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多孔 YAG:Nd3+ 纤维,在人类“近红外光学窗口”中具有激发和发射,可用作发光药物载体。

Porous YAG:Nd3+ fibers with excitation and emission in the human "NIR optical window" as luminescent drug carriers.

机构信息

Key Laboratory of Specially Functional Materials of Ministry of Education and Institute of Optical Communication Materials, South China University of Technology, Guangzhou 510640, PR China.

出版信息

Chemistry. 2012 Feb 27;18(9):2609-16. doi: 10.1002/chem.201101262. Epub 2012 Jan 23.

Abstract

The design and preparation of luminescent drug carriers has been a prosperous area of research for many years. However, the excitation and/or emission wavelength of such luminescent drug carriers haven't been optimized in the so-called human "near infrared (NIR) optical window", thus restricting their practical applications. Herein, we report the synthesis of electrospun porous YAG:Nd(3+) (neodymium-doped yttrium aluminum garnet) fibers with both excitation and emission in the "NIR optical window" as luminescent drug carriers. The YAG:Nd(3+) porous fibers were characterized by SEM, TEM, XRD, scanning transmission electron microscopy-energy-dispersive X-ray spectroscopy (STEM-EDX), and photoluminescence (PL). Ibuprofen (IBU) was used as a model drug to evaluate the drug-loading capacities and release profiles of the samples. BMSCs (bone mesenchymal stem cells) were used as model human cells to investigate cytotoxicity. Our results indicated that the YAG:Nd(3+) fibers possessed a fine, irregularly porous fibrous morphology with an average diameter of 378 nm. The florescence of the sample (1064 nm) could be excited over a wide wavelength range in the NIR region. During the release process of IBU in simulated body fluid (SBF), along with the dissolving of the drug, the solvent entered into the pores, and the emission intensity of the YAG:Nd(3+) fibers at 1064 nm decreased gradually, owing to a quenching effect of the hydroxy groups, thus provided an approach to track and monitor drug release. In addition, cytotoxicity investigations revealed that these YAG:Nd(3+) fibers were biocompatible with human cells. Consequently, the porous YAG:Nd(3+) fibers are a promising material for applications as advanced drug carriers.

摘要

多年来,制备发光药物载体一直是一个热门的研究领域。然而,此类发光药物载体的激发和/或发射波长并未在所谓的“人近红外(NIR)光学窗口”中得到优化,从而限制了它们的实际应用。在此,我们报告了具有激发和发射均在“NIR 光学窗口”中的电纺多孔 YAG:Nd(3+)(掺钕的钇铝石榴石)纤维的合成,可作为发光药物载体。通过 SEM、TEM、XRD、扫描透射电子显微镜-能量色散 X 射线光谱(STEM-EDX)和光致发光(PL)对 YAG:Nd(3+)多孔纤维进行了表征。以布洛芬(IBU)为模型药物,评估了样品的载药量和释放曲线。BMSCs(骨髓间充质干细胞)用作模型人细胞来研究细胞毒性。结果表明,YAG:Nd(3+)纤维具有精细、不规则多孔纤维形态,平均直径为 378nm。该样品的荧光(1064nm)可以在 NIR 区域的宽波长范围内被激发。在模拟体液(SBF)中 IBU 的释放过程中,随着药物的溶解,溶剂进入到孔中,YAG:Nd(3+)纤维在 1064nm 处的发射强度逐渐降低,这是由于羟基的猝灭效应,从而提供了一种跟踪和监测药物释放的方法。此外,细胞毒性研究表明,这些 YAG:Nd(3+)纤维与人细胞具有生物相容性。因此,多孔 YAG:Nd(3+)纤维是作为先进药物载体的有前途的材料。

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