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Tb3+与人类红细胞血影蛋白结合,导致构象改变和聚集。

Tb3+ binding to human erythrocyte spectrin resulting in conformation change and aggregation.

作者信息

Sun H Y, Lin H, Cao Y, Li R, Wang K, Chen R

机构信息

Inorganic Chemistry Department, Beijing Medical University, China.

出版信息

J Inorg Biochem. 1995 Jul;59(1):29-37. doi: 10.1016/0162-0134(94)00052-c.

Abstract

The Tb3+ binding to spectrin tetramer (SPT) was studied by Tb3+ fluorescence titration and CD spectra. The results indicated that the total high-affinity Tb3+ binding sites are n1 = 330, with average Kd = 3.6 x 10(-6) M. Among them, ca. 90 sites are of higher affinity and are probably more specific to Tb3+ than the remaining sites. There are 520 low affinity Tb3+ binding sites with average Kd = 1.5 x 10(-5) M. Fluorescence and CD spectra revealed that the alpha-helix content of SPT decreased with Tb3+ binding to specific sites and further binding did not result in conformation change. Tb3+ binding to SPT and the subsequent reactions were studied by employing stopped-flow fluorescence and light scattering methods. The studies demonstrate that this is a multistep reaction assembly: high-affinity terbium binding-conformation change-aggregation-low-affinity terbium binding--the second conformation change. The critical Tb3+ concentration-induced spectrin dimer (SPD) aggregation was determined with a light scattering method.

摘要

通过Tb3+荧光滴定和圆二色光谱研究了Tb3+与血影蛋白四聚体(SPT)的结合。结果表明,总的高亲和力Tb3+结合位点n1 = 330,平均解离常数Kd = 3.6×10(-6) M。其中,约90个位点具有更高的亲和力,可能比其余位点对Tb3+更具特异性。有520个低亲和力Tb3+结合位点,平均Kd = 1.5×10(-5) M。荧光和圆二色光谱显示,随着Tb3+与特定位点结合,SPT的α-螺旋含量降低,进一步结合不会导致构象变化。采用停流荧光和光散射方法研究了Tb3+与SPT的结合及后续反应。研究表明,这是一个多步反应组装过程:高亲和力铽结合-构象变化-聚集-低亲和力铽结合-第二次构象变化。用散射光法测定了临界Tb3+浓度诱导的血影蛋白二聚体(SPD)聚集。

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