Serum enhancement of human immunodeficiency virus (HIV) infection correlates with disease in HIV-infected individuals

Homsy, Jacques; Meyer, Mia; Levy, Jay A.

doi:10.1128/jvi.64.4.1437-1440.1990

Cited by 148 publications

(52 citation statements)

References 22 publications

(35 reference statements)

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“…Importantly, ADE has also been described for HIV in vitro (26,27). Although it remains unknown whether ADE could increase HIV infection risk in humans (28), it has been found that patients with HIV who have antibodies capable of ADE have more rapid disease progression (29). For ADE to mediate enhanced infection risk after HIV vaccination, the vaccine regimen would need to induce nonneutralizing or poorly neutralizing antibodies; it has been shown that the HVTN 505 regimen did induce such antibodies (namely, gp41 reactive and nonneutralizing) (30).…”

Section: Discussionmentioning

confidence: 99%

Fc Gamma Receptor Polymorphisms Modulated the Vaccine Effect on HIV-1 Risk in the HVTN 505 HIV Vaccine Trial

Gilbert

Carpp

et al. 2019

J Virol

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HIV Vaccine Trials Network (HVTN) 505 was a phase 2b efficacy trial of a DNA/recombinant adenovirus 5 (rAd5) HIV vaccine regimen. Although the trial was stopped early for lack of overall efficacy, later correlates of risk and sieve analyses generated the hypothesis that the DNA/rAd5 vaccine regimen protected some vaccinees from HIV infection yet enhanced HIV infection risk for others. Here, we assessed whether and how host Fc gamma receptor (Fc␥R) genetic variations influenced the DNA/rAd5 vaccine regimen's effect on HIV infection risk. We found that vaccine receipt significantly increased HIV acquisition compared with placebo receipt among participants carrying the FCGR2C-TATA haplotype (comprising minor alleles of four FCGR2C single-nucleotide polymorphism [SNP] sites) (hazard ratio [HR] ϭ 9.79, P ϭ 0.035) but not among participants without the haplotype (HR ϭ 0.86, P ϭ 0.67); the interaction of vaccine and haplotype effect was significant (P ϭ 0.034). Similarly, vaccine receipt increased HIV acquisition compared with placebo receipt among participants carrying the FCGR3B-AGA haplotype (comprising minor alleles of the 3 FCGR3B SNPs) (HR ϭ 2.78, P ϭ 0.058) but not among participants without the haplotype (HR ϭ 0.73, P ϭ 0.44); again, the interaction of vaccine and haplotype was significant (P ϭ 0.047). The FCGR3B-AGA haplotype also influenced whether a combined Env-specific CD8 ϩ T-cell polyfunctionality score and IgG response correlated significantly with HIV risk; an FCGR2A SNP and two FCGR2B SNPs influenced whether anti-gp140 antibody-dependent cellular phagocytosis correlated significantly with HIV risk. These results provide further evidence that Fc gamma receptor genetic variations may modulate HIV vaccine effects and immune function after HIV vaccination.

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Section: Discussionmentioning

confidence: 99%

Fc Gamma Receptor Polymorphisms Modulated the Vaccine Effect on HIV-1 Risk in the HVTN 505 HIV Vaccine Trial

Gilbert

Carpp

et al. 2019

J Virol

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“…Except for early work with FcR-ADE [31], most data on the clinical significance were reported on C-ADE. Therefore, the following discussion will be largely restricted to the latter type of infection-enhancement.…”

Section: Antibody-dependent Enhancement Of Hiv Infectionmentioning

confidence: 99%

Traitors of the immune system—Enhancing antibodies in HIV infection: Their possible implication in HIV vaccine development

Beck

Prohászka

Füst

2008

Vaccine

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Considering recent HIV vaccine failures, the authors believe that it would be most important to find new targets for vaccine-induced immunity, and to analyze the data from previous trials, using an innovative approach. In their review article, the authors briefly summarize the significance of the antibody-dependent enhancement of infection in different viral diseases and discuss role of these types of antibodies as the obstacles for vaccine development. Findings which indicate that complement-mediated antibody-dependent enhancement (C-ADE) is present also in HIV-infected patients, are summarized. Previous results of the authors, suggesting that C-ADE plays a very important role in the progression of HIV infection are described. Data reflecting that enhancing antibodies may develop even in vaccinated animals and human volunteers, and may be responsible for the paradoxical results obtained in some subgroups of vaccinees are discussed. Finally, based on their hypothesis, the authors offer some suggestions for the future development of vaccines.

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“…An attempt has been made to correlate the presence of enhancing Abs in the serum of HIV-infected patients to the progression of aquired immunodeficiency syndrome. However, the in vitro enhancement levels demonstrated were fairly low and the number of patients was limited (Homsy, et al, 1990). With HRSV, Ab may not only function to enhance infectivity, but also to enhance leukotriene production in infected cells (Ananaba and Anderson, 1991 ).…”

Section: Antibody-dependent Enhancement Of Virus Infectivitymentioning

confidence: 99%

“…The ultimate question is what bearing ADE of virus infection, as described in vitro, has upon the pathogenesis of disease in vivo and the development of virus vaccines. This question has fueled an ongoing debate among researchers ofDV (Halstead, 1989;Morens and Halstead, 1990;Rosen, 1989) and HIV (Bolognesi, 1989;Homsy, et al, 1990;Robinson, et al, 1988b). There is a substantial body of epidemiological information to suggest that ADE of DV infection of macrophages underlies the development of a more severe form of dengue called dengue hemorrhagic fever or dengue shock syndrome.…”

Section: Antibody-dependent Enhancement Of Virus Infectivitymentioning

confidence: 99%

A review of feline infectious peritonitis virus: molecular biology, immunopathogenesis, clinical aspects, and vaccination

Olsen

1993

Veterinary Microbiology

111

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Feline infectious peritonitis (FIP) has been an elusive and frustrating problem for veterinary practitioners and cat breeders for many years. Over the last several years, reports have begun to elucidate aspects of the molecular biology of the causal virus (FIPV). These papers complement a rapidly growing base of knowledge concerning the molecular organization and replication of coronaviruses in general. The fascinating immunopathogenesis of FIPV infection and the virus' interaction with macrophages has also been the subject of several recent papers. It is now clear that FIPV may be of interest to scientists other than veterinary virologists since its pathogenesis may provide a useful model system for other viruses whose infectivity is enhanced in the presence of virus-specific antibody. With these advances and the recent release of the first commercially-available FIPV vaccine, it is appropriate to review what is known about the organization and replication of coronaviruses and the pathogenesis of FIPV infection.

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Serum enhancement of human immunodeficiency virus (HIV) infection correlates with disease in HIV-infected individuals

Cited by 148 publications

References 22 publications

Fc Gamma Receptor Polymorphisms Modulated the Vaccine Effect on HIV-1 Risk in the HVTN 505 HIV Vaccine Trial

Fc Gamma Receptor Polymorphisms Modulated the Vaccine Effect on HIV-1 Risk in the HVTN 505 HIV Vaccine Trial

Traitors of the immune system—Enhancing antibodies in HIV infection: Their possible implication in HIV vaccine development

A review of feline infectious peritonitis virus: molecular biology, immunopathogenesis, clinical aspects, and vaccination

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