BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. rs3825942, PPARA, Metabolism of xenobiotics, Obesity, Leukocyte, Pharmacogenetics)
Bookmark Forward

Fabrication of self-healing magnetic nanoreceptors for glycoprotein via integrating boronate-affinity-oriented and sequential surface imprinting.

Jin-Ye Lang, Chen-Chen Bai, Shi-Song Yu, Meng-Ying Chen, Lin-Yi Dong, Zhen-Yu Zhao, Xian-Hua Wang

Analytica chimica acta 2022 Aug 15


filter terms:
  • antigen (1)
  • fetoprotein (1)
  • glycoprotein (10)
  • layer (4)
  • ovalbumin (1)
  • phenylboronic acid (2)
  • polydopamine (1)
  • polymers (2)
  • receptors (1)
  • serum (1)
  • signal (2)
    • Sizes of these terms reflect their relevance to your search.

    Molecularly imprinted polymers (MIPs) as artificial receptors have been widely applied in various fields. However, construction of MIPs for precise recognition of glycoprotein still remains a rather challenging task. To overcome this problem, we first fabricated boronate-affinity-oriented and sequential-surface imprinting magnetic nanoparticles (BSIMN) through integrating the boronate-affinity-oriented and sequential surface imprinting. The boronate-affinity-oriented immobilization of glycoprotein template endowed the BSIMN with homogeneous imprinted cavities. In addition, the polydopamine (PDA) imprinted layer was introduced by self-polymerization of dopamine in the first imprinting process, and then the phenylboronic acid (PBA) imprinted layer was introduced by boronate-affinity interaction in the second imprinting process. Surprisingly, the PBA imprinted layer possessed self-healing property due to the presence of pH-dependent boronate-affinity interaction between two imprinted layers. Therefore, the fabricated BSIMN exhibited excellent selectivity toward glycoprotein templates. To quantitatively detect glycoproteins in biological samples, the BSIMN was linked with hydrophilic rhodamine B-loaded/boronic acid-modified graphene oxide (HRBGO), which could selectively label glycoprotein and output amplified signal. In quantitative analysis, target glycoproteins were firstly captured by BSIMN and then specifically labeled by HRBGO; subsequently, the releasing agent was added to release numerous rhodamine B from HRBGO, and the corresponding fluorescence signal was used for further quantitative analysis. The proposed strategy showed ultrahigh sensitivity for ovalbumin, carcinoembryonic antigen and alpha fetoprotein with limit of detection of 4.5 fg mL-1, 3.6 fg mL-1 and 4.2 fg mL-1, respectively, and was successfully applied in determination of these glycoproteins in serum samples. Copyright © 2022 Elsevier B.V. All rights reserved.

    Citation

    Jin-Ye Lang, Chen-Chen Bai, Shi-Song Yu, Meng-Ying Chen, Lin-Yi Dong, Zhen-Yu Zhao, Xian-Hua Wang. Fabrication of self-healing magnetic nanoreceptors for glycoprotein via integrating boronate-affinity-oriented and sequential surface imprinting. Analytica chimica acta. 2022 Aug 15;1221:340108

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 35934351

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.