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接种MF59/重组gp120疫苗的HIV暴露婴儿比接种同一疫苗的成人具有更高水平的抗V1V2 IgG反应。

HIV-Exposed Infants Vaccinated with an MF59/Recombinant gp120 Vaccine Have Higher-Magnitude Anti-V1V2 IgG Responses than Adults Immunized with the Same Vaccine.

作者信息

McGuire Erin P, Fong Youyi, Toote Christopher, Cunningham Coleen K, McFarland Elizabeth J, Borkowsky William, Barnett Susan, Itell Hannah L, Kumar Amit, Gray Glenda, McElrath M Julianna, Tomaras Georgia D, Permar Sallie R, Fouda Genevieve G

机构信息

Duke University, Durham, North Carolina, USA.

HIV Vaccine Trials Network, Seattle, Washington, USA.

出版信息

J Virol. 2017 Dec 14;92(1). doi: 10.1128/JVI.01070-17. Print 2018 Jan 1.

Abstract

In the RV144 vaccine trial, IgG responses against the HIV envelope variable loops 1 and 2 (V1V2) were associated with decreased HIV acquisition risk. We previously reported that infants immunized with an MF59-adjuvanted rgp120 vaccine developed higher-magnitude anti-V1V2 IgG responses than adult RV144 vaccinees. To determine whether the robust antibody response in infants is due to differences in vaccine regimens or to inherent differences between the adult and infant immune systems, we compared Env-specific IgG responses in adults and infants immunized with the same MF59- and alum-adjuvanted HIV envelope vaccines. At peak immunogenicity, the magnitudes of the gp120- and V1V2-specific IgG responses were comparable between adults and infants immunized with the alum/MNrgp120 vaccine (gp120 median fluorescence intensities [FIs] in infants = 7,118 and in adults = 11,510, = 0.070; V1V2 median MFIs of 512 [infants] and 804 [adults], = 0.50), whereas infants immunized with the MF59/SF-2 rgp120 vaccine had higher-magnitude antibody levels than adults (gp120 median FIs of 15,509 [infants] and 2,290 [adults], < 0.001; V1V2 median FIs of 23,926 [infants] and 1,538 [adults]; < 0.001). Six months after peak immunogenicity, infants maintained higher levels Env-specific IgG than adults. Anti-V1V2 IgG3 antibodies that were associated with decreased HIV-1 risk in RV144 vaccinees were present in 43% of MF59/rgp120-vaccinated infants but only in 12% of the vaccinated adults ( = 0.0018). Finally, in contrast to the rare vaccine-elicited Env-specific IgA in infants, rgp120 vaccine-elicited Env-specific IgA was frequently detected in adults. Our results suggest that vaccine adjuvants differently modulate gp120-specific antibody responses in adults and infants and that infants can robustly respond to HIV Env immunization. More than 150,000 pediatric HIV infections occur yearly, despite the availability of antiretroviral prophylaxis. A pediatric HIV vaccine could reduce the number of these ongoing infant infections and also prime for long-term immunity prior to sexual debut. We previously reported that immunization of infants with an MF59-adjuvanted recombinant gp120 vaccine induced higher-magnitude, potentially protective anti-V1V2 IgG responses than in adult vaccinees receiving the moderately effective RV144 vaccine. In the present study, we demonstrate that the robust response observed in infants is not due to differences in vaccine regimen or vaccine dose between adults and infants. Our results suggest that HIV vaccine adjuvants may differentially modulate immune responses in adults and infants, highlighting the need to conduct vaccine trials in pediatric populations.

摘要

在RV144疫苗试验中,针对HIV包膜可变环1和2(V1V2)的IgG反应与HIV感染风险降低相关。我们之前报道过,用MF59佐剂化的rgp120疫苗免疫的婴儿产生的抗V1V2 IgG反应强度高于成人RV144疫苗接种者。为了确定婴儿中强烈的抗体反应是由于疫苗接种方案的差异还是成人和婴儿免疫系统的固有差异,我们比较了用相同的MF59和明矾佐剂化的HIV包膜疫苗免疫的成人和婴儿中Env特异性IgG反应。在免疫原性峰值时,用明矾/MNrgp120疫苗免疫的成人和婴儿中,gp120和V1V2特异性IgG反应的强度相当(婴儿中gp120的中位荧光强度[FI] = 7,118,成人中为11,510,P = 0.070;婴儿中V1V2的中位MFI为512,成人中为804,P = 0.50),而用MF59/SF - 2 rgp120疫苗免疫的婴儿的抗体水平高于成人(婴儿中gp120的中位FI为15,509,成人中为2,290,P < 0.001;婴儿中V1V2的中位FI为23,926,成人中为1,538;P < 0.001)。免疫原性峰值六个月后,婴儿维持的Env特异性IgG水平高于成人。与RV144疫苗接种者中与HIV - 1风险降低相关的抗V1V2 IgG3抗体在43%的MF59/rgp120疫苗接种的婴儿中存在,但仅在12%的接种成人中存在(P = 0.0018)。最后,与婴儿中罕见的疫苗诱导的Env特异性IgA相反,rgp120疫苗诱导的Env特异性IgA在成人中经常被检测到。我们的结果表明,疫苗佐剂对成人和婴儿中gp120特异性抗体反应的调节不同,并且婴儿能够对HIV Env免疫产生强烈反应。尽管有抗逆转录病毒预防措施,但每年仍有超过15万例儿童感染HIV。一种儿童HIV疫苗可以减少这些正在发生的婴儿感染数量,并在首次性行为之前引发长期免疫。我们之前报道过,用MF59佐剂化的重组gp120疫苗免疫婴儿诱导的抗V1V2 IgG反应强度高于接受中等效力的RV144疫苗的成人疫苗接种者。在本研究中,我们证明在婴儿中观察到的强烈反应不是由于成人和婴儿之间的疫苗接种方案或疫苗剂量的差异。我们的结果表明,HIV疫苗佐剂可能对成人和婴儿的免疫反应有不同的调节作用,突出了在儿童人群中进行疫苗试验的必要性。

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