Immunogenic properties of a trimeric gp41-based immunogen containing an exposed membrane-proximal external region

Habte, Habtom H.; Banerjee, Saikat; Shi, Huaizhong; Qin, Yali; Cho, Michael W.

doi:10.1016/j.virol.2015.09.010

Cited by 6 publications

(26 citation statements)

References 92 publications

(118 reference statements)

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“…To identify immunogenic linear epitopes, ELISAs were conducted with overlapping 10-mer peptide sets biotinylated either at the N- or C-terminal ends as we previously reported (Banerjee et al, 2016; Habte et al, 2015). After the first immunization, very little response was detected (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…3A and 3B) as previously described (Banerjee et al, 2016; Habte et al, 2015). As noted previously, the D674A mutation affects the helical conformation of the peptide (Banerjee et al, 2016; Habte et al, 2015); thus, results should be interpreted with some caution. For R2, the four residues that were most affected besides D674 were F673, N677, W678 and L679.…”

Section: Resultsmentioning

confidence: 99%

“…Residues important in R3 were N671, W672, F673 and N677; the first three of which are absolutely critical for 10E8. Of all the immunogens we evaluated to date (Banerjee et al, 2016; Habte et al, 2015), this is the first time we targeted all three of these residues. For R4, the pattern was similar to R3, except that W6762 was not targeted.…”

Section: Resultsmentioning

confidence: 99%

“…The pHR1-HR2-28×3 construct is based on a pET-21a vector. HR1-HR2-28×3 was expressed in E. coli , solubilized with 8M urea, and purified using Ni-NTA as we previously described (Banerjee et al, 2016; Habte et al, 2015; Qin et al, 2014). The fusion protein was cleaved with thrombin (GE Healthcare; cat#27-0846-01) and the gp41-28×3 fragment was purified using Ni-NTA, dialyzed into PBS (pH 8.0) and stored at −80°C.…”

Section: Methodsmentioning

confidence: 99%

“…Despite having short, linear, simple alpha-helical epitopes, efforts to develop a vaccine that can induce 4E10/10E8-like bnAbs have been unsuccessful (see (Banerjee et al, 2016; Habte et al, 2015) and references therein). Since all of the immunogens evaluated could bind 4E10/10E8, the failure to induce similar bnAbs is not because antigens could not assume the correct epitope structures.…”

Section: Introductionmentioning

confidence: 99%

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Evaluation of a novel multi-immunogen vaccine strategy for targeting 4E10/10E8 neutralizing epitopes on HIV-1 gp41 membrane proximal external region

et al. 2017

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The membrane proximal external region (MPER) of HIV-1 gp41 is targeted by broadly neutralizing antibodies (bnAbs) 4E10 and 10E8. In this proof-of-concept study, we evaluated a novel multi-immunogen vaccine strategy referred to as Incremental, Phased Antigenic Stimulation for Rapid Antibody Maturation (IPAS-RAM) to induce 4E10/10E8-like bnAbs. Rabbits were immunized sequentially, but in a phased manner, with three immunogens that are progressively more native (gp41-28×3, gp41-54CT, and rVV-gp160DH12). Although nAbs were not induced, epitope-mapping analyses indicated that IPAS-RAM vaccination was better able to target antibodies towards the 4E10/10E8 epitopes than homologous prime-boost immunization using gp41-28×3 alone. MPER-specific rabbit monoclonal antibodies were generated, including 9F6. Although it lacked neutralizing activity, the target epitope profile of 9F6 closely resembled those of 4E10 and 10E8 (671NWFDITNWLWYIK683). B-cell repertoire analyses suggested the importance of co-immunizations for maturation of 9F6, which warrants further evaluation of our IPAS-RAM vaccine strategy using an improved priming immunogen.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Evaluation of a novel multi-immunogen vaccine strategy for targeting 4E10/10E8 neutralizing epitopes on HIV-1 gp41 membrane proximal external region

et al. 2017

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Using the Sleeping Beauty (SB) Transposon to Generate Stable Cells Producing Enveloped Virus‐Like Particles (eVLPs) Pseudotyped with SARS‐CoV‐2 Proteins for Vaccination

