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鲎血蓝蛋白:10埃冷冻电镜结构、序列分析、分子建模和刚体拟合揭示了八个六聚体之间的界面。

Limulus polyphemus hemocyanin: 10 A cryo-EM structure, sequence analysis, molecular modelling and rigid-body fitting reveal the interfaces between the eight hexamers.

作者信息

Martin Andreas G, Depoix Frank, Stohr Michael, Meissner Ulrich, Hagner-Holler Silke, Hammouti Kada, Burmester Thorsten, Heyd Jochen, Wriggers Willy, Markl Jürgen

机构信息

Institute of Zoology, Johannes Gutenberg University, D-55099 Mainz, Germany.

出版信息

J Mol Biol. 2007 Mar 2;366(4):1332-50. doi: 10.1016/j.jmb.2006.11.075. Epub 2006 Dec 1.

Abstract

The blue copper protein hemocyanin from the horseshoe crab Limulus polyphemus is among the largest respiratory proteins found in nature (3.5 MDa) and exhibits a highly cooperative oxygen binding. Its 48 subunits are arranged as eight hexamers (1x6mers) that form the native 8x6mer in a nested hierarchy of 2x6mers and 4x6mers. This quaternary structure is established by eight subunit types (termed I, IIA, II, IIIA, IIIB, IV, V, and VI), of which only type II has been sequenced. Crystal structures of the 1x6mer are available, but for the 8x6mer only a 40 A 3D reconstruction exists. Consequently, the structural parameters of the 8x6mer are not firmly established, and the molecular interfaces between the eight hexamers are still to be defined. This, however, is crucial for understanding how allosteric transitions are mediated between the different levels of hierarchy. Here, we show the 10 A structure (FSC(1/2-bit) criterion) of the oxygenated 8x6mer from cryo-electron microscopy (cryo-EM) and single-particle analysis. Moreover, we show its molecular model as obtained by DNA sequencing of subunits II, IIIA, IV and VI, and molecular modelling and rigid-body fitting of all subunit types. Remarkably, the latter enabled us to improve the resolution of the cryo-EM structure from 11 A to the final 10 A. The 10 A structure allows firm assessment of various structural parameters of the 8x6mer, the 4x6mer and the 2x6mer, and reveals a total of 46 inter-hexamer bridges. These group as 11 types of interface: four at the 2x6mer level (II-II, II-IV, V-VI, IV-VI), three form the 4x6mer (V-V, V-VI, VI-IIIB/IV/V), and four are required to assemble the 8x6mer (IIIA-IIIA, IIIA-IIIB, II-IV, IV-IV). The molecular model shows the amino acid residues involved, and reveals that several of the interfaces are intriguingly histidine-rich and likely to transfer allosteric signals between the different levels of the nested hierarchy.

摘要

来自鲎(美洲鲎)的蓝色铜蛋白血蓝蛋白是自然界中发现的最大的呼吸蛋白之一(3.5兆道尔顿),并表现出高度协同的氧结合特性。它的48个亚基排列成八个六聚体(1×6聚体),这些六聚体在由2×6聚体和4×6聚体组成的嵌套层次结构中形成天然的8×6聚体。这种四级结构由八种亚基类型(称为I、IIA、II、IIIA、IIIB、IV、V和VI)构成,其中只有II型已被测序。1×6聚体的晶体结构是已知的,但对于8×6聚体,仅存在一个40 Å的三维重建结构。因此,8×6聚体的结构参数尚未完全确定,八个六聚体之间的分子界面仍有待定义。然而,这对于理解变构转变如何在不同层次之间介导至关重要。在这里,我们展示了通过冷冻电子显微镜(cryo-EM)和单颗粒分析获得的氧化态8×6聚体的10 Å结构(FSC(1/2-bit)标准)。此外,我们展示了通过对II、IIIA、IV和VI型亚基进行DNA测序以及对所有亚基类型进行分子建模和刚体拟合得到的分子模型。值得注意的是,后者使我们能够将冷冻电镜结构的分辨率从11 Å提高到最终的10 Å。10 Å的结构使我们能够可靠地评估8×6聚体、4×6聚体和2×6聚体的各种结构参数,并揭示了总共46个六聚体间桥。这些桥可分为11种界面类型:在2×6聚体水平有四种(II-II、II-IV、V-VI、IV-VI),在4×6聚体水平有三种(V-V、V-VI、VI-IIIB/IV/V),在组装8×6聚体时需要四种(IIIA-IIIA、IIIA-IIIB、II-IV、IV-IV)。分子模型显示了涉及的氨基酸残基,并揭示了几个界面富含组氨酸,可能在嵌套层次结构的不同水平之间传递变构信号。

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