AIDS Vaccination Studies Using an Ex Vivo Feline Immunodeficiency Virus Model: Failure To Protect and Possible Enhancement of Challenge Infection by Four Cell-Based Vaccines Prepared with Autologous Lymphoblasts

Giannecchini, Simone; Isola, Patrizia; Sichi, Olimpia; Matteucci, Donatella; Pistello, Mauro; Zaccaro, Lucia; Mauro, Daniela; Bendinelli, Mauro

doi:10.1128/jvi.76.14.6882-6892.2002

Cited by 29 publications

(44 citation statements)

References 70 publications

(61 reference statements)

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“…Several precedents exist for vaccines to shift the host-pathogen interaction in harmful ways upon subsequent exposure to live virus (26)(27)(28)(29), including examples of vaccinemediated enhancement of lentivirus infections (30)(31)(32). Because lentiviral vaccine-mediated enhancement does not always involve enhancing antibodies (31), a mechanism of lymphocyte activation-mediated enhancement of virus replication has been proposed (33); data consistent with such a mechanism were reported in one feline immunodeficiency virus (FIV) vaccine study (34).…”

Section: Discussionmentioning

confidence: 79%

Enhanced SIV replication and accelerated progression to AIDS in macaques primed to mount a CD4 T cell response to the SIV envelope protein

Staprans

Barry

Silvestri

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

130

113

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Given the dual role of CD4 T cells as both immune effectors and targets for HIV infection, the balance of CD4 versus CD8 T cellmediated responses induced by candidate AIDS vaccines may be critical in determining postvaccination infection outcomes. An attenuated recombinant varicella-zoster virus vaccine expressing the simian immunodeficiency virus (SIV) envelope (Env) elicited nonneutralizing Env-binding antibodies and little if any cytotoxic T lymphocyte responses in rhesus macaques (Macaca mulatta). After challenge with SIV, Env vaccinees manifested increased levels of SIV replication, more rapid CD4 depletion, and accelerated progression to AIDS compared with controls. Enhanced SIV replication correlated with increased CD4 T cell proliferation soon after SIV challenge, apparently the result of an anamnestic response to SIV antigens. Thus activation of virusspecific CD4 T cells at the time of exposure to a CD4 T cell-tropic lentivirus, in the absence of an effective CD8 response, may enhance virus replication and disease. These data suggest suggest that candidate AIDS vaccines may not simply be either efficacious or neutral; they may also have the potential to be harmful.

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Section: Discussionmentioning

confidence: 79%

Enhanced SIV replication and accelerated progression to AIDS in macaques primed to mount a CD4 T cell response to the SIV envelope protein

Staprans

Barry

Silvestri

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

130

113

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“…The FIV particles used in this study were rendered noninfectious by the internal inactivating agent AT2 (24). This agent has previously been shown to inactivate HIV and SIV without affecting Env structure and functions, including cell entry (2, 58).…”

Section: Vol 77 2003 Structural Features Of An Fiv-inhibitory Octapmentioning

confidence: 99%

“…d FIV inactivated with AT2 (5 g of protein) and incubated with MBM cells (5 ϫ 10 5 ) at 4°C for 1 h before C8 addition, to permit virus adsorption but not entry (24).…”

Section: Vol 77 2003 Structural Features Of An Fiv-inhibitory Octapmentioning

confidence: 99%

“…Titration of the viral stocks was carried out in MBM cells and, depending on experiment design, included or did not include washout of unadsorbed virus after 5 h at 37°C to reproduce the conditions used in the FIV inhibition assay (see below). Internal inactivation of the viruses used in peptide binding experiments was carried out with 2,2Ј-dithiodipyridine (also known as aldrithiol-2 [AT2]) as previously described (24). In brief, viral stocks were incubated with 300 M AT2 at 4°C for 2 h, pelleted in the cold at 20,000 ϫ g for 90 min, and resuspended at 1 mg/ml in phosphatebuffered saline.…”

