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碱性成纤维细胞生长因子(bFGF)对热变性的稳定性。

The stability of bFGF against thermal denaturation.

作者信息

Vemuri S, Beylin I, Sluzky V, Stratton P, Eberlein G, Wang Y J

机构信息

Scios Nova Inc., Mountain View, CA 94043.

出版信息

J Pharm Pharmacol. 1994 Jun;46(6):481-6. doi: 10.1111/j.2042-7158.1994.tb03831.x.

Abstract

The influence of sulphated ligand and pH on thermal denaturation of basic fibroblast growth factor (bFGF) was investigated by differential scanning calorimetry (DSC), and verified by fluorescence spectrophotometry. Purity of bFGF before and after heat denaturation was assessed by SDS-PAGE analysis. In DSC studies the samples were heated to 95 degrees C. The midpoint of the temperature change in the thermogram was designated as Tm. Sulphated ligand experiments were undertaken in potassium phosphate (pH 6.5) and sodium acetate buffers. Control thermograms (with no ligand) showed a Tm at 59 degrees C in potassium phosphate buffer. Higher Tm values were noted as sulphated ligand concentration was increased. Similarly when heparin was added, the Tm moved to a higher temperature. A ratio as low as 0.3:1 of heparin to bFGF, increased the Tm to 90 degrees C, which is a 31 degrees C shift in Tm. The effect of pH on thermal denaturation of bFGF was studied in a citrate-phosphate-borate buffer system. A shift in Tm from 46 to 65 degrees C was observed as the pH is changed from 4 to 8. Changes in protein conformation as a function of pH were monitored by fluorescence spectroscopy. It was found that a pH range from 5 to 9 is optimal for the stability of bFGF formulations. In a stability study it was noted that heparin protected bFGF from thermal denaturation only at high temperature.

摘要

采用差示扫描量热法(DSC)研究了硫酸化配体和pH对碱性成纤维细胞生长因子(bFGF)热变性的影响,并通过荧光分光光度法进行了验证。通过SDS-PAGE分析评估热变性前后bFGF的纯度。在DSC研究中,将样品加热至95℃。热谱图中温度变化的中点被指定为Tm。在磷酸钾(pH 6.5)和醋酸钠缓冲液中进行硫酸化配体实验。对照热谱图(无配体)在磷酸钾缓冲液中显示Tm为59℃。随着硫酸化配体浓度的增加,观察到更高的Tm值。同样,当加入肝素时,Tm移至更高温度。肝素与bFGF的比例低至0.3:1时,Tm升高至90℃,即Tm有31℃的变化。在柠檬酸-磷酸-硼酸盐缓冲液系统中研究了pH对bFGF热变性的影响。当pH从4变为8时,观察到Tm从46℃变为65℃。通过荧光光谱监测蛋白质构象随pH的变化。发现pH范围为5至9对bFGF制剂的稳定性最佳。在稳定性研究中注意到,肝素仅在高温下保护bFGF免受热变性。

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