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Highly Selective Capture of Monophosphopeptides by Two-Dimensional Metal-Organic Framework Nanosheets

机译:通过二维金属 - 有机框架纳米液相色谱肽的高度选择性捕获

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摘要

Separation of monophosphopeptides from multi-phosphopeptides in complex biological samples is significant in the study of protein kinase signal transduction pathways. To the best of our knowledge, very few materials have been reported that could selectively enrich monophosphopeptides because of the chemical difficulty in retaining the intermediate monophosphopeptides and excluding both non-phosphopeptides and multi-phosphopeptides in acidic conditions, which requires unique interactions to balance the metallic affinity and the hydrophobicity. With the large surface area, abundant accessible active sites, and ultrathin structures, two-dimensional (2-D) metal-organic framework (MOF) Hf-1,3,S-tris(4-carboxyphenyl)benzene (BTB) nanosheets were rationally selected. Due to the elongated organic ligands and the balance between metallic affinity of clusters and hydrophobicity from ligands, the 2-D Hf-BTB nanosheets exhibited unique enrichment selectivity toward monophosphopeptides. The 2-D MOF nanosheets demonstrated excellent sensitivity (detection limit of 0.4 fmol mu L-1) and selectivity [1:1000 molar ratios of beta-casein/BSA (bovine serum albumin)] in model phosphopeptides enrichment. The nanosheets were implemented for the analysis of nonfat milk and human saliva samples as well as in situ isotope labeling for dysregulated phosphopeptides from patients' serum with anal canal inflammation, exhibiting 6.6-fold upregulation of serum phosphopeptide HS4 (ADpSGEGDFLAEGGGVR) compared to the control healthy serum. The proteomics analysis of mouse brain cortical samples associated with Alzheimer's disease, which were from Akt (protein kinase B) conditional knockout mouse and littermate control mouse, was further established with 2-D Hf-BTB nanosheets. With high capture efficiency for monophosphopeptides, this method was capable of distinguishing the difference of monophosphopeptides from microtubule-associated protein tau (MAPT/tau) between the Akt knockout sample and control sample.
机译:在蛋白激酶信号转导途径的研究中,复杂生物样品中多磷酸肽的单磷肽的分离是显着的。据我们所知,据报道,非常少的材料,其可以选择性地富化单磷肽,因为在酸性条件下保留中间体单磷肽并不包括非磷酸盐和多磷酸酯,这需要独特的相互作用来平衡金属亲和力和疏水性。随着大表面积,丰富的可移活性位点和超薄结构,二维(2-D)金属 - 有机骨架(MOF)HF-1,3,S-TRIS(4-羧基)苯(BTB)纳米蛋白酶是合理选择。由于细长的有机配体和簇之间的金属亲和力与来自配体的疏水性之间的平衡,2-D HF-BTB纳米片对单磷酸肽具有独特的富集选择性。 2-D MOF纳米片显示出优异的敏感性(0.4 fmol mu L-1的检测限),以及在模型磷肽富集中的选择性[1:1000摩尔比β-酪蛋白/ BSA(牛血清白蛋白)]。用于分析非脂肪牛奶和人类唾液样品的纳米片,以及对患者血清具有肛门管炎症的失调磷酸肽的原位同位素标记,与对照的对照,表现出6.6倍上调血清磷酸肽HS4(AdpsgegdFlaegGGVR)血清。用2-D HF-BTB纳米片进一步建立了与Alzheimer疾病相关的小鼠脑皮质样品与阿尔茨海默病相关的蛋白质组学分析。具有高磷酸肽的捕获效率,该方法能够将单磷酸肽与MicroTumule相关蛋白Tau(Mapt / Tau)之间的单磷肽差分区分为Akt敲除样品和对照样品之间的差异。

著录项

  • 来源
    《Analytical chemistry》 |2019年第14期|共9页
  • 作者单位

    Nanjing Normal Univ Jiangsu Key Lab Biofunct Mat Jiangsu Collaborat Innovat Ctr Biomed Funct Mat Coll Chem &

    Mat Sci Nanjing 210023 Jiangsu Peoples R China;

    Nanjing Normal Univ Jiangsu Key Lab Biofunct Mat Jiangsu Collaborat Innovat Ctr Biomed Funct Mat Coll Chem &

    Mat Sci Nanjing 210023 Jiangsu Peoples R China;

    Nanjing Normal Univ Jiangsu Key Lab Biofunct Mat Jiangsu Collaborat Innovat Ctr Biomed Funct Mat Coll Chem &

    Mat Sci Nanjing 210023 Jiangsu Peoples R China;

    Nanjing Univ State Key Lab Pharmaceut Biotechnol MOE Key Lab Model Anim Dis Study Model Anim Res Ctr 12 Xuefu Ave Nanjing 210061 Jiangsu Peoples R China;

    Nanjing Univ Chinese Med Coll Clin Med 1 Key Lab Metab Dis Chinese Med Nanjing 210023 Jiangsu Peoples R China;

    Nanjing Univ Chinese Med Coll Clin Med 1 Key Lab Metab Dis Chinese Med Nanjing 210023 Jiangsu Peoples R China;

    Nanjing Univ State Key Lab Pharmaceut Biotechnol MOE Key Lab Model Anim Dis Study Model Anim Res Ctr 12 Xuefu Ave Nanjing 210061 Jiangsu Peoples R China;

    Nanjing Normal Univ Jiangsu Key Lab Biofunct Mat Jiangsu Collaborat Innovat Ctr Biomed Funct Mat Coll Chem &

    Mat Sci Nanjing 210023 Jiangsu Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分析化学;
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