稳定突变对膜表达的 HIV-1 包膜糖蛋白的抗原表位和糖基化的影响。

Impact of stabilizing mutations on the antigenic profile and glycosylation of membrane-expressed HIV-1 envelope glycoprotein.

机构信息

San Diego Biomedical Research Institute, San Diego, California, United States of America.

School of Biological Sciences, University of Southampton, Southampton, United Kingdom.

出版信息

PLoS Pathog. 2023 Aug 7;19(8):e1011452. doi: 10.1371/journal.ppat.1011452. eCollection 2023 Aug.

DOI:10.1371/journal.ppat.1011452

PMID:37549185

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10434953/

Abstract

Recent HIV-1 vaccine development has centered on "near native" soluble envelope glycoprotein (Env) trimers that are artificially stabilized laterally (between protomers) and apically (between gp120 and gp41). These mutations have been leveraged for use in membrane-expressed Env mRNA vaccines, although their effects in this context are unclear. To address this question, we used virus-like particle (VLP) produced in 293T cells. Uncleaved (UNC) trimers were laterally unstable upon gentle lysis from membranes. However, gp120/gp41 processing improved lateral stability. Due to inefficient gp120/gp41 processing, UNC is incorporated into VLPs. A linker between gp120 and gp41 neither improved trimer stability nor its antigenic profile. An artificially introduced enterokinase cleavage site allowed post-expression gp120/gp41 processing, concomitantly increasing trimer stability. Gp41 N-helix mutations I559P and NT1-5 imparted lateral trimer stability, but also reduced gp120/gp41 processing and/or impacted V2 apex and interface NAb binding. I559P consistently reduced recognition by HIV+ human plasmas, further supporting antigenic differences. Mutations in the gp120 bridging sheet failed to stabilize membrane trimers in a pre-fusion conformation, and also reduced gp120/gp41 processing and exposed non-neutralizing epitopes. Reduced glycan maturation and increased sequon skipping were common side effects of these mutations. In some cases, this may be due to increased rigidity which limits access to glycan processing enzymes. In contrast, viral gp120 did not show glycan skipping. A second, minor species of high mannose gp160 was unaffected by any mutations and instead bypasses normal folding and glycan maturation. Including the full gp41 cytoplasmic tail led to markedly reduced gp120/gp41 processing and greatly increased the proportion of high mannose gp160. Remarkably, monoclonal antibodies were unable to bind to this high mannose gp160 in native protein gels. Overall, our findings suggest caution in leveraging stabilizing mutations in nucleic acid-based immunogens to ensure they impart valuable membrane trimer phenotypes for vaccine use.

摘要

最近的 HIV-1 疫苗研发集中在“接近天然”的可溶性包膜糖蛋白（Env）三聚体上，这些三聚体在侧向（在原聚体之间）和顶端（在 gp120 和 gp41 之间）被人为稳定。这些突变已被用于膜表达的 Env mRNA 疫苗中，尽管其在这种情况下的作用尚不清楚。为了解决这个问题，我们使用 293T 细胞中产生的病毒样颗粒（VLP）。在从膜温和裂解时，未切割（UNC）三聚体在侧向不稳定。然而，gp120/gp41 的加工改善了侧向稳定性。由于 gp120/gp41 的加工效率低下，UNC 被掺入 VLP 中。gp120 和 gp41 之间的连接子既没有改善三聚体稳定性，也没有改善其抗原表位。在 gp120 中人为引入肠激酶切割位点允许 gp120/gp41 加工后表达，同时增加三聚体稳定性。gp41 N 螺旋突变 I559P 和 NT1-5 赋予侧向三聚体稳定性，但也降低了 gp120/gp41 的加工和/或影响 V2 顶点和界面 NAb 结合。I559P 始终降低了 HIV+ 人类血浆的识别，进一步支持了抗原差异。gp120 桥接片上的突变未能使融合前构象中的膜三聚体稳定，并且还降低了 gp120/gp41 的加工和暴露非中和表位。糖基化成熟减少和顺式切割增加是这些突变的常见副作用。在某些情况下，这可能是由于增加的刚性限制了糖基化加工酶的进入。相比之下，病毒 gp120 没有显示糖基化跳跃。第二种次要的高甘露糖 gp160 形式不受任何突变的影响，而是绕过正常折叠和糖基化成熟。包含全长 gp41 细胞质尾巴会导致 gp120/gp41 的加工大大减少，并大大增加高甘露糖 gp160 的比例。值得注意的是，单克隆抗体无法在天然蛋白凝胶中结合这种高甘露糖 gp160。总的来说，我们的研究结果表明，在利用核酸免疫原中的稳定突变时要谨慎，以确保它们赋予有价值的膜三聚体表型用于疫苗接种。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/983e/10434953/85c3947c4b60/ppat.1011452.g001.jpg

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稳定突变对膜表达的 HIV-1 包膜糖蛋白的抗原表位和糖基化的影响。

Impact of stabilizing mutations on the antigenic profile and glycosylation of membrane-expressed HIV-1 envelope glycoprotein.

机构信息

San Diego Biomedical Research Institute, San Diego, California, United States of America.

School of Biological Sciences, University of Southampton, Southampton, United Kingdom.

出版信息

PLoS Pathog. 2023 Aug 7;19(8):e1011452. doi: 10.1371/journal.ppat.1011452. eCollection 2023 Aug.

DOI:10.1371/journal.ppat.1011452

PMID:37549185

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10434953/

Abstract

摘要

稳定突变对膜表达的 HIV-1 包膜糖蛋白的抗原表位和糖基化的影响。

Impact of stabilizing mutations on the antigenic profile and glycosylation of membrane-expressed HIV-1 envelope glycoprotein.

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稳定突变对膜表达的 HIV-1 包膜糖蛋白的抗原表位和糖基化的影响。

Impact of stabilizing mutations on the antigenic profile and glycosylation of membrane-expressed HIV-1 envelope glycoprotein.

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