Escape of HIV-1 is associated with lack of V3 domain-specific antibodies <i>in vivo</i>

Schreiber, Michael; Müller, Harm; Wachsmuth, C; Laue, Thomas M.; Hufert, Frank T.; Laer, M D Van; Schmitz, Herbert

doi:10.1046/j.1365-2249.1996.d01-909.x

Cited by 14 publications

(13 citation statements)

References 35 publications

(52 reference statements)

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“…This has particularly been described for the V3 loop [39,53,89]. While some authors describe a lack of V3-specific neutralizing antibodies in patients who develop AIDS [89], others have found that neutralizing antibodies for one strain of HIV-1 to the V3 loop could fail to neutralize another strain of the same virus and even enhance infection in a third strain [53]. These findings have identified the variable position 311 proximal to the conserved GPGR motif at the top of the V3 crown as important for viral sensitivity to neutralization or enhancement by antibodies.…”

mentioning

confidence: 84%

“…It is thought that these loops change in structure and conformation from time to time, thereby allowing the virus to elude the immune response. This has particularly been described for the V3 loop [39,53,89]. While some authors describe a lack of V3-specific neutralizing antibodies in patients who develop AIDS [89], others have found that neutralizing antibodies for one strain of HIV-1 to the V3 loop could fail to neutralize another strain of the same virus and even enhance infection in a third strain [53].…”

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confidence: 97%

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Immune Responses to HIV Gp120 that Facilitate Viral Escape

Stevceva¹,

Yoon²,

Anastasiades³

et al. 2007

CHR

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The gp160 complex of the envelope of the HIV virus and its component gp120 are essential for viral entry into the host cell. Gp120 binding to its receptor CD4 and co-receptor, CXCR4 or CCR5 is required for fusion of viral and cellular membranes. The presence of gp120 facilitates immune escape of the virus through its profound effect on the immune cells. It is a polyclonal activator of B cells, causing them to differentiate into immunoglobulin producing cells while activating the complement cascade. This results in the formation of immune complexes that are unable to kill the virus but instead shield it from the attack of other immune cells. Such HIV-1 virus that is trapped within immune complexes and is bound to the B cells via CD21 is more infectious than the free virion. In addition, HIV virions are trapped on the membrane of follicular dendritic cells (FDC) processes in immune complexes or through complement receptors. Thus, FDC can serve as a 'Trojan horse' and transmit the trapped virus to CD4+ T lymphocytes as they migrate through the germinal centre to the follicular mantle and paracortical areas. It was demonstrated that CXCR4-binding HIV-1 X4 gp120 causes the movement of T cells, including HIV-specific CTL, away from high concentrations of the viral protein and its expression by target cells reduces CTL efficacy in vitro. Therefore, apart from the essential role in viral attachment and infection of cells, gp120 possesses several properties that affect the behavior of immune cells and skew the immune response to the virus facilitating viral escape.

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confidence: 84%

mentioning

confidence: 97%

Immune Responses to HIV Gp120 that Facilitate Viral Escape

Stevceva¹,

Yoon²,

Anastasiades³

et al. 2007

CHR

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“…3). Many mutations were located in V3, a region that contains linear and discontinuous antigenic determinants (9,18,39) that can change during disease development and immune escape (37,38,41). Some amino acid substitutions led to three new and loss of two potential N-linked glycosylation sites, which in turn might result in changes in conformation and immune recognition of gp120 (3,12,14,29,30,35,47,50).…”

Section: Nonpassaged Shiv-vpumentioning

confidence: 99%

Molecular Evolution of Human Immunodeficiency Virus env in Humans and Monkeys: Similar Patterns Occur during Natural Disease Progression or Rapid Virus Passage

Hofmann‐Lehmann

Vlasak

Chenine

et al. 2002

J Virol

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“…Serum adsorption studies have shown that type-specific V3-directed antibodies contribute to the neutralization of autologous virus and control of in vivo infection for some patients (6,41,42). The existence of V3 epitopes that mediate the neutralization of primary virus isolates and are conserved within clade B was shown by the demonstration that polyclonal V3-reactive antibodies isolated from North American patient sera possessed potent neutralizing activity against a number of clade B primary isolates (26).…”

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confidence: 99%

Antibodies That Are Cross-Reactive for Human Immunodeficiency Virus Type 1 Clade A and Clade B V3 Domains Are Common in Patient Sera from Cameroon, but Their Neutralization Activity Is Usually Restricted by Epitope Masking

Krachmarov¹,

Pinter²,

Honnen³

et al. 2005

J Virol

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Sera from human immunodeficiency virus type 1 (HIV-1)-infected North American patients recognized a fusion protein expressing a V3 loop from a clade B primary isolate virus (JR-CSF) but not from a clade A primary isolate virus (92UG037.8), while most sera from Cameroonian patients recognized both fusion proteins. Competition studies of consensus V3 peptides demonstrated that the majority of the cross-reactive Cameroonian sera contained cross-reactive antibodies that reacted strongly with both V3 sequences. V3-specific antibodies purified from all six cross-reactive sera examined had potent neutralizing activity for virus pseudotyped with envelope proteins (Env) from SF162, a neutralization-sensitive clade B primary isolate. For four of these samples, neutralization of SF162 pseudotypes was blocked by both the clade A and clade B V3 fusion proteins, indicating that this activity was mediated by cross-reactive antibodies. In contrast, the V3-reactive antibodies from only one of these six sera had significant neutralizing activity against viruses pseudotyped with Envs from typically resistant clade B (JR-FL) or clade A (92UG037.8) primary isolates. However, the V3-reactive antibodies from these cross-reactive Cameroonian sera did neutralize virus pseudotyped with chimeric Envs containing the 92UG037.8 or JR-FL V3 sequence in Env backbones that did not express V1/V2 domain masking of V3 epitopes. These data indicated that Cameroonian sera frequently contain cross-clade reactive V3-directed antibodies and indicated that the typical inability of such antibodies to neutralize typical, resistant primary isolate Env pseudotypes was primarily due to indirect masking effects rather than to the absence of the target epitopes.

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Escape of HIV-1 is associated with lack of V3 domain-specific antibodies in vivo

Cited by 14 publications

References 35 publications

Immune Responses to HIV Gp120 that Facilitate Viral Escape

Immune Responses to HIV Gp120 that Facilitate Viral Escape

Molecular Evolution of Human Immunodeficiency Virus env in Humans and Monkeys: Similar Patterns Occur during Natural Disease Progression or Rapid Virus Passage

Antibodies That Are Cross-Reactive for Human Immunodeficiency Virus Type 1 Clade A and Clade B V3 Domains Are Common in Patient Sera from Cameroon, but Their Neutralization Activity Is Usually Restricted by Epitope Masking

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