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通过高通量交叉筛选指数富集配体系统进化技术对靶向表面伯氏疏螺旋体蛋白CspZ的DNA适体进行筛选和鉴定

Selection and characterization of DNA aptamers targeting the surface Borrelia protein CspZ with high-throughput cross-over SELEX.

作者信息

Guérin Mickaël, Vandevenne Marylène, Matagne André, Aucher Willy, Verdon Julien, Paoli Emmeline, Ducrotoy Jules, Octave Stéphane, Avalle Bérangère, Maffucci Irene, Padiolleau-Lefèvre Séverine

机构信息

Unité de Génie Enzymatique et Cellulaire (GEC), CNRS UMR 7025, Université de Technologie de Compiègne, 60203, Compiègne, France.

Robotein®, InBioS Research Unit, University of Liège, Building B6, Quartier Agora, Allée du 6 Août, 13, 4000, Liège (Sart-Tilman), Belgium.

出版信息

Commun Biol. 2025 Apr 18;8(1):632. doi: 10.1038/s42003-025-08034-7.

Abstract

Lyme borreliosis (LB) is the most prevalent tick-borne illness, with an estimated 700 000 cases annually in the United States and Europe. The LB diagnosis based on a two-tiered serology remains controversial due to its indirect nature and low sensitivity during the early stage of the disease. Aptamers are single-stranded DNA or RNA oligonucleotides that exhibit high selectivity and specificity for their target due to their unique three-dimensional structure. By applying cross-over-SELEX process, an enrichment of DNA oligonucleotide sequences against a surface protein of Borrelia, named CspZ, has been performed and monitored using absorbance at 260 nm, melting curves and NGS analyses. Beyond sequence enrichment, oligonucleotides binding to CspZ were observed during the selection rounds by Dot Blot and beads assays. Thirteen unique and highly redundant oligonucleotide sequences were further characterized using multiple approaches such as Dot Blot, BioLayer Interferometry and Surface Plasmon Resonance. The selected aptamers showed K values from tens of nanomolar to the micromolar range by BLI and SPR. Two aptamers, Apta9 and Apta10, characterized by flow cytometry and epifluorescence microscopy, were able to specifically recognize Borrelia burgdorferi sensu stricto. This strategy holds promise for the development of an improved diagnostic assay.

摘要

莱姆病(LB)是最常见的蜱传疾病,在美国和欧洲,每年估计有70万例病例。基于两层血清学的莱姆病诊断因其间接性质以及在疾病早期阶段敏感性较低而仍存在争议。适体是单链DNA或RNA寡核苷酸,由于其独特的三维结构,对其靶标具有高选择性和特异性。通过应用交叉SELEX过程,已针对名为CspZ的疏螺旋体表面蛋白进行了DNA寡核苷酸序列的富集,并使用260nm处的吸光度、熔解曲线和NGS分析进行监测。除了序列富集外,在筛选轮次中通过斑点印迹和珠子测定观察到与CspZ结合的寡核苷酸。使用多种方法,如斑点印迹、生物层干涉术和表面等离子体共振,对13个独特且高度冗余的寡核苷酸序列进行了进一步表征。通过BLI和SPR,所选适体的K值在数十纳摩尔至微摩尔范围内。通过流式细胞术和落射荧光显微镜表征的两种适体Apta9和Apta10能够特异性识别狭义伯氏疏螺旋体。该策略有望用于开发改进的诊断测定方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/024a/12008269/efeee4ec5160/42003_2025_8034_Fig1_HTML.jpg

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