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人核糖体蛋白 S19 二聚体与人 C5a 过敏毒素之间分子模拟的基础。

Base of molecular mimicry between human ribosomal protein S19 dimer and human C5a anaphylatoxin.

机构信息

Department of Molecular Pathology, Faculty of Life Science, Kumamoto University, Kumamoto 860, Japan.

出版信息

Int Immunopharmacol. 2010 Dec;10(12):1541-7. doi: 10.1016/j.intimp.2010.09.002. Epub 2010 Sep 23.

DOI:10.1016/j.intimp.2010.09.002
PMID:20869475
Abstract

The crosslinked homodimer of human ribosomal protein S19 (hRP S19) but not hRP S19 monomer shares the hC5a receptor ligation capacity with anaphylatoxin hC5a. The hRP S19 dimer engages hC5a receptor-bearing monocytes in chemotactic movement and secretion as does hC5a. Two submolecular regions essential for the receptor ligation were already identified in hRP S19 as well as in hC5a. Using the tertiary structure data base of an archaeobacterial RP S19 as template, we made a tertiary structure model of hRP S19. The obtained structure was almost entirely α-helical with two short β-sheet regions, and folds a five α-helix bundle organized around a central amphipathic α-helix. While the secondary structure components were similar to those of hC5a, the gross tertiary structure of hRP S19 was loose and the distance between the two receptor binding regions was rather big in comparison to that of hC5a. Anti-recombinant hC5a rabbit antibodies cross-recognized not only the crosslinked hRP S19 dimer but also the guinea pig (gp) RP S19 dimer, however, these antibodies reacted hRP S19 monomer and crosslinked Gln137Asn-hRP S19 mutant dimer at significantly less extents. These antibodies neutralized the monocyte attracting capacity of the hRP S19 dimer in vitro and that of the gpRP S19 dimer in vivo. We assume that the crosslinkage between Lys122 of one hRP S19 molecule and Gln137 of the other one would assemble the hC5a-like structure probably providing one of two receptor binding regions by each hRP S19 subunit.

摘要

人核糖体蛋白 S19(hRP S19)的交联同源二聚体而非单体与过敏毒素 hC5a 具有 hC5a 受体结合能力。hRP S19 二聚体与携带 hC5a 受体的单核细胞发生趋化运动和分泌,与 hC5a 相同。已经在 hRP S19 以及 hC5a 中鉴定出两个亚分子区域对于受体结合是必需的。使用古细菌 RP S19 的三级结构数据库作为模板,我们构建了 hRP S19 的三级结构模型。获得的结构几乎完全是α-螺旋,有两个短的β-折叠区,并且折叠了一个围绕中央两亲性α-螺旋组织的五α-螺旋束。虽然二级结构成分与 hC5a 的相似,但 hRP S19 的总体三级结构较松散,并且两个受体结合区域之间的距离比 hC5a 的大。抗重组 hC5a 兔抗体不仅交叉识别交联的 hRP S19 二聚体,还识别豚鼠(gp)RP S19 二聚体,然而,这些抗体对 hRP S19 单体和交联的 Gln137Asn-hRP S19 突变体二聚体的反应程度要小得多。这些抗体在体外中和 hRP S19 二聚体的单核细胞吸引能力,以及体内中和 gpRP S19 二聚体的单核细胞吸引能力。我们假设一个 hRP S19 分子的 Lys122 与另一个 hRP S19 分子的 Gln137 之间的交联将组装成类似 hC5a 的结构,可能由每个 hRP S19 亚基提供两个受体结合区域之一。

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