A Direct Method to Monitor Glutathione Stability in High Concentration Protein Formulations

Seth Keever, B. Nakhle, B. Yeung
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Abstract

Due to its antioxidant properties and favorable safety profile, glutathione (GSH) finds use in protein formulations by improving overall protein stability. Once degraded, primarily by oxidation into glutathione disulfide (GSSG), the protecting effect of GSH is lost. A simple, direct method using reversed-phase separation and charged-aerosol detection (RP-CAD) to quantitate GSH is described in this paper. The analytical methodology is also capable of monitoring several by-product degradants of GSH, both oxidative and non-oxidative. For high-concentration protein formulations, the method provides direct analysis of GSH and its degradants in the presence of protein at up to 225 mg/mL simply through a dilution of the sample. Quantitation of many amino acids typically included in pharmaceutical protein formulations is also possible. Use of an online diverting valve in the method prevents interference in the detector from the high protein concentration in formulation. Accuracy and effectiveness of this method is demonstrated through monitoring the stability of GSH in high-concentration protein formulations through confirmation of GSH concentration and mass-balance of its loss over time. Monitoring GSH stability in protein formulations is necessary, as GSH concentration is indicative of protein stability.
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一种直接监测高浓度蛋白质制剂中谷胱甘肽稳定性的方法
由于其抗氧化特性和良好的安全性,谷胱甘肽(GSH)通过提高蛋白质的整体稳定性而在蛋白质配方中得到应用。一旦降解,主要通过氧化为谷胱甘肽二硫化物(GSSG),GSH的保护作用就会丧失。本文介绍了一种简单、直接的反相分离荷电气溶胶检测法(RP-CAD)测定谷胱甘肽的方法。该分析方法还能够监测GSH的几种副产物降解物,包括氧化和非氧化降解物。对于高浓度蛋白质制剂,该方法在高达225mg/mL的蛋白质存在下,仅通过稀释样品,就可以直接分析GSH及其降解物。通常包括在药物蛋白质制剂中的许多氨基酸的定量也是可能的。在该方法中使用在线转向阀防止了制剂中高蛋白浓度对检测器的干扰。通过确认GSH浓度及其随时间损失的质量平衡,监测高浓度蛋白质制剂中GSH的稳定性,证明了该方法的准确性和有效性。监测蛋白质制剂中GSH的稳定性是必要的,因为GSH浓度指示蛋白质的稳定性。
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