长期实验中,峰面积的总体RSD为10%,仅在约10次连续重复的系列中RSD为2%。特别是在较高浓度下,重现性会变差。这似乎是由吸附的蛋白质分子诱导的自放大过程导致进一步聚集的结果。在线性聚丙烯酰胺(LPA)涂层毛细管中的CZE对照实验证明,在小范围内这些效应具有很强的pH依赖性。与裸露的熔融石英表面相比,吸附效应有所降低,但并未受到抑制。只有通过控制蛋白质与毛细管壁之间的相互作用,才能提高CIEF实验的重现性。

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