Conformational Properties of HIV-1 gp120/V3 Immunogenic Domains

Galanakis, Petros; Spyroulias, Georgios A.; Rizos, Apostolos K.; Samolis, Panagiotis; Krambovitis, Elias

doi:10.2174/0929867054038982

Cited by 21 publications

(17 citation statements)

References 119 publications

(263 reference statements)

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“…V3 in different HIV-1 subtypes has distinct antigenic properties. 10,11 In this study, the main tetramers on the tip of the V3 loop in CRF01_AE and CRF07_BC were GPGQ (15/22) and (6/6), respectively (Fig. 2), whereas the tetramer in CRF07_BC was the most conservative in our study.…”

supporting

confidence: 47%

“…10 V3 of env is a cysteine-bound loop structurally composed of 35 amino acids, with the principal neutralizing antibody determinant (PND) located in the crown of the V3 loop, 10,11 which is constituted of the specific tetramer (which locates the position of 15-18 of the V3 amino acid sequence). V3 in different HIV-1 subtypes has distinct antigenic properties.…”

mentioning

confidence: 99%

“…V3 has long been a target of interest for entrybased inhibitors because of its critical role in defining the specificity of the interaction of env with cellular coreceptor molecules, usually CCR5 or CXCR4, to facilitate entry into target cells. 10,11 Our study has indicated that the tetramer on the crown of the V3 loop has greater diversity, especially for subtype B, compared with a previous study conducted in Harbin City published in 2007, which reported that 52.63% of the V3 tip amino motif was GPGQ and 21.53% was GPGR among 19 HIV-1-seropositive infectors that were identified with subtype B¢. 12 Moreover, the impact of the peculiar GWGR on the tip of the V3 loop among the B subtypes is worth noting for the development of profiles of HIV pathogenesis and vaccine design.…”

mentioning

confidence: 99%

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Subtype B Was the Dominant Strain Among HIV Type 1 Infections Except for the Population of Men Who Have Sex with Men in Harbin City, China

Lei

Liu

et al. 2013

AIDS Research and Human Retroviruses

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We sought to identify the prevalent subtypes and study the genetic variation of HIV-1 circulating in HIV infections in Harbin City, China. Forty-seven samples from the env V3-V4 region were successfully sequenced and analyzed, which involved thirty-one men who have sex with men (MSM), eight heterosexuals, seven former plasma donors (FPD)/blood transfusion recipients (BT), and one injection drug user (IDU). In all, 46.8% of CRF01_AE, 40.4% of subtype B, and 12.8% of CRF07_BC were identified. CRF01_AE (64.5%) was the dominant strain in MSM, and subtype B (81.2%) was the chief strain in other infected subjects except for the MSM population. Among all the genotypes, the B subtype possesses greater diversity of the tetramer on the tip of V3 loop than CRF07_BC and CRF01_AE, in which the peculiar GWGR was commonly found. Because nationwide there is a trend toward the increasing presence of CRF01_AE, a consecutive surveillance campaign was necessary among all HIV vulnerable populations in this locality.

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confidence: 47%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Subtype B Was the Dominant Strain Among HIV Type 1 Infections Except for the Population of Men Who Have Sex with Men in Harbin City, China

Lei

Liu

et al. 2013

AIDS Research and Human Retroviruses

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“…We had shown previously with peptide-peptide V3-CCR5 interactions [21] that the amino terminal domain of CCR5 interacted with the V3 domain [34,35]. Using lipoV3-liposomes with five positive amino acid residues (LAI V3), we performed inhibition experiments with soluble V3 peptide derivatives that contained one (V3 +1 ) or nine (V3 +9 ) positively charged amino acids.…”

Section: Discussionmentioning

confidence: 99%

HIV-1 gp120/V3-derived epitopes promote activation-induced cell death to superantigen-stimulated CD4+/CD45RO+ T cells

Porichis

Vlata²,

Hatzidakis³

et al. 2007

Immunology Letters

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“…The three peptides bound to Fab 2219 (19,23, and 23 amino acids long for the MN, UR29, and UG1033 peptides, respectively) all exhibit good electron density for 16 residues (Fig. 4), with all peptides forming a ␤-hairpin with a type II ␤-turn around residues P312 to P315.…”

