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在线近红外光谱法优化与监测γ-氨基丁酸的生物转化过程

On-line near-infrared spectroscopy optimizing and monitoring biotransformation process of γ-aminobutyric acid.

作者信息

Ding Guoyu, Hou Yuanyuan, Peng Jiamin, Shen Yunbing, Jiang Min, Bai Gang

机构信息

State Key Laboratory of Medicinal Chemical Biology, College of Pharmacy, Nankai University; Tianjin Key Laboratory of Molecular Drug Research, Nankai University, Tianjin 300071, China.

出版信息

J Pharm Anal. 2016 Jun;6(3):171-178. doi: 10.1016/j.jpha.2016.02.001. Epub 2016 Feb 6.

Abstract

Near-infrared spectroscopy (NIRS) with its fast and nondestructive advantages can be qualified for the real-time quantitative analysis. This paper demonstrates that NIRS combined with partial least squares (PLS) regression can be used as a rapid analytical method to simultaneously quantify l-glutamic acid (l-Glu) and γ-aminobutyric acid (GABA) in a biotransformation process and to guide the optimization of production conditions when the merits of NIRS are combined with response surface methodology. The high performance liquid chromatography (HPLC) reference analysis was performed by the -phthaldialdehyde pre-column derivatization. NIRS measurements of two batches of 141 samples were firstly analyzed by PLS with several spectral pre-processing methods. Compared with those of the HPLC reference analysis, the resulting determination coefficients (), root mean square error of prediction () and residual predictive deviation () of the external validation for the l-Glu concentration were 99.5%, 1.62 g/L, and 11.3, respectively. For the GABA concentration, , , and were 99.8%, 4.00 g/L, and 16.4, respectively. This NIRS model was then used to optimize the biotransformation process through a Box-Behnken experimental design. Under the optimal conditions without pH adjustment, 200 g/L l-Glu could be catalyzed by 7148 U/L glutamate decarboxylase (GAD) to GABA, reaching 99% conversion at the fifth hour. NIRS analysis provided timely information on the conversion from l-Glu to GABA. The results suggest that the NIRS model can not only be used for the routine profiling of enzymatic conversion, providing a simple and effective method of monitoring the biotransformation process of GABA, but also be considered to be an optimal tool to guide the optimization of production conditions.

摘要

近红外光谱(NIRS)具有快速、无损的优点,适用于实时定量分析。本文表明,将NIRS与偏最小二乘法(PLS)回归相结合,可作为一种快速分析方法,用于同时定量生物转化过程中的L-谷氨酸(L-Glu)和γ-氨基丁酸(GABA),并在将NIRS的优点与响应面方法相结合时指导生产条件的优化。采用邻苯二甲醛柱前衍生化法进行高效液相色谱(HPLC)参考分析。首先用几种光谱预处理方法通过PLS对两批共141个样品进行NIRS测量。与HPLC参考分析结果相比,L-Glu浓度外部验证的决定系数(R²)、预测均方根误差(RMSEP)和剩余预测偏差(RPD)分别为99.5%、1.62 g/L和11.3。对于GABA浓度,R²、RMSEP和RPD分别为99.8%、4.00 g/L和16.4。然后通过Box-Behnken实验设计使用该NIRS模型优化生物转化过程。在不调节pH值的最佳条件下,200 g/L的L-Glu可被7148 U/L的谷氨酸脱羧酶(GAD)催化生成GABA,在第5小时转化率达到99%。NIRS分析提供了从L-Glu转化为GABA的及时信息。结果表明,NIRS模型不仅可用于酶促转化的常规分析,为监测GABA的生物转化过程提供一种简单有效的方法,还可被视为指导生产条件优化的最佳工具。

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