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SERS study on myeloperoxidase and its immunocomplex: Identification of binding interactions

机译:髓过氧化物酶及其免疫复合物的SERS研究:结合相互作用的鉴定

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Surface Enhanced Raman Spectroscopy (SERS) has demonstrated significant benefit in the identification of biological molecules. In this paper we have examined how to identify and differentiate the 150 kDa protein myeloperoxidase (MPO) from its corresponding antibody (Ab) and their immunocomplex through the use of SERS. The SERS signal of these biological molecules was enabled by 40 nm gold nanoparticles. The SERS spectra for both MPO and the Ab (an IgG molecule) demonstrated results consistent with previous published work on the Raman spectra of MPO and IgG antibodies. The immunocomplex SERS spectra showed peak shifts and intensity variations that could be attributed to conformational changes that occur during immunocomplex formation. Several key spectral areas have been identified which correspond to specific amino acids being shielded from undergoing resonance while new amino acid residues are made visible in the SERS spectrum of the immunocomplex and could be a result of conformational binding. These results indicate that SERS can be used to identify binding events and distinguish an immunocomplex from its individual components.
机译:表面增强拉曼光谱(SERS)在鉴定生物分子方面已显示出显着优势。在本文中,我们研究了如何通过使用SERS从其相应的抗体(Ab)及其免疫复合物中鉴定和区分150 kDa蛋白髓过氧化物酶(MPO)。这些生物分子的SERS信号通过40 nm金纳米颗粒实现。 MPO和Ab(一个IgG分子)的SERS光谱显示的结果与以前发表的有关MPO和IgG抗体的拉曼光谱的研究结果一致。免疫复合物SERS光谱显示峰移动和强度变化,这可能归因于免疫复合物形成过程中发生的构象变化。已经确定了几个关键的光谱区域,这些区域对应于被屏蔽以免发生共振的特定氨基酸,而新的氨基酸残基则在免疫复合物的SERS光谱中可见,并且可能是构象结合的结果。这些结果表明,SERS可用于识别结合事件,并从其单个成分中区分出免疫复合物。

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