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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Secondary structure, dynamics, and architecture of the p7 membrane protein from hepatitis C virus by NMR spectroscopy.
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Secondary structure, dynamics, and architecture of the p7 membrane protein from hepatitis C virus by NMR spectroscopy.

机译:通过NMR光谱分析丙型肝炎病毒p7膜蛋白的二级结构,动力学和结构。

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摘要

P7 is a small membrane protein that is essential for the infectivity of hepatitis C virus. Solution-state NMR experiments on p7 in DHPC micelles, including hydrogen/deuterium exchange, paramagnetic relaxation enhancement and bicelle 'q-titration,' demonstrate that the protein has a range of dynamic properties and distinct structural segments. These data along with residual dipolar couplings yield a secondary structure model of p7. We were able to confirm previous proposals that the protein has two transmembrane segments with a short interhelical loop containing the two basic residues K33 and R35. The 63-amino acid protein has a remarkably complex structure made up of seven identifiable sections, four of which are helical segments with different tilt angles and dynamics. A solid-state NMR two-dimensional separated local field spectrum of p7 aligned in phospholipid bilayers provided the tilt angles of two of these segments. A preliminary structural model of p7 derived from these NMR data is presented.
机译:P7是一种小的膜蛋白,对于丙型肝炎病毒的感染力至关重要。在DHPC胶束中p7上的溶液状态NMR实验,包括氢/氘交换,顺磁弛豫增强和比塞勒“ q-滴定”,证明该蛋白具有一系列动态特性和独特的结构区段。这些数据以及残留的偶极耦合产生了p7的二级结构模型。我们能够证实先前的提议,即该蛋白质具有两个跨膜区段,其螺旋间短环包含两个基本残基K33和R35。 63个氨基酸的蛋白质具有非常复杂的结构,由七个可识别的部分组成,其中四个是螺旋段,具有不同的倾斜角度和动力学。磷脂双层中排列的p7的固态NMR二维二维分离局部场谱提供了这些片段中两个片段的倾斜角。提出了由这些NMR数据得出的p7的初步结构模型。

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