| Literature DB >> 25218293 |
Josianne Nitcheu Tefit1, Sandrine Crabé2, Bernard Orlandini3, Haylene Nell4, Albert Bendelac5, Shenglou Deng6, Paul B Savage7, Luc Teyton8, Vincent Serra9.
Abstract
We have assessed the immune-regulatory and adjuvant activities of a synthetic glycolipid, ABX196, a novel analog of the parental compound α-GalCer. As expected, ABX196 demonstrated a measurable and significant adjuvant effect in mice and monkeys with no appreciable toxicity at the doses used to promote immune responses. We performed a phase I/II dose escalation study of ABX196 in healthy volunteers, with the objectives to evaluate its safety profile, as well as its ability to be utilized as an adjuvant in the context of a prophylactic vaccine against hepatitis B. ABX196 was administered at three doses: 0.2, 0.4, and 2.0μg, in 44 subjects. In all the individuals injected with ABX196, peripheral blood NKT cells displayed hallmarks of activation, and 45% of them had measurable circulating IFN-γ 24h after the first administration. More importantly, the addition of ABX196 to the very poorly immunogenic HBs antigen resulted in protective anti-HBs antibody responses in majority of patients, demonstrating the adjuvant properties of ABX196 in human. Further analysis of the cohort of subjects receiving ABX196 with HBs antigen also indicates that a single injection appears sufficient to provide protection. A limited set of adverse events linked to the systemic delivery of ABX196 and access to the liver, is discussed in the context of formulation and the need to limit transport of ABX196 to secondary lymphoid tissues for maximal efficacy (Eudra-CT 2012-001566-15).Entities:
Keywords: ABX196; Adjuvant; Glycolipid; NKT cells; α-GalCer
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Year: 2014 PMID: 25218293 PMCID: PMC4233108 DOI: 10.1016/j.vaccine.2014.08.070
Source DB: PubMed Journal: Vaccine ISSN: 0264-410X Impact factor: 3.641