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人骨髓瘤二聚体IgA1的近平面溶液结构对黏膜免疫和IgA肾病的影响。

Implications of the near-planar solution structure of human myeloma dimeric IgA1 for mucosal immunity and IgA nephropathy.

作者信息

Bonner Alexandra, Furtado Patricia B, Almogren Adel, Kerr Michael A, Perkins Stephen J

机构信息

Department of Biochemistry and Molecular Biology, University College London, London, United Kingdom.

出版信息

J Immunol. 2008 Jan 15;180(2):1008-18. doi: 10.4049/jimmunol.180.2.1008.

DOI:10.4049/jimmunol.180.2.1008
PMID:18178841
Abstract

IgA is unique in being able to form a diverse range of polymeric structures. Increases in the levels of dimeric IgA1 (dIgA1) in serum have been implicated in diseases such as IgA nephropathy. We have determined the solution structure for dIgA1 by synchrotron x-ray and neutron scattering and analytical ultracentrifugation. The Guinier radius of gyration (RG) of 7.60-8.65 nm indicated that the two monomers within dIgA1 are arranged in an extended conformation. The distance distribution curve P(r) gave an overall length (L) of 22-26 nm. These results were confirmed by the sedimentation coefficient and frictional ratio of dIgA1. Constrained scattering modeling starting from the IgA1 monomer solution structure revealed a near-planar dimer structure for dIgA1. The two Fc regions form a slightly bent arrangement in which they form end-to-end contacts, and the J chain was located at this interface. This structure was refined by optimizing the position of the four Fab regions. From this, the best-fit solution structures show that the four Fab Ag-binding sites are independent of one another, and the two Fc regions are accessible to receptor binding. This arrangement allows dIgA1 to initiate specific immune responses by binding to FcalphaRI receptors, while still retaining Ag-binding ability, and to be selectively transported to mucosal surfaces by binding to the polymeric Ig receptor to form secretory IgA. A mechanism for the involvement of dIgA1 oligomers in the pathology of IgA nephropathy is discussed in the light of this near-planar structure.

摘要

免疫球蛋白A(IgA)能够形成多种聚合结构,这一点很独特。血清中双聚体IgA1(dIgA1)水平升高与IgA肾病等疾病有关。我们通过同步加速器X射线、中子散射和分析超速离心确定了dIgA1的溶液结构。dIgA1的吉尼埃回转半径(RG)为7.60 - 8.65纳米,表明dIgA1中的两个单体呈伸展构象排列。距离分布曲线P(r)给出的总长度(L)为22 - 26纳米。dIgA1的沉降系数和摩擦比证实了这些结果。从IgA1单体溶液结构开始的受限散射建模揭示了dIgA1的近平面二聚体结构。两个Fc区域形成略微弯曲的排列,它们端对端接触,J链位于该界面处。通过优化四个Fab区域的位置对该结构进行了优化。由此,最佳拟合溶液结构表明四个Fab抗原结合位点相互独立,并且两个Fc区域可用于受体结合。这种排列使dIgA1能够通过与FcalphaRI受体结合引发特异性免疫反应,同时仍保留抗原结合能力,并通过与聚合免疫球蛋白受体结合选择性地转运至黏膜表面以形成分泌型IgA。鉴于这种近平面结构,讨论了dIgA1寡聚体参与IgA肾病病理的机制。

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