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用于体外和体内捕获循环生物标志物的聚碳酸酯微器件的表面修饰和表征。

Surface modification and characterization of polycarbonate microdevices for capture of circulating biomarkers, both in vitro and in vivo.

机构信息

The University of Queensland , Australian Institute for Bioengineering and Nanotechnology, Delivery of Drugs and Genes Group (D2G2), St Lucia, Brisbane, Queensland, Australia , 4072.

出版信息

Anal Chem. 2013 Nov 5;85(21):10196-204. doi: 10.1021/ac402942x. Epub 2013 Oct 21.

Abstract

Herein, we report the fabrication, characterization, and testing of a polymer microprojection array, for the direct and selective capture of circulating biomarkers from the skin of live mice. First, we modified polycarbonate wafers using an electrophilic aromatic substitution reaction with nitric acid to insert aromatic nitro-groups into the benzene rings, followed by treatment with sodium borohydride to reduce the nitro-groups to primary amines. Initial characterization by ultraviolet-visible (UV-vis) spectroscopy suggested that increasing acid concentration led to increased depth of material modification and that this was associated with decreased surface hardness and slight changes in surface roughness. Chemical analysis with X-ray photoelectron spectroscopy (XPS) and attenuated total reflectance fourier transform infrared (ATR-FT-IR) spectroscopy showed nitrogen species present at the surface for all acid concentrations used, but subsurface nitrogen species were only observed at acid concentrations >35%. The nitrogen species were identified as a mixture of nitro, imine, and amine groups, and following reduction, there was sufficient amounts of primary amine groups for covalent attachment of a polyethylene glycol antifouling layer and protein capture probes, as determined by colorimetric and radiometric assays. Finally, the modification scheme was applied to polycarbonate microprojection arrays, and we show that these devices achieve flank skin penetration depths and biomarker yields comparable with our previously reported gold-coated silicon arrays, with very low nonspecific binding even in 10% mouse serum (in vitro) or directly in mouse skin (in vivo). This study is the first demonstration showing the potential utility of polymer microprojections in immunodiagnostics applications.

摘要

在此,我们报告了一种聚合物微针阵列的制造、表征和测试,用于直接和选择性地从活体小鼠皮肤中捕获循环生物标志物。首先,我们使用硝酸的亲电芳香取代反应对聚碳酸酯晶片进行修饰,将芳香硝基基团插入苯环中,然后用硼氢化钠处理将硝基基团还原为伯胺。紫外-可见(UV-vis)光谱的初步表征表明,增加酸浓度会导致材料修饰的深度增加,而这与表面硬度降低和表面粗糙度略有变化有关。X 射线光电子能谱(XPS)和衰减全反射傅里叶变换红外(ATR-FT-IR)光谱的化学分析表明,所有使用的酸浓度下表面都存在含氮物质,但仅在酸浓度>35%时才观察到次表面含氮物质。氮物种被鉴定为硝基、亚胺和胺基团的混合物,并且在还原后,存在足够数量的伯胺基团用于共价连接聚乙二醇抗污层和蛋白质捕获探针,这通过比色和放射性测定来确定。最后,将修饰方案应用于聚碳酸酯微针阵列,我们表明这些器件可实现侧翼皮肤穿透深度和生物标志物产量与我们之前报道的金涂硅阵列相当,即使在 10%的小鼠血清(体外)或直接在小鼠皮肤(体内)中,非特异性结合也非常低。这项研究首次证明了聚合物微针在免疫诊断应用中的潜在用途。

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