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Stability of domain 4 of the anthrax toxin protective antigen and the effect of the VWA domain of CMG2 on stability

机译:炭疽毒素保护抗原第4结构域的稳定性和CMG2的VWA结构域对稳定性的影响

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摘要

The major immunogenic component of the current anthrax vaccine, anthrax vaccine adsorbed (AVA) is protective antigen (PA). We have shown recently that the thermodynamic stability of PA can be significantly improved by binding to the Von‐Willebrand factor A (VWA) domain of capillary morphogenesis protein 2 (CMG2), and improvements in thermodynamic stability may improve storage and long‐term stability of PA for use as a vaccine. In order to understand the origin of this increase in stability, we have isolated the receptor binding domain of PA, domain 4 (D4), and have studied the effect of the addition of CMG2 on thermodynamic stability. We are able to determine a binding affinity between D4 and CMG2 (∼300 nM), which is significantly weaker than that between full‐length PA and CMG2 (170–300 pM). Unlike full‐length PA, we observe very little change in stability of D4 on binding to CMG2, using either fluorescence or 19F‐NMR experiments. Because in previous experiments we could observe a stabilization of both domain 4 and domain 2, the mechanism of stabilization of PA by CMG2 is likely to involve a mutual stabilization of these two domains.
机译:当前炭疽疫苗的主要免疫原性成分,吸附炭疽疫苗(AVA)是保护性抗原(PA)。我们最近发现,通过与毛细管形态发生蛋白2(CMG2)的Von-Willebrand因子A(VWA)域结合,可以显着改善PA的热力学稳定性,并且改善热力学稳定性可能会改善PA的储存和长期稳定性PA用作疫苗。为了了解这种稳定性增加的起因,我们分离了PA的受体结合结构域,结构域4(D4),并研究了添加CMG2对热力学稳定性的影响。我们能够确定D4和CMG2之间的结合亲和力(〜300 nM),这比全长PA和CMG2之间的结合亲和力(170-300 pM)弱得多。与全长PA不同,我们使用荧光或 19 F-NMR实验观察到D4与CMG2结合时稳定性几乎没有变化。因为在先前的实验中我们可以观察到域4和域2的稳定,所以CMG2稳定PA的机制可能涉及这两个域的相互稳定。

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