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Significance of surface functionalization of Gold Nanorods for reduced effect on IgG stability and minimization of cytotoxicity

机译:金纳米棒表面功能化对于降低对IgG稳定性的影响并最大程度降低细胞毒性的意义

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Gold nanorods (AuNRs) used for biomedical applications could be encountered by biomolecules in the bloodstream, of which IgG is the most abundant antibody. With a view to mitigate their side effect on encountered proteins, the effect of Au concentration (5-40 μM) and functionalization (CTAB-positive;PSS-negative; PEG-neutral) of AuNRs was investigated on the stability of a model protein, IgG (1 μM). Electron microscopic images and particle size analyses indicated least aggregation behavior for PEG-AuNRs, which can be correlated to their neutral charge (from zeta potential analyses) or stearic hindrance of PEG chains. Variations in tryptophan domain were probed by UV-visible absorption and fluorescence quenching studies. Synchronous fluorescence study helped to provide information regarding variations in the hydrophobic region of IgG. The denaturation studies also indicated the stability of AuNR-IgG complex formation. These studies showed that positively charged IgG (pI: 7.8 ± 1.0) was mostly affected by negatively charged PSS-AuNRs and least affected by PEG-AuNRs. This was verified by secondary structural investigations performed using CD and FTIR spectroscopy. For cytotoxicity studies on human lymphocytes, CTAB-AuNRs are known to show higher toxicity compared to PSS-AuNRs and PEG-AuNRs (least). Though PSS-functionalized AuNRs were shown to affect cells to a lesser degree based on the negative charge of cell membrane, they could hamper with positively charged biomolecules in the bloodstream before they reach the target, which must also be considered for choosing the right AuNR functionalization. Thus, this work indicates the effect of different AuNR functionalization on protein and cellular toxicity and stresses the necessity to use neutral particles to mitigate their side effect for theranostic applications.
机译:血液中的生物分子可能会遇到用于生物医学应用的金纳米棒(AuNRs),其中IgG是最丰富的抗体。为了减轻它们对遇到的蛋白质的副作用,研究了AuNRs的Au浓度(5-40μM)和功能化(CTAB阳性; PSS阴性; PEG中性)对模型蛋白质稳定性的影响, IgG(1μM)。电子显微镜图像和粒度分析表明,PEG-AuNRs的聚集行为最少,这可能与它们的中性电荷(来自zeta电位分析)或PEG链的硬位阻有关。色氨酸域的变化通过紫外可见吸收和荧光猝灭研究来探测。同步荧光研究有助于提供有关IgG疏水区域变化的信息。变性研究还表明AuNR-IgG复合物形成的稳定性。这些研究表明,带正电荷的IgG(pI:7.8±1.0)受负电荷PSS-AuNR的影响最大,而受PEG-AuNR的影响最小。通过CD和FTIR光谱进行的二级结构研究证实了这一点。对于人类淋巴细胞的细胞毒性研究,已知CTAB-AuNRs比PSS-AuNRs和PEG-AuNRs毒性更高(最小)。尽管已显示PSS功能化的AuNRs基于细胞膜的负电荷对细胞的影响较小,但它们可能会在到达目标之前阻碍血流中带正电荷的生物分子,因此,选择正确的AuNR功能化也必须考虑。因此,这项工作表明了不同的AuNR功能化对蛋白质和细胞毒性的影响,并强调了使用中性颗粒来减轻其在治疗中的副作用的必要性。

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