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通过含氟聚糖配体将亲和力和选择性引入半乳糖凝集素靶向纳米颗粒。

Introducing affinity and selectivity into galectin-targeting nanoparticles with fluorinated glycan ligands.

作者信息

Richards Sarah-Jane, Keenan Tessa, Vendeville Jean-Baptiste, Wheatley David E, Chidwick Harriet, Budhadev Darshita, Council Claire E, Webster Claire S, Ledru Helene, Baker Alexander N, Walker Marc, Galan M Carmen, Linclau Bruno, Fascione Martin A, Gibson Matthew I

机构信息

Department of Chemistry, University of Warwick CV4 7AL UK

Department of Chemistry, University of York Heslington York YO10 5DD UK

出版信息

Chem Sci. 2020 Nov 16;12(3):905-910. doi: 10.1039/d0sc05360k.

Abstract

Galectins are potential biomarkers and therapeutic targets. However, galectins display broad affinity towards β-galactosides meaning glycan-based (nano)biosensors lack the required selectivity and affinity. Using a polymer-stabilized nanoparticle biosensing platform, we herein demonstrate that the specificity of immobilised lacto--biose towards galectins can be 'turned on/off' by using site-specific glycan fluorination and in some cases reversal of specificity can be achieved. The panel of fluoro-glycans were obtained by a chemoenzymatic approach, exploiting BiGalK and BiGalHexNAcP enzymes from which are shown to tolerate fluorinated glycans, introducing structural diversity which would be very laborious by chemical methods alone. These results demonstrate that integrating non-natural, fluorinated glycans into nanomaterials can encode unprecedented selectivity with potential applications in biosensing.

摘要

半乳糖凝集素是潜在的生物标志物和治疗靶点。然而,半乳糖凝集素对β-半乳糖苷表现出广泛的亲和力,这意味着基于聚糖的(纳米)生物传感器缺乏所需的选择性和亲和力。在此,我们使用聚合物稳定的纳米颗粒生物传感平台证明,通过位点特异性聚糖氟化,可以“开启/关闭”固定化乳糖对半乳糖凝集素的特异性,并且在某些情况下可以实现特异性的逆转。通过化学酶法获得了一系列氟代聚糖,利用了BiGalK和BiGalHexNAcP酶,结果表明这些酶能够耐受氟化聚糖,引入了结构多样性,而仅靠化学方法获得这种多样性将非常费力。这些结果表明,将非天然的氟化聚糖整合到纳米材料中可以编码前所未有的选择性,在生物传感方面具有潜在应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e011/8179109/7755d771ecc5/d0sc05360k-f1.jpg

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