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两亲性共聚物比聚乙二醇更有效地减少未折叠溶菌酶的聚集。

Amphiphilic copolymers reduce aggregation of unfolded lysozyme more effectively than polyethylene glycol.

作者信息

Chin Jaemin, Mustafi Devkumar, Poellmann Michael J, Lee Raphael C

机构信息

Departments of Surgery, The University of Chicago, Chicago, IL 60637, United States of America.

出版信息

Phys Biol. 2017 Feb 8;14(1):016003. doi: 10.1088/1478-3975/aa5788.

Abstract

Certain amphiphilic block copolymers are known to prevent aggregation of unfolded proteins. To better understand the mechanism of this effect, the optical properties of heat-denatured and dithiothreitol reduced lysozyme were evaluated with respect to controls using UV-Vis spectroscopy, transmission electron microscopy (TEM) and circular dichroism (CD) measurements. Then, the effects of adding Polyethylene Glycol (8000 Da), the triblock surfactant Poloxamer 188 (P188), and the tetrablock copolymer Tetronic 1107 (T1107) to the lysozyme solution were compared. Overall, T1107 was found to be more effective than P188 in inhibiting aggregation, while PEG exhibited no efficacy. TEM imaging of heat-denatured and reduced lysozymes revealed spherical aggregates with on average 250-450 nm diameter. Using CD, more soluble lysozyme was recovered with T1107 than P188 with β-sheet secondary structure. The greater effectiveness of the larger T1107 in preventing aggregation of unfolded lysozyme than the smaller P188 and PEG points to steric hindrance at play; signifying the importance of size match between the hydrophobic region of denatured protein and that of amphiphilic copolymers. Thus, our results corroborate that certain multi-block copolymers are effective in preventing heat-induced aggregation of reduced lysozymes and future studies warrant more detailed focus on specific applications of these copolymers.

摘要

已知某些两亲性嵌段共聚物可防止未折叠蛋白质聚集。为了更好地理解这种作用的机制,利用紫外可见光谱、透射电子显微镜(TEM)和圆二色性(CD)测量,针对对照评估了热变性和二硫苏糖醇还原的溶菌酶的光学性质。然后,比较了向溶菌酶溶液中添加聚乙二醇(8000 Da)、三嵌段表面活性剂泊洛沙姆188(P188)和四嵌段共聚物Tetronic 1107(T1107)的效果。总体而言,发现T1107在抑制聚集方面比P188更有效,而PEG没有效果。热变性和还原溶菌酶的TEM成像显示平均直径为250 - 450 nm的球形聚集体。使用CD,与具有β - 折叠二级结构的P188相比,T1107回收的可溶性溶菌酶更多。较大的T1107在防止未折叠溶菌酶聚集方面比较小的P188和PEG更有效,这表明存在空间位阻作用;这意味着变性蛋白质的疏水区域与两亲性共聚物的疏水区域之间尺寸匹配的重要性。因此,我们的结果证实某些多嵌段共聚物可有效防止还原溶菌酶的热诱导聚集,未来的研究需要更详细地关注这些共聚物的具体应用。

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