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在用于微阵列的固相肽合成(SPPS)和肽偶联中,轻松并行筛选试剂稳定性、质量控制和计量学。

Easy parallel screening of reagent stability, quality control, and metrology in solid phase peptide synthesis (SPPS) and peptide couplings for microarrays.

作者信息

Achyuthan Komandoor E, Wheeler David R

机构信息

Biological/Chemical/Physical Microsensors Department, Sandia National Laboratories, 1515 Eubank Blvd., Albuquerque, NM, 87185, USA.

Special Technologies Department, Sandia National Laboratories, 1515 Eubank Blvd., Albuquerque, NM, 87185, USA.

出版信息

J Pept Sci. 2015 Oct;21(10):751-7. doi: 10.1002/psc.2806. Epub 2015 Aug 27.

DOI:10.1002/psc.2806
PMID:26310933
Abstract

Evaluating the stability of coupling reagents, quality control (QC), and surface functionalization metrology are all critical to the production of high quality peptide microarrays. We describe a broadly applicable screening technique for evaluating the fidelity of solid phase peptide synthesis (SPPS), the stability of activation/coupling reagents, and a microarray surface metrology tool. This technique was used to assess the stability of the activation reagent 1-{[1-(Cyano-2-ethoxy-2-oxo-ethylidenaminooxy)dimethylamino-morpholinomethylene]}methaneaminiumHexafluorophosphate (COMU) (Sigma-Aldrich, St. Louis, MO, USA) by SPPS of Leu-Enkephalin (YGGFL) or the coupling of commercially synthesized YGGFL peptides to (3-aminopropyl)triethyoxysilane-modified glass surfaces. Coupling efficiency was quantitated by fluorescence signaling based on immunoreactivity of the YGGFL motif. It was concluded that COMU solutions should be prepared fresh and used within 5 h when stored at ~23 °C and not beyond 24 h if stored refrigerated, both in closed containers. Caveats to gauging COMU stability by absorption spectroscopy are discussed. Commercial YGGFL peptides needed independent QC, due to immunoreactivity variations for the same sequence synthesized by different vendors. This technique is useful in evaluating the stability of other activation/coupling reagents besides COMU and as a metrology tool for SPPS and peptide microarrays.

摘要

评估偶联试剂的稳定性、质量控制(QC)以及表面功能化计量学对于高质量肽微阵列的生产至关重要。我们描述了一种广泛适用的筛选技术,用于评估固相肽合成(SPPS)的保真度、活化/偶联试剂的稳定性以及一种微阵列表面计量工具。该技术用于通过亮脑啡肽(YGGFL)的固相肽合成或商业合成的YGGFL肽与(3-氨丙基)三乙氧基硅烷修饰的玻璃表面的偶联来评估活化试剂1-{[1-(氰基-2-乙氧基-2-氧代-亚乙基氨基氧基)二甲基氨基-吗啉基亚甲基]}甲烷铵六氟磷酸盐(COMU)(美国密苏里州圣路易斯市西格玛奥德里奇公司)的稳定性。基于YGGFL基序的免疫反应性,通过荧光信号对偶联效率进行定量。得出的结论是,COMU溶液应新鲜制备,在约23°C下储存时应在5小时内使用,冷藏储存时不超过24小时,且均应保存在密闭容器中。讨论了通过吸收光谱法测量COMU稳定性的注意事项。由于不同供应商合成的相同序列的免疫反应性存在差异,商业YGGFL肽需要独立的质量控制。该技术除了可用于评估COMU之外,还可用于评估其他活化/偶联试剂的稳定性,并作为固相肽合成和肽微阵列的计量工具。

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