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Differences in the Effects of Solution Additives on Heat- and Refolding-Induced Aggregation

机译:溶液添加剂对热和折叠诱导聚集的影响差异

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Although a number of low-molecular-weight additives have been developed to suppress protein aggregation, it is unclear whether these aggregation suppressors affect various aggregation processes in the same manner. In this study, we evaluated the differences in the effect of solution additives on heat- and refolding-induced aggregation in the presence of guanidine (Gdn), arginine (Arg), and spermidine (Spd), and the comparable analysis showed the following differences: (i) Gdn did not suppress thermal aggregation but increased the yield of oxidative refolding, (ii) Spd showed the highest effect for heat-induced aggregation suppression among tested compounds, although it promoted aggregation in oxidative refolding, (iii) Arg was effective for both aggregation processes. Lysozyme solubility assay and thermal unfolding experiment showed that Spd was preferentially excluded from native lysozyme and Arg and Gdn solubilized the model state of intermediates during oxidative refolding. This preference of additives to protein surfaces is the cause of the different effect on aggregation suppression.
机译:尽管已经开发了许多低分子量添加剂来抑制蛋白质聚集,但是不清楚这些聚集抑制剂是否以相同的方式影响各种聚集过程。在这项研究中,我们评估了在存在胍(Gdn),精氨酸(Arg)和亚精胺(Spd)的情况下溶液添加剂对热和折叠诱导聚集的影响的差异,可比分析表明以下差异:(i)Gdn不会抑制热聚集,但会增加氧化重折叠的产量;(ii)Spd对受热诱导的聚集抑制作用在受试化合物中显示出最高的抑制作用,尽管它能促进氧化重折叠中的聚集,(iii)Arg有效对于两个聚合过程。溶菌酶溶解度测定和热解折叠实验表明,Spd优先从天然溶菌酶中排除,Arg和Gdn溶解了中间体在氧化重折叠过程中的模型状态。添加剂对蛋白质表面的偏爱是导致聚集抑制作用不同的原因。

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