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胰岛素样生长因子(IGF)I突变蛋白的结构变化影响其与IGF结合蛋白1和IGF-I受体的结合动力学速率。

Structural changes in insulin-like growth factor (IGF) I mutant proteins affecting binding kinetic rates to IGF binding protein 1 and IGF-I receptor.

作者信息

Jansson M, Uhlen M, Nilsson B

机构信息

Department of Biochemistry and Biotechnology, Royal Institute of Technology, Stockholm, Sweden.

出版信息

Biochemistry. 1997 Apr 8;36(14):4108-17. doi: 10.1021/bi961553i.

DOI:10.1021/bi961553i
PMID:9100004
Abstract

Ligand binding properties of five single amino acid substituted variants (V11A, D12A, Q15A, Q15E, and F16A) of human insulin-like growth factor I (IGF-I) were analyzed with respect to their binding affinities and binding kinetics to recombinant IGF binding protein 1 (IGFBP-1) and a soluble form of the IGF type I receptor (sIGF-I(R)), respectively. Side chains of the substituted residues are all predicted to be the most surface exposed in the alpha-helical portion of the B-region of the IGF-I molecule. The IGF-I variants were produced as fusion proteins to a IgG(Fc) binding protein domain, Z. Ligand binding kinetic rates were determined using BIAcore biosensor interaction analysis technology. All IGF-I variants showed altered binding affinities to both IGFBP- I and sIGF-I(R). Secondary structure content of the IGF-I variants was estimated using far-UV circular dichroism spectroscopy, followed by variable selection secondary structure calculations. The amount of calculated alpha-helicity is reduced for all the mutants, most predominantly for IGF-I(V11A) and IGF-I(F16A) proteins. Surprisingly, most of the effects of reduced binding affinities to both target proteins are attributed to lowered on-rates of binding, and these are correlated with the amount of alpha-helicity in each IGF-I variant. In addition, in some of the IGF-I variants, lowered off-rates of binding are observed. From the results, we propose that IGF-I is unusually sensitive to structural changes by surface amino acid substitutions in the B-region of the molecule. Therefore, biochemical or biological properties of amino acid substituted variants of IGF-I cannot be used in a straightforward way to dissect the direct involvement in binding of individual amino acid residues since structural changes may be involved.

摘要

分析了人胰岛素样生长因子I(IGF-I)的五个单氨基酸取代变体(V11A、D12A、Q15A、Q15E和F16A)与重组IGF结合蛋白1(IGFBP-1)和可溶性I型IGF受体(sIGF-I(R))的结合亲和力和结合动力学的配体结合特性。取代残基的侧链均预计在IGF-I分子B区域的α螺旋部分中最暴露于表面。IGF-I变体作为与IgG(Fc)结合蛋白结构域Z的融合蛋白产生。使用BIAcore生物传感器相互作用分析技术测定配体结合动力学速率。所有IGF-I变体对IGFBP-I和sIGF-I(R)的结合亲和力均发生了改变。使用远紫外圆二色光谱法估计IGF-I变体的二级结构含量,随后进行可变选择二级结构计算。所有突变体的计算α螺旋含量均降低,其中IGF-I(V11A)和IGF-I(F16A)蛋白最为明显。令人惊讶的是,与两种靶蛋白结合亲和力降低的大多数影响都归因于结合速率的降低,并且这些与每个IGF-I变体中的α螺旋含量相关。此外,在一些IGF-I变体中,观察到解离速率降低。根据结果,我们提出IGF-I对分子B区域中表面氨基酸取代引起的结构变化异常敏感。因此,IGF-I氨基酸取代变体的生化或生物学特性不能直接用于剖析单个氨基酸残基在结合中的直接参与情况,因为可能涉及结构变化。

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