Proteoliposomal formulations of an HIV-1 gp41-based miniprotein elicit a lipid-dependent immunodominant response overlapping the 2F5 binding motif

Molinos-Albert, Luis M.; Bilbao, Eneritz; Agulló, Luís; Marfil, Sílvia; García, Elisabet; Concepción, Maria Luisa Rodrı́guez de la; Izquierdo-Useros, Nuria; Vilaplana, Cristina; Nieto-Garai, Jon Ander; Contreras, F.‐Xabier; Floor, Martin; Cardona, Père-Joan; Martínez-Picado, Javier; Clotet, Bonaventura; Villà­-Freixa, Jordi; Lorizate, Maier; Carrillo, Jorge; Blanco, Julià

doi:10.1038/srep40800

Cited by 13 publications

(20 citation statements)

References 84 publications

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“…However, recent work by Luis et al showed that addition of combinatory PS/GM3 (ganglioside of mono-sialic acid) into the Ag-loaded POPC liposomes remarkably increased the anti-Ag immune reactions in vaccinated mice, though insertion of PS alone into the carrier made a minimal contribution to the enhancement [97]. Also, Cauvi et al revealed in murine model that anionic empty PS liposomes triggered peritoneal MPs to have about 4700 genes specifically modified, resulting in changed protein expressions by peritoneal cells, including increased secretion of several chemokines (CXCL1, CXCL2, CSF-2, and CSF-3) and cytokines (TNF-a, IL-6, IL-10).…”

Section: Surface Propertymentioning

confidence: 99%

“…Luis et al using a HIV-1 gp41 MPER (membrane proximal external region) engrafted with tetanus toxoid (TT) as Ags, and POPC (1-palmitoyl-2-oleoylphosphatidylcholine) as the matrix material, prepared the Ag-loaded liposomes as a VADS against HIV. To enhance efficacy, the liposomes were further incorporated with other lipids, including PS (phosphatidylserine), GM3, or combinatory CHO/SM (sphingomyelin) which are enriched in HIV viral membrane lipid rafts, where MPER is embedded for maintaining peptide conformation [97]. In mice, the gp41-TTloaded POPC liposomes when combined with PS/GM3 or CHO/SM induced significantly increased anti-gp41 immune reactions which was further enhanced by the addition of MPLA.…”

Section: Membrane Fluiditymentioning

confidence: 99%

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Liposomes used as a vaccine adjuvant-delivery system: From basics to clinical immunization

Wang

Chen

Wang

2019

Journal of Controlled Release

198

155

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Section: Surface Propertymentioning

confidence: 99%

Section: Membrane Fluiditymentioning

confidence: 99%

Liposomes used as a vaccine adjuvant-delivery system: From basics to clinical immunization

Wang

Chen

Wang

2019

Journal of Controlled Release

198

155

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“…Given that the complete epitope of anti-MPER bNAbs includes membrane components ( 74 , 89 ) and that lipid recognition by CDR H3 impacts into their functionality ( 69 , 72 , 73 , 86 , 87 ), their potential for contributing to MPER-specific neutralizing responses by immunization is worth exploring. In this regard, membrane-mimicking platforms including viral-like particles (VLP) ( 137 , 138 ) or liposomes ( 122 – 124 ) have been approached. It has been shown that membrane lipids can modulate the MPER structure likely by promoting a native-like conformation and demonstrated to improve immunogenicity ( 123 , 124 ).…”

Section: Eliciting Anti-mper Antibodies By Immunizationmentioning

confidence: 99%

“…In this regard, membrane-mimicking platforms including viral-like particles (VLP) ( 137 , 138 ) or liposomes ( 122 – 124 ) have been approached. It has been shown that membrane lipids can modulate the MPER structure likely by promoting a native-like conformation and demonstrated to improve immunogenicity ( 123 , 124 ). In particular, we previously demonstrated that those lipids overrepresented in the viral membrane such as cholesterol and sphingomyelin have the potential to induce stronger antibody titers comparing with simple POPC lipids ( 124 ).…”

