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Agitation-induced aggregation and subvisible particulate formation in model proteins

机译:激荡诱导的聚集和模型蛋白中的亚可见颗粒形成

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摘要

The kinetics of agitation-induced subvisible particle formation was investigated for a few model proteins - human serum albumin (HSA), hen egg white lysozyme (HEWL), and a monoclonal antibody (IgG2). Experiments were carried out for the first time under relatively low protein concentration and low agitation speed to investigate the details of subvisible particle formation at the initial phase of aggregation (<2%) process. Upon agitation, both soluble higher molecular mass species (HMMS) and subvisible particles (SbVPs) formed at different rates, and via different mechanisms. Agitation enhanced exposure of hydrophobic sites in HSA but did not cause detectable structural changes in HEWL and IgG2. SbVPs from HSA partially dissociates in a neutral pH buffer (SEC mobile phase) but does not upon dilution in the same formulation buffer. Opposite results were obtained for SbVPs from IgG2 and HEWL. Neither the relative hydrophobic surface area nor the Tm of the model proteins seems to be an indicator of tendency for agitation-mediated SbVP formation. Taken together, our data suggests that agitation-induced SbVP formation can occur through different mechanisms and can vary, depending on the protein and solution conditions.
机译:研究了几种模型蛋白-人血清白蛋白(HSA),蛋清溶菌酶(HEWL)和单克隆抗体(IgG2)的搅拌诱导的亚可见颗粒形成的动力学。第一次在相对较低的蛋白质浓度和较低的搅拌速度下进行实验,以研究在聚集初始阶段(<2%)的亚可见颗粒形成的细节。搅拌后,可溶性高分子量物质(HMMS)和亚可见颗粒(SbVPs)的形成速率不同,机制不同。搅拌增强了HSA中疏水位点的暴露,但并未引起HEWL和IgG2的可检测结构变化。来自HSA的SbVP在中性pH缓冲液(SEC流动相)中部分解离,但在同一制剂缓冲液中稀释后不会解离。从IgG2和HEWL获得SbVP的结果相反。模型蛋白的相对疏水表面积和Tm都不能指示搅拌介导的SbVP形成的趋势。两者合计,我们的数据表明,搅拌诱导的SbVP形成可以通过不同的机制发生,并且可以变化,这取决于蛋白质和溶液条件。

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