IMP321 (sLAG-3), an immunopotentiator for T cell responses against a HBsAg antigen in healthy adults: a single blind randomised controlled phase I study.

Journal of immune based therapies and vaccines Pub Date : 2007-03-29 DOI:10.1186/1476-8518-5-5

Chrystelle Brignone, Caroline Grygar, Manon Marcu, Gaëlle Perrin, Frédéric Triebel

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引用次数: 32

Abstract

Background: LAG-3 (CD223) is a natural high affinity ligand for MHC class II. The soluble form (sLAG-3) induces maturation of monocyte-derived dendritic cells in vitro and is used as a potent Th1-like immune enhancer with many antigens in animal models. To extend this observation to human, a proof of concept study was conducted with a clinical-grade sLAG-3, termed IMP321, coinjected with alum-non-absorbed recombinant hepatitis B surface antigen.

Methods: In a randomised, single blind controlled phase I dose escalation study, 48 seronegative healthy volunteers aged 18-55 years were vaccinated at 0, 4 and 8 weeks by subcutaneous injection with 10 microg HBsAg mixed with saline (control) or with IMP321 at one of four doses (3, 10, 30 and 100 microg). To evaluate the efficacy of this three injections over 2 months immunization protocol, an additional control group was injected with the commercial vaccine Engerix-B.

Results: IMP321 was very well tolerated. Indeed, a lower incidence of adverse events was reported from the HBsAg plus IMP321 groups than from the Engerix-B group. HBsAg-specific antibody responses (anti-HBs) appeared sooner and were higher at 8 and 12 weeks in IMP321 recipients compared to HBsAg control subjects. More importantly, increased numbers of responders to HBsAg were found in IMP321 recipients compared HBsAg group, as revealed by higher post-vaccination frequencies of CD4 Th1 or CD8 Tc1 antigen specific T cells. IMP321 induced CD4 Th1 antigen-specific T cells in some of these naïve individuals after only one injection, especially in the 10 and 30 microg dose groups.

Conclusion: IMP321 as an adjuvant to HBsAg was well-tolerated and enhanced T cell response vaccine immunogenicity (i.e. induced both CD4 Th1 and CD8 Tc1 antigen-specific T cells). This latter property has allowed the development of IMP321 as an immunopotentiator for therapeutic vaccines.

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IMP321 (sLAG-3)，一种针对健康成人HBsAg抗原的T细胞应答免疫增强剂:一项单盲随机对照I期研究

背景:LAG-3 (CD223)是MHC II类的天然高亲和力配体。可溶性形式(sLAG-3)在体外诱导单核细胞来源的树突状细胞成熟，并在动物模型中被用作具有多种抗原的强效th1样免疫增强剂。为了将这一观察结果扩展到人类，将临床级sLAG-3(称为IMP321)与铝非吸收重组乙型肝炎表面抗原共注射，进行了概念验证研究。方法:在一项随机、单盲对照I期剂量递增研究中，48名年龄在18-55岁的血清阴性健康志愿者在0、4和8周时皮下注射10微克HBsAg混合生理盐水(对照)或IMP321，注射剂量为4种剂量(3、10、30和100微克)中的一种。为了评估这三次超过2个月的免疫方案的效果，另外一组对照组注射了商业疫苗Engerix-B。结果:IMP321耐受性良好。事实上，HBsAg + IMP321组的不良事件发生率低于Engerix-B组。与HBsAg对照组相比，在8周和12周时，IMP321受体的HBsAg特异性抗体反应(anti-HBs)出现得更快，更高。更重要的是，与HBsAg组相比，IMP321受体中HBsAg应答者的数量增加，这是由接种后CD4 Th1或CD8 Tc1抗原特异性T细胞的更高频率所揭示的。仅在一次注射后，在这些naïve个体中，特别是在10和30微剂量组，IMP321诱导CD4 Th1抗原特异性T细胞。结论:IMP321作为HBsAg佐剂具有良好的耐受性和增强T细胞应答疫苗的免疫原性(即诱导CD4 Th1和CD8 Tc1抗原特异性T细胞)。后一种特性使得IMP321成为治疗性疫苗的免疫增强剂。

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Journal of immune based therapies and vaccines

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