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本文引用的文献

1
Global Increases in Human Immunodeficiency Virus Neutralization Sensitivity Due to Alterations in the Membrane-Proximal External Region of the Envelope Glycoprotein Can Be Minimized by Distant State 1-Stabilizing Changes.全球范围内由于包膜糖蛋白膜近端外部区域的改变导致人类免疫缺陷病毒中和敏感性增加,可以通过稳定远距离状态 1 来最小化。
J Virol. 2022 Apr 13;96(7):e0187821. doi: 10.1128/jvi.01878-21. Epub 2022 Mar 15.
2
A multiclade env-gag VLP mRNA vaccine elicits tier-2 HIV-1-neutralizing antibodies and reduces the risk of heterologous SHIV infection in macaques.一种多分支env-gag VLP mRNA疫苗可诱导2级HIV-1中和抗体,并降低猕猴感染异源SHIV的风险。
Nat Med. 2021 Dec;27(12):2234-2245. doi: 10.1038/s41591-021-01574-5. Epub 2021 Dec 9.
3
Altered Env conformational dynamics as a mechanism of resistance to peptide-triazole HIV-1 inactivators.改变的 Env 构象动力学作为对肽-三唑 HIV-1 失活剂产生耐药性的机制。
Retrovirology. 2021 Oct 9;18(1):31. doi: 10.1186/s12977-021-00575-z.
4
Dual Pathways of Human Immunodeficiency Virus Type 1 Envelope Glycoprotein Trafficking Modulate the Selective Exclusion of Uncleaved Oligomers from Virions.人类免疫缺陷病毒 1 包膜糖蛋白的双重运输途径调节未切割寡聚体从病毒粒子中的选择性排除。
J Virol. 2021 Jan 13;95(3). doi: 10.1128/JVI.01369-20.
5
Shedding-Resistant HIV-1 Envelope Glycoproteins Adopt Downstream Conformations That Remain Responsive to Conformation-Preferring Ligands.抗失活的 HIV-1 包膜糖蛋白采用下游构象,这些构象仍然对构象优先配体有反应。
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6
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7
Cryo-EM Structure of Full-length HIV-1 Env Bound With the Fab of Antibody PG16.全长 HIV-1 包膜蛋白与抗体 PG16 的 Fab 片段复合物的冷冻电镜结构
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Asymmetric opening of HIV-1 Env bound to CD4 and a coreceptor-mimicking antibody.HIV-1 Env 与 CD4 和类共受体抗体结合后的不对称开口。
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Vaccination with Glycan-Modified HIV NFL Envelope Trimer-Liposomes Elicits Broadly Neutralizing Antibodies to Multiple Sites of Vulnerability.糖基化修饰的 HIV NFL 包膜三聚体脂质体疫苗诱导针对多个弱点的广谱中和抗体。
Immunity. 2019 Nov 19;51(5):915-929.e7. doi: 10.1016/j.immuni.2019.10.008. Epub 2019 Nov 12.
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Similarities and differences between native HIV-1 envelope glycoprotein trimers and stabilized soluble trimer mimetics.天然 HIV-1 包膜糖蛋白三聚体与稳定可溶性三聚体模拟物之间的相似性和差异。
PLoS Pathog. 2019 Jul 15;15(7):e1007920. doi: 10.1371/journal.ppat.1007920. eCollection 2019 Jul.

富含预触发构象的功能性和高度交联的 HIV-1 包膜糖蛋白。

Functional and Highly Cross-Linkable HIV-1 Envelope Glycoproteins Enriched in a Pretriggered Conformation.

机构信息

Department of Cancer Immunology and Virology, Dana-Farber Cancer Institute, Boston, Massachusetts, USA.

Department of Microbiology, Harvard Medical Schoolgrid.471403.5, Boston, Massachusetts, USA.

出版信息

J Virol. 2022 Apr 27;96(8):e0166821. doi: 10.1128/jvi.01668-21. Epub 2022 Mar 28.

