化学
生物物理学
变性(裂变材料)
蛋白质稳定性
蛋白质聚集
蛋白质折叠
磷酸甘油酸激酶
高分子拥挤
热稳定性
绿色荧光蛋白
蛋白质工程
生物化学
酶
生物
有机化学
基因
高分子
核化学
作者
R. Chang,Martin Gruebele,Deborah Leckband
出处
期刊:Biomacromolecules
[American Chemical Society]
日期:2022-09-02
卷期号:23 (10): 4063-4073
被引量:6
标识
DOI:10.1021/acs.biomac.2c00297
摘要
Polymers designed to stabilize proteins exploit direct interactions or crowding, but mechanisms underlying increased stability or reduced aggregation are rarely established. Alginate is widely used to encapsulate proteins for drug delivery and tissue regeneration despite limited knowledge of its impact on protein stability. Here, we present evidence that alginate can both increase protein folding stability and suppress the aggregation of unfolded protein through direct interactions without crowding. We used a fluorescence-based conformational reporter of two proteins, the metabolic protein phosphoglycerate kinase (PGK) and the hPin1 WW domain to monitor protein stability and aggregation as a function of temperature and the weight percent of alginate in solution. Alginate stabilizes PGK by up to 14.5 °C, but stabilization is highly protein-dependent, and the much smaller WW domain is stabilized by only 3.5 °C against thermal denaturation. Stabilization is greatest at low alginate weight percent and decreases at higher alginate concentrations. This trend cannot be explained by crowding, and ionic screening suggests that alginate stabilizes proteins through direct interactions with a significant electrostatic component. Alginate also strongly suppresses aggregation at high temperature by irreversibly associating with unfolded proteins and preventing refolding. Both the beneficial and negative impacts of alginate on protein stability and aggregation have important implications for practical applications.
科研通智能强力驱动
Strongly Powered by AbleSci AI