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胰岛素样生长因子结合蛋白-2:NMR 分析及 N 端结构域的结构特征。

Insulin-like growth factor binding protein-2: NMR analysis and structural characterization of the N-terminal domain.

机构信息

Medicinal Chemistry and Drug Action, Monash Institute of Pharmaceutical Sciences, Monash University, Parkville, Victoria 3052, Australia.

出版信息

Biochimie. 2012 Mar;94(3):608-16. doi: 10.1016/j.biochi.2011.09.012. Epub 2011 Sep 22.

DOI:10.1016/j.biochi.2011.09.012
PMID:21951978
Abstract

The insulin-like growth factor binding proteins are a family of six proteins (IGFBP-1 to -6) that bind insulin-like growth factors-I and -II (IGF-I/II) with high affinity. In addition to regulating IGF actions, IGFBPs have IGF-independent functions. IGFBP-2, the largest member of this family, is over-expressed in many cancers and has been proposed as a possible target for the development of novel anti-cancer therapeutics. The IGFBPs have a common architecture consisting of conserved N- and C-terminal domains joined by a variable linker domain. The solution structure and dynamics of the C-terminal domain of human IGFBP-2 have been reported (Kuang Z. et al. J. Mol. Biol. 364, 690-704, 2006) but neither the N-domain (N-BP-2) nor the linker domain have been characterised. Here we present NMR resonance assignments for human N-BP-2, achieved by recording spectra at low protein concentration using non-uniform sampling and maximum entropy reconstruction. Analysis of secondary chemical shifts shows that N-BP-2 possesses a secondary structure similar to that of other IGFBPs. Although aggregation hampered determination of the solution structure for N-BP-2, a homology model was generated based on the high degree of sequence and structure homology exhibited by the IGFBPs. This model was consistent with experimental NMR and SAXS data and displayed some unique features such as a Pro/Ala-rich non-polar insert, which formed a flexible solvent-exposed loop on the surface of the protein opposite to the IGF-binding interface. NMR data indicated that this loop could adopt either of two alternate conformations in solution - an entirely flexible conformation and one containing nascent helical structure. This loop and an adjacent poly-proline sequence may comprise a potential SH3 domain interaction site for binding to other proteins.

摘要

胰岛素样生长因子结合蛋白是一个由 6 种蛋白质组成的家族(IGFBP-1 至 -6),它们与胰岛素样生长因子-I 和 -II(IGF-I/II)具有高亲和力。除了调节 IGF 的作用外,IGFBPs 还具有 IGF 独立的功能。该家族中最大的成员 IGFBP-2 在许多癌症中过度表达,并被提议作为开发新型抗癌治疗方法的可能靶点。IGFBPs 具有由保守的 N-和 C-末端结构域通过可变连接结构域连接而成的共同结构。已经报道了人 IGFBP-2 的 C-末端结构域的溶液结构和动力学(Kuang Z. 等人,J. Mol. Biol. 364, 690-704, 2006),但尚未对 N-结构域(N-BP-2)或连接结构域进行表征。在这里,我们通过在低蛋白浓度下使用非均匀采样和最大熵重建记录光谱,为人类 N-BP-2 提供了 NMR 共振分配。对二级化学位移的分析表明,N-BP-2 具有与其他 IGFBPs 相似的二级结构。尽管聚集妨碍了 N-BP-2 的溶液结构的确定,但根据 IGFBPs 表现出的高度序列和结构同源性,生成了同源模型。该模型与实验 NMR 和 SAXS 数据一致,并显示出一些独特的特征,例如富含脯氨酸/丙氨酸的非极性插入物,该插入物在蛋白质表面形成一个与 IGF 结合界面相对的灵活溶剂暴露环。NMR 数据表明,该环在溶液中可以采用两种交替构象之一 - 完全灵活的构象和一种包含新生螺旋结构的构象。该环和相邻的多脯氨酸序列可能包含一个潜在的 SH3 结构域结合位点,用于与其他蛋白质结合。

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