Section: Vol 80 2006 Crystal Structures Of Hiv-1 Neutralizing Antibmentioning

confidence: 99%

Crystal Structures of Human Immunodeficiency Virus Type 1 (HIV-1) Neutralizing Antibody 2219 in Complex with Three Different V3 Peptides Reveal a New Binding Mode for HIV-1 Cross-Reactivity

Stanfield

Gorny

Zolla‐Pazner

et al. 2006

J Virol

112

123

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Human monoclonal antibody 2219 is a neutralizing antibody isolated from a human immunodeficiency virus type 1-infected individual. 2219 was originally selected for binding to a V3 fusion protein and can neutralize primary isolates from subtypes B, A, and F. Thus, 2219 represents a cross-reactive, human anti-V3 antibody. Fab 2219 binds to one face of the variable V3 ␤-hairpin, primarily contacting conserved residues on the N-terminal ␤-strand of V3, leaving the V3 crown or tip largely accessible. Three V3/2219 complexes reveal the antibody-bound conformations for both the N-and C-terminal regions that flank the V3 crown and illustrate how twisting of the V3 loop alters the relative dispositions and pairing of the amino acids in the adjacent V3 ␤-strands and how the antibody can accommodate V3 loops with different sequences.Recent crystal structures of human immunodeficiency virus type 1 (HIV-1) neutralizing antibodies have revealed how the immune system can utilize many different strategies to recognize this constantly evolving virus. Prototypic examples include the broadly neutralizing antibody b12, which is thought to use its long complementarity-determining region (CDR) loops to access the recessed, but conserved, CD4 binding site (63), and antibody 2G12, which capitalizes on a unique domain-swapped dimer-of-Fab configuration to create a multivalent binding surface to enhance avidity for low-affinity carbohydrate epitopes (5) on the gp120 silent face. Novel antibodies that block gp120 binding to its chemokine receptor have recently been shown to contain sulfated tyrosines in their CDR loops that likely mimic sulfated tyrosines in the chemokine receptor itself (12), whereas the anti-V3 antibody 447-52D uses a long CDR H3 loop to bind V3 in a way that makes the recognition largely sequence independent, except for interaction with the relatively conserved GPGR crown region (72). Finally, antibody 4E10, the most broadly HIV-1-neutralizing antibody known, binds to a membrane-proximal epitope on gp41 and may also use its long CDR H3 loop to interact with the membrane (6). We report here the structure of a human anti-V3 neutralizing antibody, 2219, that shows yet another way the immune system has found to evoke broad recognition of multiple HIV-1 viral isolates.The HIV-1 viral proteins gp120 and gp41 are located on the outer membrane surface of the virus, forming a trimeric assembly of the two noncovalently associated proteins. Antibodies that neutralize the virus are directed against these envelope proteins. One of the major epitopes on gp120 is its V3 (third hypervariable) loop, a region of approximately 35 amino acids, linked by a disulfide bond at the base (Cys296-Cys331; HXB2 numbering). Although V3 is termed "hypervariable," much of the V3 loop, including the tip or crown, is fairly well conserved, with usually just one or two chemically similar amino acid types found at each position (Table 1). The V3 region is highly immunogenic and induces a spectrum of antibodies that can either be highly specific for a par...

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Conformational Properties of HIV-1 gp120/V3 Immunogenic Domains

Cited by 21 publications

References 119 publications

Subtype B Was the Dominant Strain Among HIV Type 1 Infections Except for the Population of Men Who Have Sex with Men in Harbin City, China

Subtype B Was the Dominant Strain Among HIV Type 1 Infections Except for the Population of Men Who Have Sex with Men in Harbin City, China

HIV-1 gp120/V3-derived epitopes promote activation-induced cell death to superantigen-stimulated CD4+/CD45RO+ T cells

Crystal Structures of Human Immunodeficiency Virus Type 1 (HIV-1) Neutralizing Antibody 2219 in Complex with Three Different V3 Peptides Reveal a New Binding Mode for HIV-1 Cross-Reactivity

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