Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo

Max Medina-Ramírez; Fernando Garces; Amelia Escolano; Patrick Skog; Steven W. de Taeye; Ivan Del Moral-Sanchez; Andrew T. McGuire; Anila Yasmeen; Anna-Janina Behrens; Gabriel Ozorowski; Tom L.G.M. van den Kerkhof; Natalia T. Freund; Pia Dosenovic; Yuanzi Hua; Alexander D. Gitlin; Albert Cupo; Patricia van der Woude; Michael Golabek; Kwinten Sliepen; Tanya Blane; Neeltje Kootstra; Mari?lle J. van Breemen; Laura K. Pritchard; Robyn L. Stanfield; Max Crispin; Andrew B. Ward; Leonidas Stamatatos; Per Johan Klasse; John P. Moore; David Nemazee; Michel C. Nussenzweig; Ian A. Wilson; Rogier W. Sanders

首页> 外文期刊>The Journal of Experomental Medicine >Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo

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Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo

机译：类似于天然的HIV-1包膜三聚体的设计和晶体结构，在体内可与多种广泛中和的抗体前体结合

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Induction of broadly neutralizing antibodies (bNAbs) by HIV-1 envelope glycoprotein immunogens would be a major advance toward an effective vaccine. A critical step in this process is the activation of naive B cells expressing germline (gl) antibody precursors that have the potential to evolve into bNAbs. Here, we reengineered the BG505 SOSIP.664 glycoprotein to engage gl precursors of bNAbs that target either the trimer apex or the CD4-binding site. The resulting BG505 SOSIP.v4.1-GT1 trimer binds multiple bNAb gl precursors in vitro. Immunization experiments in knock-in mice expressing gl-VRC01 or gl-PGT121 show that this trimer activates B cells in vivo, resulting in the secretion of specific antibodies into the sera. A crystal structure of the gl-targeting trimer at 3.2-? resolution in complex with neutralizing antibodies 35O22 and 9H+109L reveals a native-like conformation and the successful incorporation of design features associated with binding of multiple gl-bNAb precursors.

机译：HIV-1包膜糖蛋白免疫原诱导广泛中和抗体（bNAb）将是朝着有效疫苗迈出的重要一步。该过程中的关键步骤是激活表达具有发展成bNAb潜能的种系（gl）抗体前体的幼稚B细胞。在这里，我们重新设计了BG505 SOSIP.664糖蛋白，使其与靶向三聚体顶点或CD4结合位点的bNAbs的gl前体结合。所得的BG505 SOSIP.v4.1-GT1三聚体在体外与多种bNAb gl gl前体结合。表达gl-VRC01或gl-PGT121的基因敲入小鼠的免疫实验表明，该三聚体在体内激活B细胞，导致特异性抗体分泌到血清中。靶向gl的三聚体的晶体结构为3.2-π。与中和抗体35O22和9H + 109L形成复合体的高分辨率显示了类似天然的构象，并且成功整合了与多种gl-bNAb前体结合相关的设计特征。

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《The Journal of Experomental Medicine 》 |2017年第9期| 共18页
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Max Medina-Ramírez; Fernando Garces; Amelia Escolano; Patrick Skog; Steven W. de Taeye; Ivan Del Moral-Sanchez; Andrew T. McGuire; Anila Yasmeen; Anna-Janina Behrens; Gabriel Ozorowski; Tom L.G.M. van den Kerkhof; Natalia T. Freund; Pia Dosenovic; Yuanzi Hua; Alexander D. Gitlin; Albert Cupo; Patricia van der Woude; Michael Golabek; Kwinten Sliepen; Tanya Blane; Neeltje Kootstra; Mari?lle J. van Breemen; Laura K. Pritchard; Robyn L. Stanfield; Max Crispin; Andrew B. Ward; Leonidas Stamatatos; Per Johan Klasse; John P. Moore; David Nemazee; Michel C. Nussenzweig; Ian A. Wilson; Rogier W. Sanders;
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1. Binding of inferred germline precursors of broadly neutralizing HIV-1 antibodies to native-like envelope trimers [J] . Virology . 2015 ,第Null期

机译：广泛中和的HIV-1抗体的推断种系前体与天然样包膜三聚体的结合
2. Correction: Neutralization-guided design of HIV-1 envelope trimers with high affinity for the unmutated common ancestor of CH235 lineage CD4bs broadly neutralizing antibodies [J] . Celia C. LaBranche, Rory Henderson, Allen Hsu, PLoS Pathogens . 2019 ,第12期

机译：校正：HIV-1包络三聚体的中和引导设计，具有高亲和力的CH235谱系CD4Bs广泛中和抗体的未定义共同祖先
3. Structure-based design of native-like HIV-1 envelope trimers to silence non-neutralizing epitopes and eliminate CD4 binding [J] . Daniel W. Kulp, Jon M. Steichen, Matthias Pauthner, Nature Communications . 2017 ,第1期

机译：基于结构的天然样HIV-1包膜三聚体的设计可沉默非中和抗原决定簇并消除CD4结合
4. Synthesis of HIV Gp41 Trimer Mimics Inducing Neutralizing Antibodies Based on Remodeling of Dynamic Structures of HIV-1 Envelope Proteins [C] . Wataru Nomera, Toru Nakahara, Chie Hashimoto American Peptide Symposium . 2011

机译：基于HIV-1包络蛋白动态结构的重塑诱导中和抗体的HIV GP41三聚体模拟物的合成
5. Selection and Analysis of HIV-1 Envelope Epitopes for Design of Vaccines that can Induce Broadly Neutralizing Antibodies [D] . Wieczorek, Lindsay 2012

机译：HIV-1包膜抗原决定簇的选择和分析，用于设计可诱导广泛中和抗体的疫苗
6. Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo [O] . Max Medina-Ramírez, Fernando Garces, Amelia Escolano, 2017

机译：类似于天然的HIV-1包膜三聚体的设计和晶体结构在体内可与多种广泛中和的抗体前体结合
7. Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo [O] . Medina-Ramírez, Max, Garces, Fernando, Escolano, Amelia, 2017

机译：类似于天然的HIV-1包膜三聚体的设计和晶体结构，在体内可与多种广泛中和的抗体前体结合

Design and crystal structure of a native-like HIV-1 envelope trimer that engages multiple broadly neutralizing antibody precursors in vivo

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