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Trapping and proliferation of target cells on C60 fullerene nano fibres

机译:C60富勒烯纳米纤维上靶细胞的诱捕和增殖

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摘要

The ratio of the surface area to the volume of materials increases in inverse proportion to their size and therefore the surface area of nanostructures and nanomaterials is extremely large compared to that of macroscopic materials of the same volume, thanks to which it is supposed that chemical and biochemical reactions may be greatly enhanced and target molecules and cells may be efficiently trapped on the surface of nanomaterials. It is well known that C60 molecules are stable both physically and chemically and the affinity of C60 molecules with biomolecules is rather high. Here, we synthesise fibres composed of C60 and sulphur and immobilise the surface of the fibres with the primary antibody; i.e., epithelial cell adhesion molecules (anti-EpCAM), to trap target cells. The primary antibody is evenly immobilised on the fibres confirmed by a fluorescent secondary antibody attached to the primary one and then TE2 esophageal and DLD-1 colon cancer cells are successfully trapped by the primary antibody immobilised on the fibres thanks to its high affinity with TE2 and DLD-1 cells, whereas few IM9 B lymphoblast cells are captured on the fibres since the affinity of the primary antibody with IM9 cells is extremely low. Furthermore, those cells trapped by the primary antibody immobilised on the fibres proliferate faster than native cells thanks to the primary antibody acting as a growth factor. The present result suggests that different types of cells can be trapped and grown on nano fibres by immobilising appropriate antibody molecules on the surface of the fibres. Even an extremely small number of cells in sample fluids may be analysed and characterised for the detection of diseases such as cancer in the early stage by trapping and proliferating target cells on the fibres.
机译:表面积与材料体积的比值与它们的尺寸成反比,因此,与相同体积的宏观材料相比,纳米结构和纳米材料的表面积非常大。生物化学反应可以大大增强,目标分子和细胞可以有效地捕获在纳米材料的表面。众所周知,C60分子在物理和化学上都是稳定的,并且C60分子与生物分子的亲和力很高。在这里,我们合成了由C60和硫组成的纤维,并用一抗固定了纤维的表面。即上皮细胞粘附分子(anti-EpCAM),以捕获靶细胞。将一抗均匀地固定在纤维上,这是通过附着在一抗上的荧光二抗证实的,然后由于固定在纤维上的一抗与TE2和CD2的亲和力高,成功将TE2食道和DLD-1结肠癌细胞捕获。由于一抗与IM9细胞的亲和力极低,DLD-1细胞却很少捕获IM9 B淋巴母细胞在纤维上。此外,由于一抗作为生长因子,被固定在纤维上的一抗捕获的细胞比天然细胞增殖更快。本结果表明,通过将适当的抗体分子固定在纤维表面上,可以将不同类型的细胞捕获并在纳米纤维上生长。通过在纤维上捕获和增殖靶细胞,甚至可以对样品液中的极少数细胞进行分析和表征,以在早期阶段检测疾病,例如癌症。

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