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制备具有优异抗蛋白质吸附性能的受限硼酸亲和吸附剂,用于直接从生物基质中提取小的顺式二醇分子。

Preparation of restricted-access boronate affinity adsorbent with excellent anti-protein adsorption property for directly extracting small cis-diol molecules from biological matrices.

机构信息

Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of Ministry of Education, College of Chemistry & Materials Science, Northwest University, Xi'an, 710127, China.

Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of Ministry of Education, College of Chemistry & Materials Science, Northwest University, Xi'an, 710127, China.

出版信息

Talanta. 2023 Dec 1;265:124867. doi: 10.1016/j.talanta.2023.124867. Epub 2023 Jun 22.

DOI:10.1016/j.talanta.2023.124867
PMID:37385192
Abstract

Boronate affinity adsorbents are of great promise in the enrichment of small cis-diol-containing molecules (cis-diols) from biological matrices. This work develops a restricted-access boronate affinity mesoporous adsorbent, in which boronate sites are only distributed on the internal surface of mesopores and the external surface is a strongly hydrophilic layer. The adsorbent has high binding capacities (30.3 mg g, 22.9 mg g and 14.9 mg g for dopamine, catechol and adenosine, respectively) in spite of removal of the boronate sites on the external surface of adsorbent. The adsorption specific of adsorbent towards cis-diols was assessed by dispersive solid-phase extraction (d-SPE) method, and the results show that the adsorbent can selectively extract small cis-diols in the biosamples while exclude proteins completely. Under the optimal d-SPE, the nucleosides and cis-diol drugs in human serum were successfully analyzed by coupling d-SPE with high-performance liquid chromatography. Where, the detection limits are between 6.1 and 13.4 ng mL for four nucleosides, and 24.9 and 34.3 ng mL for two cis-diol drugs; the relative recoveries of all the analytes vary from 84.1% to 110.1% (RSDs <13.4%, n = 6). The results indicate that the adsorbent can directly treat the real biosamples without the necessary protein precipitation steps in advance, thus simplifying the analysis process.

摘要

硼酸亲和吸附剂在从生物基质中富集含有小顺式二醇的分子(顺式二醇)方面具有很大的应用前景。本工作开发了一种受限进入硼酸亲和介孔吸附剂,其中硼酸位点仅分布在介孔的内表面,而外表面是强亲水性层。尽管去除了吸附剂外表面上的硼酸位点,但该吸附剂仍具有较高的结合能力(多巴胺、儿茶酚和腺苷的结合能力分别为 30.3、22.9 和 14.9 mg g)。通过分散固相萃取(d-SPE)方法评估了吸附剂对顺式二醇的吸附特异性,结果表明,该吸附剂可以选择性地从生物样品中提取小顺式二醇,同时完全排除蛋白质。在最佳的 d-SPE 条件下,通过将 d-SPE 与高效液相色谱法相结合,成功分析了人血清中的核苷和顺式二醇药物。其中,四种核苷的检测限在 6.1 至 13.4 ng mL 之间,两种顺式二醇药物的检测限在 24.9 至 34.3 ng mL 之间;所有分析物的相对回收率在 84.1%至 110.1%之间(RSDs <13.4%,n = 6)。结果表明,该吸附剂可以直接处理真实的生物样品,而无需事先进行必要的蛋白质沉淀步骤,从而简化了分析过程。

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