A randomised, placebo-controlled, first-in-human study of a novel clade C therapeutic peptide vaccine administered ex vivo to autologous white blood cells in HIV infected individuals

Akil Jackson, Henrik N Kløverpris, Marta Boffito, Amanda Handley, Mark Atkins, Peter Hayes, Jill Gilmour, Lynn Riddel, Fabian Chen, Melanie Bailey-Tippets, Bruce Walker, Jim Ackland, Mark Sullivan, Philip Goulder, Akil Jackson, Henrik N Kløverpris, Marta Boffito, Amanda Handley, Mark Atkins, Peter Hayes, Jill Gilmour, Lynn Riddel, Fabian Chen, Melanie Bailey-Tippets, Bruce Walker, Jim Ackland, Mark Sullivan, Philip Goulder

Abstract

Background: Preclinical studies of overlapping 15mer peptides, spanning SIV, SHIV or HIV, pulsed on autologous PBMC ex vivo have demonstrated high level, virus-specific T cell responses and viral suppression in non-human primates (NHP). Opal-HIV-Gag(c) consists of 120 synthetic 15mer peptides spanning Clade C, consensus Gag, manufactured to current good manufacturing practice; having been evaluated in a good laboratory practice toxicology study in Macaca mulatta. We evaluated the safety and preliminary immunogenicity of such peptides administered intravenously after short-duration ex vivo incubation, to HIV-positive adults on suppressive antiretroviral therapy.

Methods and findings: A first-in-human, placebo-controlled, double-blind, dose escalation study was conducted. Twenty-three patients with virus suppressed by antiretroviral therapy were enrolled in four groups 12 mg (n = 6), 24 mg (n = 6), 48 mg (n = 2) or matching placebo (n = 8). Treatment was administered intravenously after bedside enrichment of 120 mL whole blood for white cells using a closed system (Sepax S-100 device), with ex vivo peptide admixture (or diluent alone) and 37°C incubation for one hour prior to reinfusion. Patients received 4 administrations at monthly intervals followed by a 12-week observation post-treatment. Opal-HIV-Gag(c) was reasonably tolerated at doses of 12 and 24 mg. There was an increased incidence of temporally associated pyrexia, chills, and transient/self-limiting lymphopenia in Opal-HIV-Gag(c) recipients compared to placebo. The study was terminated early, after two patients were recruited to the 48 mg cohort; a serious adverse event of hypotension, tachycardia secondary to diarrhoea occurred following a single product administration. An infectious cause for the event could not be identified, leaving the possibility of immunologically mediated product reaction.

Conclusions: A serious, potentially life-threatening event of hypotension led to early, precautionary termination of the study. In the absence of a clearly defined mechanism or ability to predict such occurrence, further development of Opal-HIV-Gag(c) will not be undertaken in the current form.

Registration: ClinicalTrials.gov NCT01123915; EudraCT: 2008-005142-23.

Conflict of interest statement

Competing Interests: MS and AH are employees of the study sponsor, Medicines Development Limited, a not-for-profit company. MB-T is an employee of iNC Research, responsible for data management and statistical analysis of the study. JA is an employee of Global Biosolutions, involved in product development, manufacture and regulatory oversight. This does not alter our adherence to all the PLOS ONE policies on sharing data and materials.

