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首页> 外文期刊>Nanoscale >Comparative evaluation of MAX-Ti3AlC2 and MXene-Ti3C2 as affinity chromatographic materials for highly selective enrichment of phosphopeptides
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Comparative evaluation of MAX-Ti3AlC2 and MXene-Ti3C2 as affinity chromatographic materials for highly selective enrichment of phosphopeptides

机译:MAX-Ti3AlC2和比较评价MXene-Ti3C2亲和色谱材料高度的选择性富集此处则

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MAX and MXene have received considerable attention owing to their outstanding performance in fields like battery and catalysis. However, their possible biomedical applications have rarely been considered, especially the affinity chromatographic applications in proteomics. In this work, considering the large number of exposed metal sites, small binding potential resistance and fast mass transfer speed, layered ternary carbides MAX-Ti3AlC2 and MXene-Ti3C2 with a two-dimensional nanostructure were successfully explored for the first time as affinity chromatography stationary phases for the specific capture of phosphopeptides from complex biological samples. Helium ion microscopy, transmission electron microscopy, atomic force microscopy, X-ray diffraction spectra, X-ray photoelectron spectroscopy and zeta potential measurement results confirmed that the MXene-Ti3C2 was well exfoliated from the pristine MAX-Ti3AlC2. Ti3AlC2 showed better enrichment specificity than MXene-Ti3C2. The detection limit of Ti3AlC2 was as low as 5 fmol. Even when the molar ratio of BSA to beta-casein tryptic digests increased to 1000 : 1, two characteristic phosphopeptides with a relatively clear background could be detected after enrichment. After five cycles of repeated use, the enrichment specificity of Ti3AlC2 still remains. Furthermore, 91 and 830 unique phosphopeptides from 23 and 525 phosphoproteins were identified from milk and BEL7402 cells, respectively. Among them, 27 and 170 phosphopeptides, 12 and 56 phosphoproteins identified from milk and BEL7402 cells were not detected with commercial TiO2 after three independent replicates, which have great potential in providing complementary coverage of phosphoproteome. This work opens up new applications of Ti3AlC2 and MXene-Ti3C2, and will play more important role for phosphorylated proteomics in biomedicine.
机译:麦克斯和MXene得到了相当大的关注由于他们的出色的表现领域如电池和催化作用。可能的生物医学应用很少考虑,尤其是亲和力色谱在蛋白质组学中的应用。这项工作,考虑到大量的暴露的金属网站,小绑定的潜力阻力和传质速度快,分层三元碳化物MAX-Ti3AlC2和MXene-Ti3C2二维纳米结构是成功首次探讨了亲和力特定的色谱固定相捕获的此处则复杂生物样品。透射电子显微镜,原子力显微镜、x射线衍射谱、x光光电子能谱和电动电势测量结果证实从原始MXene-Ti3C2很清新MAX-Ti3AlC2。比MXene-Ti3C2特异性。Ti3AlC2低至5 fmol。摩尔BSA比β-酪蛋白胰蛋白酶的消化增加到1000:1,两个特点此处则相对清晰背景浓缩后可以检测到。经过五周期的重复使用,浓缩特异性Ti3AlC2仍然存在。此外,91年和830年独特的此处则从23和525磷蛋白质识别分别从牛奶和BEL7402细胞。27和170此处则,12和56从牛奶和BEL7402磷蛋白质鉴定没有检测到细胞与商业二氧化钛后三个独立复制,巨大的潜力提供互补的报道。法的组织磷酸化蛋白质组新应用程序的Ti3AlC2 MXene-Ti3C2,将为磷酸化发挥更重要的作用蛋白质组学在生物医学。

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