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无定形蛋白质寡聚物的生物物理和生物化学性质决定了免疫反应的强度和 T 细胞记忆的产生。

Biophysical and biochemical nature of amorphous protein oligomers determines the strength of immune response and the generation of T-cell memory.

机构信息

Department of Biotechnology and Life Science, Graduate School of Engineering, Tokyo University of Agriculture and Technology, Koganei-shi, Japan.

Institute of Global Innovation Research, Tokyo University of Agriculture and Technology, Fuchu-Shi, Japan.

出版信息

FEBS J. 2023 Oct;290(19):4712-4725. doi: 10.1111/febs.16884. Epub 2023 Jun 21.

DOI:10.1111/febs.16884
PMID:37287403
Abstract

Here, we used domain 3 of dengue virus serotype 3 envelope protein (D3ED3), a natively folded globular low-immunogenicity protein, to ask whether the biophysical nature of amorphous oligomers can affect immunogenicity. We prepared nearly identical 30 ~ 50 nm-sized amorphous oligomers in five distinct ways and looked at any correlation between their biophysical properties and immunogenicity. One oligomer type was produced using our SCP tag (solubility controlling peptide) made of 5 isoleucines (C5I). The others were prepared by miss-shuffling the SS bonds (Ms), heating (Ht), stirring (St) and freeze-thaw (FT). Dynamic light scattering showed that all five formulations contained oligomers of approximately identical sizes with hydrodynamic radii (Rh) between 30 and 55 nm. Circular dichroism (cd) indicated that the secondary structure content of oligomers formed by stirring and freeze-thaw was essentially identical to that of the native monomeric D3ED3. The secondary structure content of the Ms showed moderate changes, whereas the C5I and heat-induced (Ht) oligomers exhibited a significant change. The Ms contained D3ED3 with intermolecular SS bonds as assessed by nonreducing size exclusion chromatography (SEC). Immunization in JcL:ICR mice showed that both C5I and Ms significantly increased the anti-D3ED3 IgG titre. Ht, St and FT were only mildly immunogenic, similar to the monomeric D3ED3. Cell surface CD marker analysis by flow cytometry confirmed that immunization with Ms generated a strong central and effector T-cell memory. Our observations indeed suggest that controlled oligomerization can provide a new, adjuvant-free method for increasing a protein's immunogenicity, yielding a potentially powerful platform for protein-based (subunit) vaccines.

摘要

在这里,我们使用登革热病毒 3 型包膜蛋白(D3ED3)的结构域 3,一种天然折叠的球状低免疫原性蛋白,来探讨无定形寡聚物的生物物理性质是否会影响其免疫原性。我们用五种不同的方法制备了几乎相同的 30 ~ 50nm 大小的无定形寡聚物,并观察了它们的生物物理性质和免疫原性之间的任何相关性。其中一种寡聚物类型是使用我们的 SCP 标签(可溶性控制肽)制备的,该标签由 5 个异亮氨酸(C5I)组成。其他四种则是通过错配 SS 键(Ms)、加热(Ht)、搅拌(St)和冻融(FT)制备的。动态光散射显示,所有五种制剂都含有大小约为 30 ~ 55nm 的寡聚物。圆二色性(cd)表明,搅拌和冻融形成的寡聚物的二级结构含量与天然单体 D3ED3 的二级结构含量基本相同。Ms 寡聚物的二级结构含量显示出适度的变化,而 C5I 和热诱导(Ht)寡聚物则发生了显著的变化。通过非还原的尺寸排阻色谱(SEC)评估,Ms 含有具有分子间 SS 键的 D3ED3。在 JcL:ICR 小鼠中的免疫接种表明,C5I 和 Ms 均显著提高了抗 D3ED3 IgG 滴度。Ht、St 和 FT 仅具有轻度免疫原性,与单体 D3ED3 相似。通过流式细胞术进行的细胞表面 CD 标记分析证实,Ms 免疫产生了强烈的中枢和效应 T 细胞记忆。我们的观察结果确实表明,受控的寡聚化可以为提高蛋白质的免疫原性提供一种新的、无佐剂的方法,为基于蛋白质(亚单位)的疫苗提供了一个潜在的强大平台。

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