降级(电信)
介电谱
电阻抗
材料科学
肽
电极
化学工程
化学
分析化学(期刊)
电化学
色谱法
生物化学
电子工程
电气工程
工程类
物理化学
作者
Anna Biela,Michael Watkinson,Ute‐Christiane Meier,David Baker,Gavin Giovannoni,C. Remzi Becer,Steffi Krause
标识
DOI:10.1016/j.bios.2015.01.060
摘要
Matrix metalloproteinase-9 (MMP-9) plays an important role in both physiological and pathological processes. This enzyme is a peripheral biomarker of neuroinflammation in multiple sclerosis (MS), a chronic autoimmune disease of the central nervous system . Presently, expensive magnetic resonance imaging (MRI) studies are used to monitor subclinical disease activity in MS. An alternative to costly MRI scans could be the detection of MMP-9, using a low-cost, disposable sensor system for MMP-9 suitable for home-monitoring of inflammation. This would allow an early prediction of the failure of anti-inflammatory therapies and more timely clinical intervention to limit neuronal damage and prevent disability. Herein we present the development of a disposable sensor for fast and straightforward detection of MMP-9. Biosensors were produced by coating electrodes with oxidized dextran and subsequent cross-linking with peptides containing specific cleavage sites for MMP-9. Exposure of the films to the enzyme resulted in the degradation of the films, which was monitored using impedance measurements. Sensor response was rapid, a significant impedance change was usually observed within 5 min after the addition of MMP-9. Sensors showed a negligible response to matrix metalloproteinase-2 (MMP-2), a protease which may interfere with MMP-9 detection. The peptide sequence with the highest sensitivity and selectivity Leu–Gly–Arg–Met–Gly–Leu–Pro–Gly–Lys was selected to construct calibration curves . MMP-9 was successfully detected in a clinically relevant range from 50 to 400 ng/ml. Two different processes of hydrogel degradation were observed on electrode surfaces with different roughness, and both appeared suitable to monitor MMP-9 activity. The sensor materials are generic and can be easily adopted to respond to other proteases by selecting peptide cross-linkers with suitable cleavage sites. • Disposable sensor capable of detecting MMP-9 in clinically relevant range for relapsing remitting multiple sclerosis was developed. • The sensor material showed good selectivity to MMP-9 in the presence of MMP-2. • The sensors response to MMP-9 was rapid. Enzyme activities could be detected in 5 min. • The sensor fabrication process is simple, lending itself to mass production in the future.
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