DOI:10.1128/jvi.01668-21
PMID:35343783
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9044932/
Abstract

Binding to the receptor, CD4, drives the pretriggered, "closed" (state-1) conformation of the human immunodeficiency virus type 1 (HIV-1) envelope glycoprotein (Env) trimer into more "open" conformations (states 2 and 3). Broadly neutralizing antibodies, which are elicited inefficiently, mostly recognize the state-1 Env conformation, whereas the more commonly elicited poorly neutralizing antibodies recognize states 2/3. HIV-1 Env metastability has created challenges for defining the state-1 structure and developing immunogens mimicking this labile conformation. The availability of functional state-1 Envs that can be efficiently cross-linked at lysine and/or acidic amino acid residues might assist these endeavors. To that end, we modified HIV-1 Env, which exhibits an intermediate level of triggerability by CD4. We introduced lysine/acidic residues at positions that exhibit such polymorphisms in natural HIV-1 strains. Env changes that were tolerated with respect to gp120-gp41 processing, subunit association, and virus entry were further combined. Two common polymorphisms, Q114E and Q567K, as well as a known variant, A582T, additively rendered pseudoviruses resistant to cold, soluble CD4, and a CD4-mimetic compound, phenotypes indicative of stabilization of the pretriggered state-1 Env conformation. Combining these changes resulted in two lysine-rich HIV-1 Env variants (E.2 and AE.2) with neutralization- and cold-resistant phenotypes comparable to those of natural, less triggerable tier 2/3 HIV-1 isolates. Compared with these and the parental Envs, the E.2 and AE.2 Envs were cleaved more efficiently and exhibited stronger gp120-trimer association in detergent lysates. These highly cross-linkable Envs enriched in a pretriggered conformation should assist characterization of the structure and immunogenicity of this labile state. The development of an efficient vaccine is critical for combating HIV-1 infection worldwide. However, the instability of the pretriggered shape (state 1) of the viral envelope glycoprotein (Env) makes it difficult to raise neutralizing antibodies against HIV-1. Here, by introducing multiple changes in Env, we derived two HIV-1 Env variants that are enriched in state 1 and can be efficiently cross-linked to maintain this shape. These Env complexes are more stable in detergent, assisting their purification. Thus, our study provides a path to a better characterization of the native pretriggered Env, which should assist vaccine development.

摘要

与受体 CD4 结合,促使人类免疫缺陷病毒 1(HIV-1)包膜糖蛋白(Env)三聚体的预触发“关闭”(状态 1)构象转变为更“开放”的构象(状态 2 和 3)。低效诱导产生的广谱中和抗体主要识别状态 1 Env 构象,而更常见的低效中和抗体识别状态 2/3。HIV-1 Env 的不稳定性给定义状态 1 结构和开发模拟这种不稳定构象的免疫原带来了挑战。具有功能的状态 1 Env 的可用性,可以有效地在赖氨酸和/或酸性氨基酸残基处交联,可能有助于这些努力。为此,我们修饰了 HIV-1 Env,它通过 CD4 表现出中等程度的触发能力。我们在天然 HIV-1 株中存在多态性的位置引入了赖氨酸/酸性残基。在 gp120-gp41 加工、亚基缔合和病毒进入方面能够耐受的 Env 变化进一步组合。两个常见的多态性 Q114E 和 Q567K 以及一个已知的变体 A582T,使假病毒对冷、可溶性 CD4 和 CD4 模拟化合物具有抗性,这些表型表明预触发状态 1 Env 构象的稳定性增加。将这些变化结合起来,导致两种富含赖氨酸的 HIV-1 Env 变体(E.2 和 AE.2)具有与天然、触发能力较低的 2/3 层 HIV-1 分离株相当的中和和耐冷表型。与这些变体和亲本 Env 相比,E.2 和 AE.2 Env 在去污剂裂解物中更有效地切割,并表现出更强的 gp120-三聚体结合。这些富含预触发构象的高度可交联 Env 应该有助于研究这种不稳定状态的结构和免疫原性。 开发有效的疫苗对于对抗全球范围内的 HIV-1 感染至关重要。然而,病毒包膜糖蛋白(Env)的预触发形状(状态 1)的不稳定性使得针对 HIV-1 产生中和抗体变得困难。在这里,通过在 Env 中引入多种变化,我们得到了两种富含状态 1 的 HIV-1 Env 变体,它们可以有效地交联以保持这种形状。这些 Env 复合物在去污剂中更稳定,有助于它们的纯化。因此,我们的研究为更好地表征天然预触发 Env 提供了一种途径,这应该有助于疫苗的开发。