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中性粒细胞激活肽-2和黑色素瘤生长刺激活性作为中性粒细胞激活的单体发挥作用。

Neutrophil-activating peptide-2 and melanoma growth-stimulatory activity are functional as monomers for neutrophil activation.

作者信息

Rajarathnam K, Kay C M, Dewald B, Wolf M, Baggiolini M, Clark-Lewis I, Sykes B D

机构信息

Protein Engineering Network of Centres of Excellence (PENCE) and the Department of Biochemistry, University of Alberta, Edmonton, Alberta T6G 2S2, Canada.

出版信息

J Biol Chem. 1997 Jan 17;272(3):1725-9. doi: 10.1074/jbc.272.3.1725.

DOI:10.1074/jbc.272.3.1725
PMID:8999852
Abstract

Neutrophil-activating peptide-2 (NAP-2) and melanoma growth-stimulatory activity (MGSA) are members of the chemokine family of inflammatory proteins. The structures of NAP-2, determined by x-ray crystallography, and MGSA, elucidated by NMR spectroscopy, revealed a tetramer and dimer, respectively. In order to address the relevance of multimeric species to their activities on neutrophils, analogs of NAP-2 and MGSA were synthesized in which the backbone amide proton of Leu-22 in NAP-2, and Val-26 in MGSA, was substituted with the bulky methyl group (NH --> NCH3). These analogs were shown to be monomeric by sedimentation equilibrium ultracentrifugation studies and were similar to the corresponding native protein in assays for neutrophil elastase release and Ca2+ mobilization from IL-8R1 and IL-8R2 transformed cells. Sedimentation equilibrium studies of the native NAP-2 and MGSA were also carried out to address the association behavior. For NAP-2, there was no evidence for the tetramer, but an equilibrium between monomers and dimers and the dissociation constant was calculated to be 50-100 microM. Similarly, MGSA showed a monomer-dimer equilibrium with a Kd of approximately 5 microM. The data from the monomeric analogs and also the calculation of dissociation constants indicate that NAP-2 and MGSA have a tendency to associate above the concentrations required for maximal activity or for receptor activation, but at functional concentrations they are predominantly monomers.

摘要

中性粒细胞激活肽-2(NAP-2)和黑色素瘤生长刺激活性因子(MGSA)是炎症蛋白趋化因子家族的成员。通过X射线晶体学确定的NAP-2结构以及通过核磁共振光谱阐明的MGSA结构分别显示为四聚体和二聚体。为了研究多聚体形式与其对中性粒细胞活性的相关性,合成了NAP-2和MGSA的类似物,其中NAP-2中Leu-22的主链酰胺质子以及MGSA中Val-26的主链酰胺质子被庞大的甲基取代(NH→NCH3)。沉降平衡超速离心研究表明这些类似物为单体,并且在中性粒细胞弹性蛋白酶释放测定以及从IL-8R1和IL-8R2转化细胞中动员Ca2+的测定中,它们与相应的天然蛋白相似。还对天然NAP-2和MGSA进行了沉降平衡研究以探讨缔合行为。对于NAP-2,没有证据表明存在四聚体,但存在单体和二聚体之间的平衡,计算得出的解离常数为50 - 100 microM。同样,MGSA显示出单体 - 二聚体平衡,Kd约为5 microM。来自单体类似物的数据以及解离常数的计算表明,NAP-2和MGSA在高于最大活性或受体激活所需浓度时倾向于缔合,但在功能浓度下它们主要是单体。

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