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掺杂吲哚菁绿结合白蛋白的红细胞衍生光学纳米探针:材料特性及癌细胞成像评估

Erythrocyte-Derived Optical Nanoprobes Doped with Indocyanine Green-Bound Albumin: Material Characteristics and Evaluation for Cancer Cell Imaging.

作者信息

Mac Jenny T, Vankayala Raviraj, Patel Dipti K, Wueste Sabrina, Anvari Bahman

出版信息

ACS Biomater Sci Eng. 2018 Aug 13;4(8):3055-3062. doi: 10.1021/acsbiomaterials.8b00621. Epub 2018 Jul 16.

Abstract

Nanosize structures activated by near-infrared (NIR) photoexcitation can provide an optical platform for the image-guided removal of small tumor nodules. We have engineered nanoparticles derived from erythrocytes that can be doped with NIR fluorophore indocyanine green (ICG). We refer to these constructs as NIR erythrocyte-derived transducers (NETs). The objective of this study was to determine if ICG-bound albumin (IbA), as the doping material, could enhance the fluorescence emission of NETs, and evaluate the capability of these nanoprobes in imaging cancer cells. Erythrocytes were isolated from bovine whole blood and depleted of hemoglobin to form erythrocyte ghosts (EGs). EGs were then extruded through nanosize porous membranes in the presence of 10-100 μm ICG or Iba (1:1 molar ratio) to form ICG- or IbA-doped NETs. The resulting nanosize constructs were characterized for their diameters, zeta-potentials, absorption, and fluorescence emission spectra. We used fluorescence microscopic imaging to evaluate the capability of the constructs in imaging SKOV3 ovarian cancer cells. Based on dynamic light-scattering measurements, ICG- and IbA-doped NETs had similar diameter distributions (-average diameter of 236 and 238 nm, respectively) in phosphate-buffered saline supplemented with 10% fetal bovine serum, which remained nearly constant over the course of 2 h at 37 °C. Despite a much-lower loading efficiency of IbA (∼0.7-8%) as compared to ICG (10-45%), the integrated normalized fluorescence emission of IbA-NETs was 2- to 6-fold higher than ICG-doped NETs. IbA-NETs also demonstrated an enhanced capability in fluorescence imaging of SKOV3 ovarian cancer cells, and can serve as potentially effective nanoprobes for the fluorescence imaging of cancerous cells.

摘要

由近红外(NIR)光激发激活的纳米级结构可为图像引导下切除小肿瘤结节提供一个光学平台。我们设计了源自红细胞的纳米颗粒,其可掺杂近红外荧光团吲哚菁绿(ICG)。我们将这些构建体称为近红外红细胞衍生换能器(NETs)。本研究的目的是确定作为掺杂材料的ICG结合白蛋白(IbA)是否能增强NETs的荧光发射,并评估这些纳米探针成像癌细胞的能力。从牛全血中分离出红细胞并去除血红蛋白以形成红细胞影(EGs)。然后在10 - 100μm ICG或Iba(摩尔比1:1)存在的情况下,将EGs通过纳米尺寸的多孔膜挤出,以形成ICG或IbA掺杂的NETs。对所得的纳米级构建体进行直径、zeta电位、吸收和荧光发射光谱表征。我们使用荧光显微镜成像来评估构建体成像SKOV3卵巢癌细胞的能力。基于动态光散射测量,在补充有10%胎牛血清的磷酸盐缓冲盐水中,ICG和IbA掺杂的NETs具有相似的直径分布(平均直径分别为236和238nm),在37℃下2小时的过程中基本保持恒定。尽管与ICG(10 - 45%)相比,IbA的负载效率低得多(约0.7 - 8%),但IbA - NETs的积分归一化荧光发射比ICG掺杂的NETs高2至6倍。IbA - NETs在SKOV3卵巢癌细胞的荧光成像中也表现出增强的能力,并且可作为潜在有效的纳米探针用于癌细胞的荧光成像。

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