Disruption of the HIV-1 Envelope allosteric network blocks CD4-induced rearrangements

Henderson, Rory; Lu, Maolin; Zhou, Ye; Mu, Zekun; Parks, Robert; Han, Qingmei; Hsu, Allen; Carter, Elizabeth; Blanchard, Scott C.; Edwards, R. J.; Wiehe, Kevin; Saunders, Kevin O.; Borgnia, Mario J.; Bartesaghi, Alberto; Mothes, Walther; Haynes, Barton F.; Acharya, Priyamvada; Alam, S. Munir

doi:10.1101/827857

Cited by 5 publications

(10 citation statements)

References 101 publications

(147 reference statements)

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“…A different but related question is whether reducing CD4 binding or CD4induced conformational changes qualitatively improves the immunogenicity of Env by preventing responses to previously cryptic and potentially distractive non-NAb epitopes. Multiple SOSIP trimer variants have been designed and tested for exploring this hypothesis, but although some reductions in non-NAb responses have been observed, they have not been accompanied by major increases in autologous or heterologous NAb titers (Chuang et al, 2017;de Taeye et al, 2015;Henderson et al, 2020;Joyce et al, 2017;Kulp et al, 2017;Ringe et al, 2017;Torrents de la Peñ a et al, 2017;Zhang et al, 2018). Additional research in this area, including attempts to better suppress the immunogenicity of non-NAb neo-epitopes at the base of soluble trimers (Kulp et al, 2017;Ringe et al, 2020), is ongoing.…”

Section: Trimersmentioning

confidence: 99%

Env Exceptionalism: Why Are HIV-1 Env Glycoproteins Atypical Immunogens?

Klasse

Ozorowski

Sanders

et al. 2020

Cell Host & Microbe

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Recombinant HIV-1 envelope (Env) glycoproteins of ever-increasing sophistication have been evaluated as vaccine candidates for over 30 years. Structurally defined mimics of native trimeric Env glycoproteins (e.g., SOSIP trimers) present multiple epitopes for broadly neutralizing antibodies (bNAbs) and their germline precursors, but elicitation of bNAbs remains elusive. Here, we argue that the interactions between Env and the immune system render it exceptional among viral vaccine antigens and hinder its immunogenicity in absolute and comparative terms. In other words, Env binds to CD4 on key immune cells and transduces signals that can compromise their function. Moreover, the extensive array of oligomannose glycans on Env shields peptidic B cell epitopes, impedes the presentation of T helper cell epitopes, and attracts mannose binding proteins, which could affect the antibody response. We suggest lines of research for assessing how to overcome obstacles that the exceptional features of Env impose on the creation of a successful HIV-1 vaccine.

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Section: Trimersmentioning

confidence: 99%

Env Exceptionalism: Why Are HIV-1 Env Glycoproteins Atypical Immunogens?

Klasse

Ozorowski

Sanders

et al. 2020

Cell Host & Microbe

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“…Strategies have been proposed either to stabilize the Env trimer protein in the prefusion closed conformation or to prevent CD4-triggered structural rearrangements (de Taeye et al, 2015;Guenaga et al, 2015; Henderson et al, 2020; Kong et al, 2016; Zhang et al, 2018). We studied nine stabilization designs in CH848 10.17DT Env for expression as modified mRNAs ( Table S1 ).…”

Section: Resultsmentioning

confidence: 99%

“…The Env open conformation exposes non-neutralizing antibody (nnAb) epitopes that can create competition for Env antigen between nnAb and bnAb precursors (Havenar-Daughton et al, 2017; Lee et al, 2021; McGuire et al, 2014). To address the problem of Env trimers opening and the exposure of non-neutralizing epitopes, multiple strategies have been designed to stabilize Env trimers in native-like conformations (de Taeye et al, 2015; Guenaga et al, 2015; Henderson et al, 2020; Kong et al, 2016). We hypothesized that the inclusion of optimal stabilizing mutations will be critical for modified mRNAs to express antigenic and immunogenic Envs, since delivering immunogens directly as mRNA-LNP does not allow for immunogen purification.…”

Section: Introductionmentioning

confidence: 99%

Ability of nucleoside-modified mRNA to encode HIV-1 envelope trimer nanoparticles

Wiehe

Saunders

et al. 2021

Preprint

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The success of nucleoside-modified mRNAs in lipid nanoparticles (mRNA-LNP) as COVID-19 vaccines heralded a new era of vaccine development. For HIV-1, multivalent envelope (Env) trimer protein nanoparticles are superior immunogens compared to trimers alone for priming of broadly neutralizing antibody (bnAb) B cell lineages. The successful expression of complex multivalent nanoparticle immunogens with mRNAs has not been demonstrated. Here we show that mRNAs can encode antigenic Env trimers on ferritin nanoparticles that initiate bnAb precursor B cell expansion and induce serum autologous tier 2 neutralizing activity in bnAb precursor VH + VL knock-in mice. Next generation sequencing demonstrated acquisition of critical mutations, and monoclonal antibodies that neutralized heterologous HIV-1 isolates were isolated. Thus, mRNA-LNP can encode complex immunogens and are of use in design of germline-targeting and sequential boosting immunogens for HIV-1 vaccine development.

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“…The gp41-chimeric SOSIP gp140s were further stabilized by the addition of E64K and A316W mutations 68 . CH505 SOSIP gp140 Envs were expressed as previously described 71 mRNA production. mRNAs were produced as previously described 72 LNP formulation of mRNA.…”

Section: Discussionmentioning

confidence: 99%

Lipid nanoparticle encapsulated nucleoside-modified mRNA vaccines elicit polyfunctional HIV-1 antibodies comparable to proteins in nonhuman primates

Saunders

Pardi

Parks

et al. 2020

Preprint

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Development of an effective AIDS vaccine remains a challenge. Nucleoside-modified mRNAs formulated in lipid nanoparticles (mRNA-LNP) have proved to be a potent mode of immunization against infectious diseases in preclinical studies, and are being tested for SARS-CoV-2 in humans. A critical question is how mRNA-LNP vaccine immunogenicity compares to that of traditional adjuvanted protein vaccines in primates. Here, we found that mRNA-LNP immunization compared to protein immunization elicited either the same or superior magnitude and breadth of HIV-1 Env-specific polyfunctional antibodies. Immunization with mRNA-LNP encoding Zika premembrane and envelope (prM-E) or HIV-1 Env gp160 induced durable neutralizing antibodies for at least 41 weeks. Doses of mRNA-LNP as low as 5 μg were immunogenic in macaques. Thus, mRNA-LNP can be used to rapidly generate single or multi-component vaccines, such as sequential vaccines needed to protect against HIV-1 infection. Such vaccines would be as or more immunogenic than adjuvanted recombinant protein vaccines in primates.

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Disruption of the HIV-1 Envelope allosteric network blocks CD4-induced rearrangements

Cited by 5 publications

References 101 publications

Env Exceptionalism: Why Are HIV-1 Env Glycoproteins Atypical Immunogens?

Env Exceptionalism: Why Are HIV-1 Env Glycoproteins Atypical Immunogens?

Ability of nucleoside-modified mRNA to encode HIV-1 envelope trimer nanoparticles

Lipid nanoparticle encapsulated nucleoside-modified mRNA vaccines elicit polyfunctional HIV-1 antibodies comparable to proteins in nonhuman primates

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