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疏螺旋体脂蛋白在脑膜炎球菌外膜囊泡上的表面展示。

Surface display of a borrelial lipoprotein on meningococcal outer membrane vesicles.

作者信息

Salverda Merijn L M, Meinderts Sanne M, Hamstra Hendrik-Jan, Wagemakers Alex, Hovius Joppe W R, van der Ark Arno, Stork Michiel, van der Ley Peter

机构信息

Institute for Translational Vaccinology (InTraVacc), Antonie van Leeuwenhoeklaan 9, 3721 MA Bilthoven, The Netherlands.

Institute for Translational Vaccinology (InTraVacc), Antonie van Leeuwenhoeklaan 9, 3721 MA Bilthoven, The Netherlands.

出版信息

Vaccine. 2016 Feb 17;34(8):1025-33. doi: 10.1016/j.vaccine.2016.01.019. Epub 2016 Jan 19.

Abstract

Outer Membrane Vesicles (OMVs) are gaining attention as vaccine candidates. The successful expression of heterologous antigens in OMVs, with the OMV functioning both as adjuvant and delivery vehicle, has greatly enhanced their vaccine potential. Since there are indications that surface exposed antigens might induce a superior immune response, targeting of heterologous antigens to the OMV surface is of special interest. Several systems for surface display of heterologous antigens on OMVs have been developed. However, these systems have not been used to display lipidated membrane-associated proteins known as lipoproteins, which are emerging as key targets for protective immunity. We were therefore interested to see whether we could express a foreign lipoprotein on the outer surface of OMVs. When outer surface protein A (OspA), a borrelial surface-exposed lipoprotein, was expressed in meningococci, it was found that although OspA was present in OMVs, it was no longer surface-exposed. Therefore, a set of fusions of OspA to different regions of factor H binding protein (fHbp), a meningococcal surface-exposed lipoprotein, were designed and tested for their surface-exposure. An N-terminal part of fHbp was found to be necessary for the successful surface display of OspA on meningococcal OMVs. When mice were immunized with this set of OMVs, an OspA-specific antibody response was only elicited by OMVs with clearly surface-exposed OspA, strengthening the idea that the exact positioning of an antigen in the OMV affects the immune response. This method for the surface display of heterologous lipoproteins on OMVs is a step forward in the development of OMVs as a vaccine platform.

摘要

外膜囊泡(OMV)作为候选疫苗正受到越来越多的关注。在OMV中成功表达异源抗原,且OMV同时作为佐剂和递送载体,极大地增强了它们的疫苗潜力。由于有迹象表明表面暴露的抗原可能诱导更强的免疫反应,将异源抗原靶向至OMV表面备受关注。已经开发了几种在OMV上表面展示异源抗原的系统。然而,这些系统尚未用于展示被称为脂蛋白的脂化膜相关蛋白,而脂蛋白正成为保护性免疫的关键靶点。因此,我们感兴趣的是能否在OMV的外表面表达一种外源脂蛋白。当疏螺旋体表面暴露的脂蛋白外表面蛋白A(OspA)在脑膜炎球菌中表达时,发现尽管OspA存在于OMV中,但它不再暴露于表面。因此,设计了一组OspA与脑膜炎球菌表面暴露的脂蛋白因子H结合蛋白(fHbp)不同区域的融合体,并测试它们的表面暴露情况。发现fHbp的N端部分对于OspA在脑膜炎球菌OMV上成功进行表面展示是必需的。当用这组OMV免疫小鼠时,只有具有明显表面暴露OspA的OMV引发了OspA特异性抗体反应,这强化了抗原在OMV中的精确定位会影响免疫反应的观点。这种在OMV上表面展示异源脂蛋白的方法是将OMV开发为疫苗平台的一个进步。

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