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Insight into the cellular fate and toxicity of aluminium adjuvants used in clinically approved human vaccinations

机译:了解临床批准的人类疫苗接种中铝佐剂的细胞命运和毒性

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Aluminium adjuvants remain the most widely used and effective adjuvants in vaccination and immunotherapy. Herein, the particle size distribution (PSD) of aluminium oxyhydroxide and aluminium hydroxyphosphate adjuvants was elucidated in attempt to correlate these properties with the biological responses observed post vaccination. Heightened solubility and potentially the generation of Al(3+) in the lysosomal environment were positively correlated with an increase in cell mortality in vitro, potentially generating a greater inflammatory response at the site of simulated injection. The cellular uptake of aluminium based adjuvants (ABAs) used in clinically approved vaccinations are compared to a commonly used experimental ABA, in an in vitro THP-1 cell model. Using lumogallion as a direct-fluorescent molecular probe for aluminium, complemented with transmission electron microscopy provides further insight into the morphology of internalised particulates, driven by the physicochemical variations of the ABAs investigated. We demonstrate that not all aluminium adjuvants are equal neither in terms of their physical properties nor their biological reactivity and potential toxicities both at the injection site and beyond. High loading of aluminium oxyhydroxide in the cytoplasm of THP-1 cells without immediate cytotoxicity might predispose this form of aluminium adjuvant to its subsequent transport throughout the body including access to the brain.
机译:铝佐剂仍然是疫苗接种和免疫疗法中使用最广泛和最有效的佐剂。在此,阐明羟基氧化铝和羟基磷酸铝佐剂的粒度分布(PSD),以试图使这些性质与疫苗接种后观察到的生物学反应相关。溶酶体环境中的增加的溶解度和潜在的Al(3+)的产生与体外细胞死亡率的增加呈正相关,可能在模拟注射部位产生更大的炎症反应。在体外THP-1细胞模型中,将临床批准的疫苗接种中使用的铝基佐剂(ABA)的细胞吸收与常用实验ABA进行了比较。使用lumogallion作为铝的直接荧光分子探针,辅以透射电子显微镜,可以进一步深入了解由研究的ABA的物理化学变化驱动的内在化颗粒形态。我们证明并非所有的铝佐剂在注射部位和注射部位以外的物理性质,生物学反应性和潜在毒性都不相同。 THP-1细胞的细胞质中高含量的羟基氧化铝没有立即的细胞毒性,这可能会使这种形式的铝佐剂易于随后转移到全身,包括进入大脑。

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