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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >HIV-1 antibodies and vaccine antigen selectively interact with lipid domains
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HIV-1 antibodies and vaccine antigen selectively interact with lipid domains

机译:HIV-1抗体和疫苗抗原与脂质结构域选择性相互作用

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The rare, broadly neutralizing antibodies, 4E10 and 2F5, that target the HIV-1 membrane proximal external region also associate with HIV-1 membrane lipids as part of a required first-step in HIV-1 neutralization. HIV-1 virions have high concentration of cholesterol and sphingomyelin, which are able to organize into liquid-ordered domains (i.e., lipid rafts), and could influence the interaction of neutralizing antibodies with epitopes proximal to the membrane. The objective of this research is to understand how these lipid domains contribute to 2F5/4E10 membrane interactions and to antigen presentation in liposomal form of HIV-1 vaccines. To this end we have engineered biomimetic supported lipid bilayers and are able to use atomic force microscopy to visualize membrane domains, antigen clustering, and antibody-membrane interactions. Our results demonstrate that 2F5/4E10 do not interact with highly ordered gel and liquid-ordered domains and exclusively bind to a liquid-disordered lipid phase. This suggests that vaccine liposomes that contain key viral membrane components, such as high cholesterol content, may not be advantageous for 2F5/4E10 vaccine strategies. Rather, vaccine liposomes that primarily contain a liquid-disordered phase may be more likely to elicit production of lipid reactive, 2F5- and 4E10-like antibodies.
机译:靶向HIV-1膜近端外部区域的稀有,广泛中和的抗体4E10和2F5也与HIV-1膜脂质相关联,这是HIV-1中和所需第一步的一部分。 HIV-1病毒体具有高浓度的胆固醇和鞘磷脂,它们能够组织成液体有序域(即脂质筏),并可能影响中和抗体与膜近端表位的相互作用。这项研究的目的是了解这些脂质结构域如何促进2F5 / 4E10膜相互作用以及以脂质体形式的HIV-1疫苗呈递抗原。为此,我们设计了仿生支持的脂质双层,并能够使用原子力显微镜观察膜结构域,抗原簇和抗体-膜相互作用。我们的结果证明2F5 / 4E10不与高度有序的凝胶和液体有序域相互作用,并且仅与液体无序脂质相结合。这表明,含有关键病毒膜成分(例如高胆固醇含量)的疫苗脂质体可能对2F5 / 4E10疫苗策略不利。相反,主要包含液相紊乱相的疫苗脂质体可能更有可能引发脂质反应性2F5和4E10样抗体的产生。

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