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首页> 外文期刊>Journal of Physics. Condensed Matter >Surfactant-induced protein unfolding as studied by small-angle neutron scattering and dynamic light scattering
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Surfactant-induced protein unfolding as studied by small-angle neutron scattering and dynamic light scattering

机译:通过小角度中子散射和动态光散射研究表面活性剂诱导的蛋白质展开

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The structural changes of protein bovine serum albumin ( BSA) during its unfolding on the addition of anionic surfactant sodium dodecyl sulfate ( SDS) have been studied using small-angle neutron scattering ( SANS) and dynamic light scattering (DLS). It is observed that at small surfactant concentrations, individual surfactant molecules bind to the protein, increasing the size of the protein. On the other hand, surfactant molecules at higher concentrations aggregate to form micelle-like clusters along the unfolded polypeptide chains of the protein. SANS data indicates the formation of a fractal structure representing a necklace model of micelle-like clusters randomly distributed along the polypeptide chain. The overall size of the complex increases and the fractal dimension decreases on increasing the surfactant concentration. The size of the micelle-like clusters does not show any change, while the number of such micelle-like clusters in protein-surfactant complexes increases with the surfactant concentration. The conformation of the unfolded protein has been determined directly using contrast variation SANS measurements by contrast matching the surfactant to the medium. It is found that the protein acquires a random coil Gaussian conformation on unfolding, with its radius of gyration increasing with an increase in surfactant concentration. The results of DLS measurements are found to be in good agreement with those obtained using SANS.
机译:使用小角度中子散射(SANS)和动态光散射(DLS)研究了添加牛磺酸阴离子表面活性剂十二烷基硫酸钠(SDS)后蛋白质牛血清白蛋白(BSA)展开过程中的结构变化。观察到在低表面活性剂浓度下,单独的表面活性剂分子与蛋白质结合,从而增加了蛋白质的大小。另一方面,较高浓度的表面活性剂分子聚集在一起,沿着蛋白质的未折叠多肽链形成胶束状簇。 SANS数据表明分形结构的形成,该分形结构代表了沿多肽链随机分布的胶束状簇的项链模型。随着表面活性剂浓度的增加,络合物的总尺寸增加,分形维数减小。胶束状簇的大小没有任何变化,而蛋白质表面活性剂复合物中此类胶束状簇的数目随表面活性剂浓度的增加而增加。已通过使用对比度变化SANS测量,通过将表面活性剂与介质进行对比匹配,直接确定了未折叠蛋白的构象。发现该蛋白质在展开时获得随机的线圈高斯构象,其旋转半径随表面活性剂浓度的增加而增加。发现DLS测量的结果与使用SANS获得的结果非常一致。

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