首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >Determining intramolecular binding sites on surface-bound von Willebrand factor under aqueous conditions.
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Determining intramolecular binding sites on surface-bound von Willebrand factor under aqueous conditions.

机译:在水性条件下测定表面结合的von Willebrand因子上的分子内结合位点。

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The results described in this report demonstrate the feasibility of using AFM in combination with immuno-gold labeling to investigate the accessibility of various binding sites on vWF and to localize the binding site within a vWF multimer. With the aid of monoclonal antibodies [5, 11 and 23] it should be possible to use this approach to perform a quantitative assessment of the differential accessibility of various binding sites on vWF. This should allow localization and quantification of binding sites within the observed tertiary structure of the vWF, providing a measure of the accessibility, a point of reference with which the tertiary structure of vWF could be correlated to the primary sequence, and a means to determine the structural features of the antibody binding regions under physiologic buffer conditions. There are a number of obvious questions that are not addressed here: The role of different biologic and artificial surfaces; time-dependent effects; vWF orientation with respect to different thrombogenic surfaces; and the location of critical binding sites, such as for platelet GPIalpha and GPIIb-IIIa binding regions in the hydrated tertiary structure of vWF. Nevertheless, the work described in this report provides essential groundwork that should provide a novel basis on which to explore the molecular steps, both structural and functional, of vWF in thrombus development. In a wider sense, this experimental approach is applicable to structure-function studies on a wide variety of proteins in physiologic environments.
机译:本报告中描述的结果证明了结合使用AFM和免疫金标记来研究vWF上各种结合位点的可及性并在vWF多聚体中定位结合位点的可行性。借助于单克隆抗体[5、11和23],应该有可能使用这种方法对vWF上各种结合位点的差异可及性进行定量评估。这应允许在vWF的三级结构内对结合位点进行定位和定量,提供可及性的量度,vWF的三级结构可以与一级序列相关的参考点,以及确定vWF三级结构的方法。生理缓冲条件下抗体结合区的结构特征。这里有许多明显的问题没有解决:不同的生物和人造表面的作用;时间依赖性效应; vWF相对于不同血栓形成表面的取向;以及关键结合位点的位置,例如vWF的水合三级结构中的血小板GPIalpha和GPIIb-IIIa结合区。然而,本报告中描述的工作提供了必要的基础,应为探索血栓形成中vWF的分子步骤(结构和功能)提供新的基础。从广义上讲,这种实验方法适用于生理环境中各种蛋白质的结构功能研究。

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