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X-ray diffraction reveals the intrinsic difference in the physical properties of membrane and soluble proteins

机译:X射线衍射揭示了膜和可溶性蛋白质的物理性质的内在差异

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Membrane proteins are distinguished from soluble proteins by their insertion into biological membranes. This insertion is achieved via a noticeable arrangement of hydrophobic amino acids that are exposed at the surface of the protein, and renders the interaction with the aliphatic tails of lipids more energetically favorable. This important difference between these two categories of proteins is the source of the need for a specific handling of membrane proteins, which transpired in the creation of new tools for their recombinant expression, purification and even crystallization. Following this line, we show here that crystals of membrane proteins display systematically higher diffraction anisotropy than those of soluble proteins. This phenomenon dramatically hampers structure solution and refinement, and has a strong impact on the quality of electron-density maps. A farther search for origins of this phenomenon showed that the type of crystallization, and thus the crystal packing, has no impact on anisotropy, nor does the nature or function of the membrane protein. Membrane proteins fully embedded within the membrane display equal anisotropy compared to the ones with extra membranous domains or fusions with soluble proteins. Overall, these results overturn common beliefs and call for a specific handling of their diffraction data.
机译:膜蛋白与可溶性蛋白的区别在于它们插入生物膜中。这种插入是通过疏水氨基酸的显着排列而实现的,该氨基酸暴露在蛋白质表面,使与脂质的脂族尾部的相互作用更加有力。这两类蛋白质之间的这一重要区别是需要对膜蛋白进行特殊处理的原因,膜蛋白的重组产生于表达其重组表达,纯化甚至结晶的新工具。遵循这条线,我们在这里显示膜蛋白的晶体显示出比可溶性蛋白更高的衍射各向异性。这种现象极大地阻碍了结构的求解和改进,并且对电子密度图的质量产生了很大的影响。进一步寻找这种现象的根源表明,结晶的类型以及由此的晶体堆积对各向异性都没有影响,膜蛋白的性质或功能也没有影响。与具有额外膜结构域或与可溶性蛋白融合的蛋白相比,完全嵌入膜中的膜蛋白表现出相同的各向异性。总体而言,这些结果推翻了普遍的看法,并要求对其衍射数据进行特定处理。

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