References

    1. UNAIDS JUNPOHA, editor (n.d.) Global report: UNAIDS report on the global AIDS epidemic 2012. WHO Library Cataloguing-in-Publication Data. 1 p. Available: Accessed 11Jul22013.
    1. Goulder PJRP, Walker BDB (2012) HIV and HLA class I: an evolving relationship. Immunity 37: 426–440 doi:
    1. Mudd PAP, Martins MAM, Ericsen AJA, Tully DCD, Power KAK, et al. (2012) Vaccine-induced CD8+ T cells control AIDS virus replication. Nature 491: 129–133 doi:
    1. Barouch DHD, Liu JJ, Li HH, Maxfield LFL, Abbink PP, et al. (2012) Vaccine protection against acquisition of neutralization-resistant SIV challenges in rhesus monkeys. Nature 482: 89–93 doi:
    1. Goepfert PAP, Lumm WW, Farmer PP, Matthews PP, Prendergast AA, et al. (2008) Transmission of HIV-1 Gag immune escape mutations is associated with reduced viral load in linked recipients. J Exp Med 205: 1009–1017 doi:
    1. Kiepiela PP, Ngumbela KK, Thobakgale CC, Ramduth DD, Honeyborne II, et al. (2007) CD8+ T-cell responses to different HIV proteins have discordant associations with viral load. Nat Med 13: 46–53 doi:
    1. Chea SS, Dale CJC, De Rose RR, Ramshaw IAI, Kent SJS (2005) Enhanced cellular immunity in macaques following a novel peptide immunotherapy. J Virol 79: 3748–3757 doi:
    1. De Rose R, Fernandez CS, Loh L, Peut V, Mason RD, et al. (2008) Delivery of immunotherapy with peptide-pulsed blood in macaques. Virology 378: 201–204 doi:
    1. De Rose RR, Mason RDR, Loh LL, Peut VV, Smith MZM, et al. (2008) Safety, immunogenicity and efficacy of peptide-pulsed cellular immunotherapy in macaques. J Med Primatol 37 Suppl 269–78 doi:
    1. De Rose R, Fernandez CS, Smith MZ, Batten CJ, Alcântara S, et al. (2008) Control of viremia and prevention of AIDS following immunotherapy of SIV-infected macaques with peptide-pulsed blood. PLoS Pathog 4: e1000055 doi:
    1. Geels MJM, Dubey SAS, Anderson KK, Baan EE, Bakker MM, et al. (2005) Broad cross-clade T-cell responses to gag in individuals infected with human immunodeficiency virus type 1 non-B clades (A to G): importance of HLA anchor residue conservation. J Virol 79: 11247–11258 doi:
    1. Taylor BS, Sobieszczyk ME, McCutchan FE, Hammer SM (2008) The Challenge of HIV-1 Subtype Diversity. N Engl J Med 358: 1590–1602 doi:
    1. CDER F (1997) Guidance for Industry: General considerations for the clinical evaluation of drugs. U.S. Department of Health and Human Services - Food and Drug Administration- Center for Drug Evaluation and Research (CDER). Available: . Accessed 11July,2013.
    1. Guidance for Industry - Estimating the Maximum Safe Starting Dose in Initial Clinical Trials for Therapeutics in Adult Healthy Volunteers (2005) U.S. Department of Health and Human Services - Food and Drug Administration - Center for Drug Evaluation and Research (CDER). Available: . Accessed 11July,2013.
    1. Chow S-C, Liu J-P (2008) Design and Analysis of Clinical Trials. Wiley-Interscience. 1 pp.
    1. Haining WNW, Davies JJ, Kanzler HH, Drury LL, Brenn TT, et al. (2008) CpG oligodeoxynucleotides alter lymphocyte and dendritic cell trafficking in humans. Clin Cancer Res 14: 5626–5634 doi:
    1. Ferrucci PF, Martinoni A, Cocorocchio E, Civelli M, Cinieri S, et al. (2000) Evaluation of acute toxicities associated with autologous peripheral blood progenitor cell reinfusion in patients undergoing high-dose chemotherapy. Bone Marrow Transplant 25: 173–177.
    1. Windrum PP, Morris TCMT, Drake MBM, Niederwieser DD, Ruutu TT (2005) Variation in dimethyl sulfoxide use in stem cell transplantation: a survey of EBMT centres. Bone Marrow Transplant 36: 601–603 doi:
    1. Rowley SDS, Feng ZZ, Yadock DD, Holmberg LL, Macleod BB, et al. (1999) Post-thaw removal of DMSO does not completely abrogate infusional toxicity or the need for pre-infusion histamine blockade. Cytotherapy 1: 439–446 doi:
    1. McKim AS, Strub R (2008) Dimethyl sulfoxide USP, PhEur in approved pharmaceutical products and medical devices.
    1. Staprans SIS, Feinberg MBM (2004) The roles of nonhuman primates in the preclinical evaluation of candidate AIDS vaccines. Expert Rev Vaccines 3: S5–S32.
    1. Girard MP, Plotkin SA (2012) HIV vaccine development at the turn of the 21st century. Curr Opin HIV AIDS 7: 4–9 doi:

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