School of Biological Sciences, University of Liverpool, Liverpool L69 7ZB, United Kingdom.
J Biol Chem. 2010 Jan 8;285(2):914-22. doi: 10.1074/jbc.M109.010892. Epub 2009 Nov 16.
Elevated levels of the calcium-binding protein S100A4 promote metastasis and in carcinoma cells are associated with reduced survival of cancer patients. S100A4 interacts with target proteins that affect a number of activities associated with metastatic cells. However, it is not known how many of these interactions are required for S100A4-promoted metastasis, thus hampering the design of specific inhibitors of S100A4-induced metastasis. Intracellular S100A4 exists as a homodimer through previously identified, well conserved, predominantly hydrophobic key contacts between the subunits. Here it is shown that mutating just one key residue, phenylalanine 72, to alanine is sufficient to reduce the metastasis-promoting activity of S100A4 to 50% that of the wild type protein, and just 2 or 3 specific mutations reduces the metastasis-promoting activity of S100A4 to less than 20% that of the wild type protein. These mutations inhibit the self-association of S100A4 in vivo and reduce markedly the affinity of S100A4 for at least two of its protein targets, a recombinant fragment of non-muscle myosin heavy chain isoform A, and p53. Inhibition of the self-association of S100 proteins might be a novel means of inhibiting their metastasis-promoting activities.
钙结合蛋白 S100A4 水平升高可促进转移,并且在癌细胞中与癌症患者的生存率降低有关。S100A4 与靶蛋白相互作用,影响与转移细胞相关的许多活动。但是,尚不清楚 S100A4 促进转移所需的这些相互作用有多少,从而阻碍了 S100A4 诱导转移的特异性抑制剂的设计。细胞内 S100A4 通过先前鉴定的、高度保守的、主要是亚基之间的疏水关键接触形成同源二聚体。这里显示,仅突变一个关键残基(苯丙氨酸 72)为丙氨酸足以将 S100A4 的促转移活性降低至野生型蛋白的 50%,而仅 2 或 3 个特定突变将 S100A4 的促转移活性降低至野生型蛋白的 20%以下。这些突变抑制了 S100A4 的体内自缔合,并显着降低了 S100A4 与其至少两个蛋白靶标(非肌肉肌球蛋白重链同工型 A 的重组片段和 p53)的亲和力。S100 蛋白的自缔合抑制可能是抑制其促转移活性的新方法。
