产生复制缺陷型人类免疫缺陷病毒粒子的诱导细胞系,这些粒子含有以预触发构象稳定的包膜糖蛋白。

IF 4 2区 医学 Q2 VIROLOGY Journal of Virology Pub Date : 2024-11-07 DOI:10.1128/jvi.01720-24
Haitao Ding, Hanh T Nguyen, Wenwei Li, Ashlesha Deshpande, Shijian Zhang, Fan Jiang, Zhiqing Zhang, Saumya Anang, Walther Mothes, Joseph Sodroski, John C Kappes
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引用次数: 0

摘要

在人类免疫缺陷病毒(HIV-1)进入细胞的过程中,病毒表面的包膜糖蛋白(Env)三聚体与宿主细胞受体结合。与受体 CD4 结合会诱导 Env 从预先触发的 "封闭"(状态 1)构象转变为更 "开放"(状态 2/3)的构象。大多数难以诱导的广谱中和抗体(bNAbs)都能识别预触发(状态-1)构象。弱中和抗体(pNAbs)能识别更开放的 Env 构象,这种抗体在自然感染和接种当前 Env 免疫原时很容易被激发出来。Env 的异质性可能会使抗体反应偏离预触发构象,从而导致 HIV-1 持久存在。受感染细胞或病毒表面构象灵活的 gp160 Env 前体可能向宿主免疫系统提供多个 pNAb 表位。虽然蛋白酶裂解产生的功能性成熟 Env 三聚体[(gp120/gp41)3]能稳定状态-1,但许多原生 HIV-1 Env 会自发形成更开放的构象。在这里,我们建立了诱导型细胞系,这些细胞系能产生复制缺陷的 HIV-1 颗粒,其 Env 三聚体稳定在预触发构象中。成熟的 Env 富集在类病毒颗粒(VLPs)上。利用互补方法,我们估计每个 VLP 上平均有 25-50 个 Env 三聚体。Env的稳定变化限制了VLP Env三聚体的天然构象异质性,从而允许bNAbs识别,但不允许pNAbs识别。这些有缺陷的 VLP 为原生膜环境中的预触发 Env 三聚体提供了更均匀的来源。重要意义开发有效的艾滋病毒/艾滋病疫苗的主要障碍是人类免疫缺陷病毒(HIV-1)包膜糖蛋白不能有效地激发中和多种病毒株的抗体。中和抗体能识别包膜糖蛋白的一种特殊形状,这种糖蛋白在病毒进入宿主细胞之前就存在于病毒膜上。在这里,我们报告了诱导产生非感染性 HIV 样颗粒的稳定细胞系的创建情况。这些病毒样颗粒上通常具有弹性的包膜糖蛋白尖峰已被稳定在可被广谱中和抗体识别的构象中。通过这些病毒样颗粒,可以研究包膜糖蛋白的构象、糖对其的修饰及其激发所需中和抗体的能力。
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Inducible cell lines producing replication-defective human immunodeficiency virus particles containing envelope glycoproteins stabilized in a pretriggered conformation.

During the process by which human immunodeficiency virus (HIV-1) enters cells, the envelope glycoprotein (Env) trimer on the virion surface engages host cell receptors. Binding to the receptor CD4 induces Env to undergo transitions from a pretriggered, "closed" (State-1) conformation to more "open" (State 2/3) conformations. Most broadly neutralizing antibodies (bNAbs), which are difficult to elicit, recognize the pretriggered (State-1) conformation. More open Env conformations are recognized by poorly neutralizing antibodies (pNAbs), which are readily elicited during natural infection and vaccination with current Env immunogens. Env heterogeneity likely contributes to HIV-1 persistence by skewing antibody responses away from the pretriggered conformation. The conformationally flexible gp160 Env precursor on the infected cell or virion surface potentially presents multiple pNAb epitopes to the host immune system. Although proteolytic cleavage to produce the functional, mature Env trimer [(gp120/gp41)3] stabilizes State-1, many primary HIV-1 Envs spontaneously sample more open conformations. Here, we establish inducible cell lines that produce replication-defective HIV-1 particles with Env trimers stabilized in a pretriggered conformation. The mature Env is enriched on virus-like particles (VLPs). Using complementary approaches, we estimate an average of 25-50 Env trimers on each VLP. The stabilizing changes in Env limit the natural conformational heterogeneity of the VLP Env trimers, allowing recognition by bNAbs but not pNAbs. These defective VLPs provide a more homogeneous source of pretriggered Env trimers in a native membrane environment. Thus, these VLPs may facilitate the characterization of this functionally important Env conformation and its interaction with the immune system.IMPORTANCEA major impediment to the development of an effective HIV/AIDS vaccine is the inefficiency with which human immunodeficiency virus (HIV-1) envelope glycoproteins elicit antibodies that neutralize multiple virus strains. Neutralizing antibodies recognize a particular shape of the envelope glycoproteins that resides on the viral membrane before the virus engages the host cell. Here, we report the creation of stable cell lines that inducibly produce non-infectious HIV-like particles. The normally flexible envelope glycoprotein spikes on these virus-like particles have been stabilized in a conformation that is recognized by broadly neutralizing antibodies. These virus-like particles allow the study of the envelope glycoprotein conformation, its modification by sugars, and its ability to elicit desired neutralizing antibodies.

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来源期刊
Journal of Virology
Journal of Virology 医学-病毒学
CiteScore
10.10
自引率
7.40%
发文量
906
审稿时长
1 months
期刊介绍: Journal of Virology (JVI) explores the nature of the viruses of animals, archaea, bacteria, fungi, plants, and protozoa. We welcome papers on virion structure and assembly, viral genome replication and regulation of gene expression, genetic diversity and evolution, virus-cell interactions, cellular responses to infection, transformation and oncogenesis, gene delivery, viral pathogenesis and immunity, and vaccines and antiviral agents.
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