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氢氧化铝凝胶佐剂、超声分散和蛋白结合:TEM 和分析研究。

Alhydrogel® adjuvant, ultrasonic dispersion and protein binding: a TEM and analytical study.

机构信息

Institute for Cell and Molecular Biosciences, Newcastle University, Newcastle upon Tyne NE2 4HH, UK.

出版信息

Micron. 2012 Feb;43(2-3):192-200. doi: 10.1016/j.micron.2011.07.012. Epub 2011 Jul 27.

DOI:10.1016/j.micron.2011.07.012
PMID:21831642
Abstract

Aluminium-based vaccine adjuvants have been in use since the 1920s. Aluminium hydroxide (alum) that is the chemical basis of Alhydrogel, a widely used adjuvant, is a colloid that binds proteins to the particular surface for efficient presentation to the immune system during the vaccination process. Using conventional TEM and cryo-TEM we have shown that Alhydrogel can be finely dispersed by ultrasonication of the aqueous suspension. Clusters of ultrasonicated aluminium hydroxide micro-fibre crystals have been produced (∼ 10-100 nm), that are significantly smaller than those present the untreated Alhydrogel (∼ 2-12 μm). However, even prolonged ultrasonication did not produce a homogenous suspension of single aluminium hydroxide micro-fibres. The TEM images of unstained and negatively stained air-dried Alhydrogel are very similar to those obtained by cryo-electron microscopy. Visualization of protein on the surface of the finely dispersed Alhydrogel by TEM is facilitated by prior ultrasonication. Several examples are given, including some of medical relevance, using proteins of widely ranging molecular mass and oligomerization state. Even with the smaller mass proteins, their presence on the Alhydrogel surface can be readily defined by TEM. It has been found that low quantities of protein tend to cross-link and aggregate the small Alhydogel clusters, in a more pronounced manner than high protein concentrations. This indicates that complete saturation of the available Alhydrogel surface with protein may be achieved, with minimal cross-linkage, and future exploitation of this treatment of Alhydrogel is likely to be of immediate value for more efficient vaccine production.

摘要

铝基疫苗佐剂自 20 世纪 20 年代以来就一直在使用。作为广泛使用的佐剂 Alhydrogel 的化学基础的氢氧化铝(明矾)是一种胶体,可在疫苗接种过程中将蛋白质结合到特定表面,从而有效地呈递给免疫系统。我们使用常规 TEM 和 cryo-TEM 表明,通过对水悬浮液进行超声处理可以精细分散 Alhydrogel。已经产生了(∼ 10-100nm)簇状超声处理的氢氧化铝微纤维晶体,其尺寸明显小于未处理的 Alhydrogel 中存在的晶体(∼ 2-12μm)。然而,即使长时间超声处理也没有产生单氢氧化铝微纤维的均匀悬浮液。未染色和负染色空气干燥 Alhydrogel 的 TEM 图像与通过 cryo-电子显微镜获得的图像非常相似。通过 TEM 观察经精细分散的 Alhydrogel 表面上的蛋白质,通过预先超声处理可得到促进。提供了几个示例,包括一些具有广泛分子质量和寡聚状态的蛋白质,即使对于较小质量的蛋白质,也可以通过 TEM 轻松定义其在 Alhydrogel 表面上的存在。已经发现,少量的蛋白质倾向于交联和聚集较小的 Alhydogel 簇,其程度比高蛋白质浓度更为明显。这表明可以通过 TEM 实现最小交联,以最小的交叉连接方式使可用的 Alhydrogel 表面完全饱和蛋白质,并且未来对 Alhydrogel 的这种处理的开发可能会立即对更有效的疫苗生产产生价值。

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