Section: Eliciting Anti-mper Antibodies By Immunizationmentioning

confidence: 99%

Immunologic Insights on the Membrane Proximal External Region: A Major Human Immunodeficiency Virus Type-1 Vaccine Target

et al. 2017

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Broadly neutralizing antibodies (bNAbs) targeting conserved regions within the human immunodeficiency virus type-1 (HIV-1) envelope glycoprotein (Env) can be generated by the human immune system and their elicitation by vaccination will be a key point to protect against the wide range of viral diversity. The membrane proximal external region (MPER) is a highly conserved region within the Env gp41 subunit, plays a major role in membrane fusion and is targeted by naturally induced bNAbs. Therefore, the MPER is considered as an attractive vaccine target. However, despite many attempts to design MPER-based immunogens, further study is still needed to understand its structural complexity, its amphiphilic feature, and its limited accessibility by steric hindrance. These particular features compromise the development of MPER-specific neutralizing responses during natural infection and limit the number of bNAbs isolated against this region, as compared with other HIV-1 vulnerability sites, and represent additional hurdles for immunogen development. Nevertheless, the analysis of MPER humoral responses elicited during natural infection as well as the MPER bNAbs isolated to date highlight that the human immune system is capable of generating MPER protective antibodies. Here, we discuss the recent advances describing the immunologic and biochemical features that make the MPER a unique HIV-1 vulnerability site, the different strategies to generate MPER-neutralizing antibodies in immunization protocols and point the importance of extending our knowledge toward new MPER epitopes by the isolation of novel monoclonal antibodies. This will be crucial for the redesign of immunogens able to skip non-neutralizing MPER determinants.

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“…Arg 696 has been suggested to play a structural role in trimerization by forming polar contacts within the membrane, either alone or in combination with a GxxxG motif, and computational studies on the gp41 TM domain support this claim. 9,[12][13][14] Biophysical studies on the HIV TM have yielded inconsistent results on the oligomeric state of this domain. An NMR analysis of a TM peptide in a DMPC/DHPC mixed micelle showed no evidence of trimerization, but the specific transmembrane peptide used in that study contained significant portions of the MPER and cytoplasmic tail.…”

Section: Introductionmentioning

confidence: 99%

The Conserved Positive Charge in the Transmembrane Domain of HIV Gp41 Contributes to Its Intrinsic Preference for Trimerization

Reichart¹,

Leaman²,

Sands³

et al. 2020

Preprint

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The transmembrane (TM) domain of HIV glycoprotein gp41 anchors the envelope (Env) spike in the viral membrane and is highly conserved. The mid-span arginine 696 is particularly conserved, and the only other residue found in this position is lysine. Seeking to examine the role of this conserved positive charge in the structure and function of the gp41 TM domain, we synthesized a series of peptides corresponding to this region. Analysis of the peptides in a previously validated fluorescence assay in model membranes showed that the native TM domain is trimeric. Peptides in which the intramembrane arginine was mutated to alanine showed significantly lower trimerization propensity. In contrast, this mutation in the context of infectious pseudovirus caused only modest decreases in viral stability and infectivity. We propose a model to explain the importance of this charge to gp41 structure and to HIV infection.

show abstract

Proteoliposomal formulations of an HIV-1 gp41-based miniprotein elicit a lipid-dependent immunodominant response overlapping the 2F5 binding motif

Cited by 13 publications

References 84 publications

Liposomes used as a vaccine adjuvant-delivery system: From basics to clinical immunization

Liposomes used as a vaccine adjuvant-delivery system: From basics to clinical immunization

Immunologic Insights on the Membrane Proximal External Region: A Major Human Immunodeficiency Virus Type-1 Vaccine Target

The Conserved Positive Charge in the Transmembrane Domain of HIV Gp41 Contributes to Its Intrinsic Preference for Trimerization

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