et al. 2022

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The Sleeping Beauty (SB) transposon system is an efficient non‐viral tool for gene transfer into a variety of cells, including human cells. Through a cut‐and‐paste mechanism, your favorite gene (YFG) is integrated into AT‐rich regions within the genome, providing stable long‐term expression of the transfected gene. The SB system is evolving and has become a powerful tool for gene therapy. There are no safety concerns using this system, the handling is easy, and the time required to obtain a stable cell line is significantly reduced compared to other systems currently available. Here, we present a novel application of this system to generate, within 8 days, a stable producer HEK293T cell line capable of constitutively delivering enveloped virus‐like particles (eVLPs) for vaccination. We provide step‐by‐step protocols for generation of the SB transposon constructs, transfection procedures, and validation of the produced eVLPs. We next describe a method to pseudotype the constitutively produced eVLPs using the Spike protein derived from the SARS‐CoV‐2 virus (by coating the eVLP capsid with the heterologous antigen). We also describe optimization methods to scale up the production of pseudotyped eVLPs in a laboratory setting (from 100 µg to 5 mg). © Published 2022. This article is a U.S. Government work and is in the public domain in the USA. Basic Protocol 1: Generation of the SB plasmids Basic Protocol 2: Generation of a stable HEK293T cell line constitutively secreting MLV‐based eVLPs Basic Protocol 3: Evaluation of the SB constructs by immunofluorescence assay Basic Protocol 4: Validation of eVLPs by denaturing PAGE and western blot Alternate Protocol 1: Analysis of SARS‐CoV‐2 Spike protein oligomerization using blue native gel electrophoresis and western blot Alternate Protocol 2: Evaluation of eVLP quality by electron microscopy (negative staining) Basic Protocol 5: Small‐scale production of eVLPs Alternate Protocol 3: Large‐scale production of eVLPs (up to about 1 to 3 mg VLPs) Alternate Protocol 4: Large‐scale production of eVLPs (up to about 3 to 5 mg VLPs) Support Protocol: Quantification of total protein concentration by Bradford assay

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The development of HIV vaccines targeting gp41 membrane-proximal external region (MPER): challenges and prospects

Liu

et al. 2018

Protein &Amp; Cell

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A human immunodeficiency virus type-1 (HIV-1) vaccine which is able to effectively prevent infection would be the most powerful method of extinguishing pandemic of the acquired immunodeficiency syndrome (AIDS). Yet, achieving such vaccine remains great challenges. The membrane-proximal external region (MPER) is a highly conserved region of the envelope glycoprotein (Env) gp41 subunit near the viral envelope surface, and it plays a key role in membrane fusion. It is also the target of some reported broadly neutralizing antibodies (bNAbs). Thus, MPER is deemed to be one of the most attractive vaccine targets. However, no one can induce these bNAbs by immunization with immunogens containing the MPER sequence(s). The few attempts at developing a vaccine have only resulted in the induction of neutralizing antibodies with quite low potency and limited breadth. Thus far, vaccine failure can be attributed to various characteristics of MPER, such as those involving structure and immunology; therefore, we will focus on these and review the recent progress in the field from the following perspectives: (1) MPER structure and its role in membrane fusion, (2) the epitopes and neutralization mechanisms of MPER-specific bNAbs, as well as the limitations in eliciting neutralizing antibodies, and (3) different strategies for MPER vaccine design and current harvests.

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Immunogenic properties of a trimeric gp41-based immunogen containing an exposed membrane-proximal external region

Cited by 6 publications

References 92 publications

Evaluation of a novel multi-immunogen vaccine strategy for targeting 4E10/10E8 neutralizing epitopes on HIV-1 gp41 membrane proximal external region

Evaluation of a novel multi-immunogen vaccine strategy for targeting 4E10/10E8 neutralizing epitopes on HIV-1 gp41 membrane proximal external region

Using the Sleeping Beauty (SB) Transposon to Generate Stable Cells Producing Enveloped Virus‐Like Particles (eVLPs) Pseudotyped with SARS‐CoV‐2 Proteins for Vaccination

The development of HIV vaccines targeting gp41 membrane-proximal external region (MPER): challenges and prospects

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