首页> 外文期刊>Acta crystallographica. Section F, Structural biology communications >Formulation screening by differential scanning fluorimetry: how often does it work?
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Formulation screening by differential scanning fluorimetry: how often does it work?

机译:通过差示扫描荧光法进行配方筛选:它多久运作一次?

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摘要

There is strong evidence to suggest that a protein sample needs to be well folded and uniform in order to form protein crystals, and it is accepted knowledge that the formulation can have profound effects on the behaviour of the protein sample. The technique of differential scanning fluorimetry (DSF) is a very accessible method to determine protein stability as a function of the formulation chemistry and the temperature. A diverse set of 252 soluble protein samples was subjected to a standard formulation-screening protocol using DSF. Automated analysis of the DSF results suggest that in over 35% of cases buffer screening significantly increases the stability of the protein sample. Of the 28 standard formulations tested, three stood out as being statistically better than the others: these included a formulation containing the buffer citrate, long known to be 'protein friendly'; bis-tris and ADA were also identified as being very useful buffers in protein formulations.
机译:有强有力的证据表明,蛋白质样品需要很好地折叠和均匀,以形成蛋白质晶体,并且已接受该制剂对蛋白质样品的行为产生深远的影响。 差分扫描荧光测定法(DSF)的技术是一种非常可接近的方法,以确定蛋白质稳定性作为制剂化学和温度的函数。 使用DSF对不同的252种可溶性蛋白质样品进行标准配方筛选方案。 DSF结果的自动分析表明,在35%的病例缓冲筛查中显着提高了蛋白质样品的稳定性。 在测试的28种标准制剂中,三个突出的统计学上比其他制剂更好:这些包括含有柠檬酸盐的缓冲液,长度为“蛋白质”的制剂; BIS-TRIS和ADA也被鉴定为蛋白质制剂中的非常有用的缓冲剂。

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