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泊洛沙姆188与聚山梨酯80相比对重组人凝血因子VIII的稳定作用

Stabilization of a human recombinant factor VIII by poloxamer 188 in relation to polysorbate 80.

作者信息

Clark Jakson, Montgomery Jade, Squires Ryan, McGuire Joseph

机构信息

a School of Chemical, Biological and Environmental Engineering , Oregon State University , Corvallis , OR , USA.

出版信息

Pharm Dev Technol. 2016 Mar;21(2):250-4. doi: 10.3109/10837450.2014.987297. Epub 2014 Dec 4.

Abstract

Detection of enhanced surface tension depression by surfactant in the presence of protein was recently suggested as a basis for determining whether protein stabilization by that surfactant is owing to surfactant forming a steric barrier at interfaces or surfactant association with the protein. In particular, protein interaction with surfactant aggregates may lead to an increased concentration of monomers thus enhancing surfactant adsorption, or to formation of surfactant-protein complexes having little or no effect on adsorption. We compared the initial rates of surface tension depression by poloxamer 188 and polysorbate 80 (PS 80) in the presence and absence of a human recombinant factor VIII (rFVIII). Indirect evidence had suggested poloxamer 188 enters into stable associations with rFVIII in solution but does not form a steric barrier at the interface, while PS 80 behaves in contrary fashion. In this study, we show the presence of rFVIII caused an increase in the rate (reduction in the activation energy) of PS 80 adsorption, while no such change was recorded in the case of poloxamer 188. Thus, we provide substantiation for detection of protein-mediated acceleration of surfactant adsorption as a means to compare different surfactants in relation to their favored mechanism for protein stabilization.

摘要

最近有人提出,在蛋白质存在的情况下检测表面活性剂引起的表面张力降低增强,以此作为确定该表面活性剂对蛋白质的稳定作用是由于表面活性剂在界面处形成空间位阻屏障,还是由于表面活性剂与蛋白质缔合的依据。特别是,蛋白质与表面活性剂聚集体的相互作用可能导致单体浓度增加,从而增强表面活性剂的吸附,或者形成对吸附几乎没有影响或没有影响的表面活性剂 - 蛋白质复合物。我们比较了泊洛沙姆188和聚山梨酯80(PS 80)在有和没有重组人因子VIII(rFVIII)存在时表面张力降低的初始速率。间接证据表明,泊洛沙姆188在溶液中与rFVIII形成稳定缔合,但在界面处不形成空间位阻屏障,而PS 80的行为则相反。在本研究中,我们发现rFVIII的存在导致PS 80吸附速率增加(活化能降低),而泊洛沙姆188的情况未记录到这种变化。因此,我们为检测蛋白质介导的表面活性剂吸附加速提供了证据,以此作为比较不同表面活性剂在蛋白质稳定化方面偏好机制的一种手段。

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