Analysis of Memory B Cell Responses and Isolation of Novel Monoclonal Antibodies with Neutralizing Breadth from HIV-1-Infected Individuals

Corti, Davide; Langedijk, Johannes P. M.; Hinz, Andreas; Seaman, Michael S.; Vanzetta, Fabrizia; Fernandez-Rodriguez, Blanca; Silacci, Chiara; Pinna, Debora; Jarrossay, David; Balla-Jhagjhoorsingh, Sunita S.; Willems, Betty; Zekveld, Maria J.; Dreja, Hanna; O'Sullivan, Eithne; Pade, Corinna; Orkin, Chloe; Jeffs, Simon A.; Montefiori, David C.; Davis, David A.; Weissenhorn, Winfríed; McKnight, Áine; Heeney, Jonathan L.; Sallusto, Federica; Sattentau, Quentin J.; Weiss, Robin A.; Lanzavecchia, Antonio

doi:10.1371/journal.pone.0008805

Cited by 407 publications

(432 citation statements)

References 74 publications

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“…Nevertheless, the differential ability of KNH1144 and JR-FL trimers to bind antibodies such as 17b could be useful for immunogen design, and variant gp140 trimers preferentially stabilized in distinct intermediate states could potentially be engineered and then mixed to create a composite vaccine, with the goal of increasing the breadth of the neutralizing antibody response. Any variations in the extent to which different regions on gp120 and gp41 are accessible in the open state may also increase the likelihood of inducing broadly neutralizing antibodies, such as b12 (23), PG9/16 (24), VRC01 (25), or HJ16 (26).…”

Section: Discussionmentioning

confidence: 99%

Trimeric HIV-1 glycoprotein gp140 immunogens and native HIV-1 envelope glycoproteins display the same closed and open quaternary molecular architectures

Harris

Borgnia

Shi

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

144

180

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The initial step in HIV-1 infection occurs with the binding of cell surface CD4 to trimeric HIV-1 envelope glycoproteins (Env), a heterodimer of a transmembrane glycoprotein (gp41) and a surface glycoprotein (gp120). The design of soluble versions of trimeric Env that display structural and functional properties similar to those observed on intact viruses is highly desirable from the viewpoint of designing immunogens that could be effective as vaccines against HIV/AIDS. Using cryoelectron tomography combined with subvolume averaging, we have analyzed the structure of SOSIP gp140 trimers, which are cleaved, solubilized versions of the ectodomain of trimeric HIV-1 Env. We show that unliganded gp140 trimers adopt a quaternary arrangement similar to that displayed by native unliganded trimers on the surface of intact HIV-1 virions. When complexed with soluble CD4, Fab 17b, which binds to gp120 at its chemokine coreceptor binding site, or both soluble CD4 and 17b Fab, gp140 trimers display an open conformation in which there is an outward rotation and displacement of each gp120 protomer. We demonstrate that the molecular arrangements of gp120 trimers in the closed and open conformations of the soluble trimer are the same as those observed for the closed and open states, respectively, of trimeric gp120 on intact HIV-1 BaL virions, establishing that soluble gp140 trimers can be designed to mimic the quaternary structural transitions displayed by native trimeric Env. viral entry | cryoelectron microscopy | HIV spike | HIV vaccine | AIDS vaccine

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Section: Discussionmentioning

confidence: 99%

Trimeric HIV-1 glycoprotein gp140 immunogens and native HIV-1 envelope glycoproteins display the same closed and open quaternary molecular architectures

Harris

Borgnia

Shi

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

144

180

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“…This bnAb, in contrast to VRC01, does not induce conformational changes in gp120 upon binding 25. Many additional CD4‐binding site bnAbs were isolated using RSC356 or other Env baits40 and one by EBV immortalization of B cells followed by an ELISA‐based binding screen 75. Structural studies have enabled comparison of the CD4‐binding site bnAbs and the definition of two subclasses: those that bind predominantly using their CDRH3 and those that are genetically restricted and use either the VH1‐2 or VH1‐46 V gene 76.…”

Section: Specificity Of Hiv Bnabsmentioning

confidence: 99%

Identification and specificity of broadly neutralizing antibodies against HIV

McCoy

Burton

2017

Immunological Reviews

204

193

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SummaryBeginning in 2009, studies of the humoral responses of HIV‐positive individuals have led to the identification of scores, if not hundreds, of antibodies that are both broadly reactive and potently neutralizing. This development has provided renewed impetus toward an HIV vaccine and led directly to the development of novel immunogens. Advances in identification of donors with the most potent and broad anti‐HIV serum neutralizing responses were crucial in this effort. Equally, development of methods for the rapid generation of human antibodies from these donors was pivotal. Primarily these methods comprise single B‐cell culture coupled to high‐throughput neutralization screening and flow cytometry‐based sorting of single B cells using HIV envelope protein baits. In this review, the advantages and disadvantages of these methodologies are discussed in the context of the specificities targeted by individual antibodies and the need for further improvements to evaluate HIV vaccine candidates.

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“…VRC01 and CH31) and 8ANC131-class of bnAbs that use V H 1-46 (e.g.8ANC131 and CH235) (16, 18,26,27,33,42, 43). In contrast, the variable heavy third complementarity determining region (CDR H3)-binder -class of CD4bs bnAbs, such as CH103, HJ16 and CH98 bnAbs, use multiple V H genes (17, 21, 42, 44). …”

Section: Characteristics Of Broadly Neutralizing Antibodiesmentioning

confidence: 99%

Antibody‐virus co‐evolution in HIV infection: paths for HIV vaccine development

Bonsignori

Liao

Gao

et al. 2017

Immunological Reviews

Self Cite

156

150

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Summary Induction of HIV-1 broadly neutralizing antibodies (bnAbs) to date has only been observed in the setting of HIV-1 infection, and then only years after HIV transmission. Thus, the concept has emerged that one path to induction of bnAbs is to define the viral and immunologic events that occur during HIV-1 infection, and then to mimic those events with a vaccine formulation. This concept has led to efforts to map both virus and antibody events that occur from the time of HIV-1 transmission to development of bnAbs. This work has revealed that a virus-antibody “arms race” occurs in which a HIV-1 transmitted/founder (TF) Env induces autologous neutralizing antibodies that can not only neutralize the TF virus but also can select virus escape mutants that in turn select affinity-matured neutralizing antibodies. From these studies has come a picture of bnAb development that has led to new insights in host-pathogen interactions and, as well, led to insight into immunologic mechanisms of control of bnAb development. Here we review the progress to date in elucidating bnAb B cell lineages in HIV-1 infection, discuss new research leading to understanding the immunologic mechanisms of bnAb induction, and address issues relevant to the use of this information for the design of new HIV-1 sequential envelope vaccine candidates.

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Analysis of Memory B Cell Responses and Isolation of Novel Monoclonal Antibodies with Neutralizing Breadth from HIV-1-Infected Individuals

Cited by 407 publications

References 74 publications

Trimeric HIV-1 glycoprotein gp140 immunogens and native HIV-1 envelope glycoproteins display the same closed and open quaternary molecular architectures

Trimeric HIV-1 glycoprotein gp140 immunogens and native HIV-1 envelope glycoproteins display the same closed and open quaternary molecular architectures

Identification and specificity of broadly neutralizing antibodies against HIV

Antibody‐virus co‐evolution in HIV infection: paths for HIV vaccine development

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