Section: Cells and Viruses Mbm Cells Are A Line Of Cd3mentioning

confidence: 99%

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Antiviral Activity and Conformational Features of an Octapeptide Derived from the Membrane-Proximal Ectodomain of the Feline Immunodeficiency Virus Transmembrane Glycoprotein

Giannecchini

Fenza

D’Ursi

et al. 2003

J Virol

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Feline immunodeficiency virus (FIV) provides a valuable animal model by which criteria for lentivirus control strategies can be tested. Previous studies have shown that a 20-mer synthetic peptide of the membraneproximal ectodomain of FIV transmembrane glycoprotein, designated peptide 59, potently inhibited the growth of tissue culture-adapted FIV in feline fibroblastoid CrFK cells. In the present report we describe the potential of this peptide to inhibit the replication of primary FIV isolates in lymphoid cells. Because antiviral activity of peptide 59 was found to map to a short segment containing three conserved Trp residues, further analyses focused on a derivative of eight amino acids ( 770 W-I 777 ), designated C8. Peptide C8 activity was found to be dependent on conservation of the Trp motif, to be removed from solution by FIV absorbed onto substrate cells, and to be blocked by a peptide derived from the N-terminal portion of FIV transmembrane glycoprotein. Structural studies showed that peptide C8 possesses a conformational propensity highly uncommon for peptides of its size, which may account for its considerable antiviral potency in spite of small size.

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“…The accelerated virus replication correlated with the presence of envelope-specific antibodies at the time of challenge in some studies 3Present address: UMC Utrecht, Department of Immunology, Heidelberglaan 100, 3584 CX Utrecht, The Netherlands. (Lombardi et al, 1994;Siebelink et al, 1995c;Karlas et al, 1999;Giannecchini et al, 2002), but not in others (Hosie et al, 1992;Richardson et al, 1997Richardson et al, , 2002. Hence, the mechanism underlying this enhancement phenomenon has not been fully elucidated.…”

Section: Introductionmentioning

confidence: 99%

Antibodies specific for hypervariable regions 3 to 5 of the feline immunodeficiency virus envelope glycoprotein are not solely responsible for vaccine-induced acceleration of challenge infection in cats

Huisman

Schrauwen

Pas

et al. 2004

Journal of General Virology

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In a previous vaccination study in cats, the authors reported on accelerated feline immunodeficiency virus (FIV) replication upon challenge in animals vaccinated with a candidate envelope subunit vaccine. Plasma transfer studies as well as antibody profiles in vaccinated cats indicated a causative role for antibodies directed against the hypervariable regions HV3, HV4 and HV5 (HV3–5) of the envelope glycoprotein. The present study was designed to investigate further the contribution of antibodies in envelope vaccine-induced acceleration of FIV infection. To this end, regions HV3–5 of the envelope glycoprotein were deleted from the original vaccine, thus addressing the contributing role of antibodies directed against these hypervariable regions. Interestingly, this approach did not prevent acceleration of challenge infection. Analysis of the antibody responses in the respective groups suggested that removal of HV3–5 redirected the humoral immune response towards other regions of the envelope glycoprotein, indicating that these regions can also induce antibodies that accelerate virus replication.

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AIDS Vaccination Studies Using an Ex Vivo Feline Immunodeficiency Virus Model: Failure To Protect and Possible Enhancement of Challenge Infection by Four Cell-Based Vaccines Prepared with Autologous Lymphoblasts

Cited by 29 publications

References 70 publications

Enhanced SIV replication and accelerated progression to AIDS in macaques primed to mount a CD4 T cell response to the SIV envelope protein

Enhanced SIV replication and accelerated progression to AIDS in macaques primed to mount a CD4 T cell response to the SIV envelope protein

Antiviral Activity and Conformational Features of an Octapeptide Derived from the Membrane-Proximal Ectodomain of the Feline Immunodeficiency Virus Transmembrane Glycoprotein

Antibodies specific for hypervariable regions 3 to 5 of the feline immunodeficiency virus envelope glycoprotein are not solely responsible for vaccine-induced acceleration of challenge infection in cats

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