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首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >Discrimination of cysteamine from mercapto amino acids through isoelectric point-mediated surface ligand exchange of beta-cyclodextrin-modified gold nanoparticles
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Discrimination of cysteamine from mercapto amino acids through isoelectric point-mediated surface ligand exchange of beta-cyclodextrin-modified gold nanoparticles

机译:通过等电点介导的β-环糊精改性金纳米颗粒的等电点介导的表面配体交换鉴别巯基氨基酸的半胱胺辨别

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摘要

The discrimination of cysteamine (CA) from mercapto amino acids (including glutathione, cysteine and homocysteine, GSH/Cys/Hcy) with high efficiency is essential to detect biothiols in a physiological environment. Herein, a nano-assembly was constructed by combining one-pot synthesized beta-cyclodextrin-modified AuNPs and encapsulated rhodamine 6G (R6G-beta-CD@AuNPs) without covalent modification. Interestingly, when the pH value of the tested solution was approximately the isoelectric point (pI) of the biothiol, the quenched fluorescence of R6G-beta-CD@AuNPs was obviously restored by the introduction of the biothiol, which was due to the replacement of the R6G-beta-CD composite by the biothiol on the surfaces of AuNPs via a stronger S-Au bond. The pI-mediated surface ligand exchange process was designed for the first time for the discrimination and detection of CA and GSH/Cys/Hcy at the pH values of 9.5 and 5.5, respectively. Under the optimized conditions, the enhanced fluorescence intensity displayed a good linear response to the concentration of each biothiol, with the detection limits of CA, GSH, Cys and Hcy calculated as 66.8, 417.6, 652.7 and 603.4 nM, respectively. The ingenious fabrication of the R6G-beta-CD@AuNPs sensing platform eliminated the interferences from cholesterol by host-guest interactions and enabled high selectivity for the detection of biothiols in human serum samples. The pI-mediated sensing platform exhibits great potential for biothiol-related therapeutic drug monitoring.
机译:具有高效率的巯基氨基酸(包括谷胱甘肽,半胱氨酸,半胱氨酸,GSH / Cys / Hcy)的半胱胺(CA)的鉴定对于在生理环境中检测生物醇是必不可少的。在此,通过将单罐合成的β-环糊精改性的AUNP和包封的罗丹明6g(R6G-BETA-CD-AUNPS)组合而没有共价修饰来构建纳米组件。有趣的是,当测试溶液的pH值大致为生物硫醇的等电点(PI)时,通过引入Biothiol显然恢复了R6G-β-CD的淬火荧光,这是由于更换通过较强的S-Au键在AUNPS表面上的Biothiol的R6G-Beta-CD复合。 PI介导的表面配体交换过程首次设计用于鉴别和检测pH值为9.5和5.5的Ca和Gsh / Cys / Hcy。在优化条件下,增强的荧光强度显示出对每种生物醇浓度的良好线性响应,分别计算为66.8,417.6,652.7和603.4nm的Ca,Gsh,Cys和Hcy的检测限。 R6G-Beta-CD / AUNPS传感平台的巧妙制造消除了宿主访客的相互作用从胆固醇的干扰,并使能量高选择性用于检测人血清样品中的生物醇。 PI介导的传感平台表现出与生物醇相关的治疗药物监测有巨大潜力。

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