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Bradford 法在含有药物聚合物时定量蛋白质浓度。

Quantification of protein concentration by the Bradford method in the presence of pharmaceutical polymers.

机构信息

Department of Chemical and Biological Engineering, Chalmers University of Technology, SE-412 96 Gothenburg, Sweden.

出版信息

Anal Biochem. 2011 Apr 1;411(1):116-21. doi: 10.1016/j.ab.2010.12.026. Epub 2010 Dec 22.

Abstract

We investigated how the Bradford assay for measurements of protein released from a drug formulation may be affected by a concomitant release of a pharmaceutical polymer used to formulate the protein delivery device. The main result is that polymer-caused perturbations of the Coomassie dye absorbance at the Bradford monitoring wavelength (595nm) can be identified and corrected by recording absorption spectra in the region of 350-850mm. The pharmaceutical polymers Carbopol and chitosan illustrate two potential types of perturbations in the Bradford assay, whereas the third polymer, hydroxypropylmethylcellulose (HPMC), acts as a nonperturbing control. Carbopol increases the apparent absorbance at 595nm because the polymer aggregates at the low pH of the Bradford protocol, causing a turbidity contribution that can be corrected quantitatively at 595nm by measuring the sample absorbance at 850nm outside the dye absorption band. Chitosan is a cationic polymer under Bradford conditions and interacts directly with the anionic Coomassie dye and perturbs its absorption spectrum, including 595nm. In this case, the Bradford method remains useful if the polymer concentration is known but should be used with caution in release studies where the polymer concentration may vary and needs to be measured independently.

摘要

我们研究了在测定药物制剂中释放的蛋白质时,考马斯亮蓝法可能会受到用于蛋白质递送装置配方的药用聚合物同时释放的影响。主要结果表明,可以通过记录 350-850nm 区域的吸收光谱来识别和校正考马斯亮蓝监测波长(595nm)处聚合物引起的考马斯亮蓝染料吸光度的干扰。药用聚合物 Carbopol 和壳聚糖说明了 Bradford 测定法中的两种潜在干扰类型,而第三种聚合物羟丙基甲基纤维素(HPMC)则作为非干扰对照。Carbopol 在 595nm 处增加了表观吸光度,因为聚合物在 Bradford 方案的低 pH 下聚集,导致浊度贡献,可通过在染料吸收带外测量 850nm 处的样品吸光度在 595nm 处进行定量校正。壳聚糖在 Bradford 条件下是一种阳离子聚合物,与阴离子考马斯亮蓝染料直接相互作用,干扰其吸收光谱,包括 595nm。在这种情况下,如果知道聚合物浓度,Bradford 方法仍然有用,但在聚合物浓度可能变化且需要独立测量的释放研究中应谨慎使用。

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