Tuero Iskra, Mohanram Venkatramanan, Musich Thomas, Miller Leia, Vargas-Inchaustegui Diego A, Demberg Thorsten, Venzon David, Kalisz Irene, Kalyanaraman V S, Pal Ranajit, Ferrari Maria Grazia, LaBranche Celia, Montefiori David C, Rao Mangala, Vaccari Monica, Franchini Genoveffa, Barnett Susan W, Robert-Guroff Marjorie
Immune Biology of Retroviral Infection Section, Vaccine Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland, United States of America.
Biostatistics and Data Management Section, National Cancer Institute, National Institutes of Health, Bethesda, Maryland, United States of America.
PLoS Pathog. 2015 Aug 12;11(8):e1005101. doi: 10.1371/journal.ppat.1005101. eCollection 2015 Aug.
Many viral infections, including HIV, exhibit sex-based pathogenic differences. However, few studies have examined vaccine-related sex differences. We compared immunogenicity and protective efficacy of monomeric SIV gp120 with oligomeric SIV gp140 in a pre-clinical rhesus macaque study and explored a subsequent sex bias in vaccine outcome. Each immunization group (16 females, 8 males) was primed twice mucosally with replication-competent Ad-recombinants encoding SIVsmH4env/rev, SIV239gag and SIV239nefΔ1-13 and boosted twice intramuscularly with SIVmac239 monomeric gp120 or oligomeric gp140 in MF59 adjuvant. Controls (7 females, 5 males) received empty Ad and MF59. Up to 9 weekly intrarectal challenges with low-dose SIVmac251 were administered until macaques became infected. We assessed vaccine-induced binding, neutralizing, and non-neutralizing antibodies, Env-specific memory B cells and plasmablasts/plasma cells (PB/PC) in bone marrow and rectal tissue, mucosal Env-specific antibodies, and Env-specific T-cells. Post-challenge, only one macaque (gp140-immunized) remained uninfected. However, SIV acquisition was significantly delayed in vaccinated females but not males, correlated with Env-specific IgA in rectal secretions, rectal Env-specific memory B cells, and PC in rectal tissue. These results extend previous correlations of mucosal antibodies and memory B cells with protective efficacy. The gp140 regimen was more immunogenic, stimulating elevated gp140 and cyclic V2 binding antibodies, ADCC and ADCP activities, bone marrow Env-specific PB/PC, and rectal gp140-specific IgG. However, immunization with gp120, the form of envelope immunogen used in RV144, the only vaccine trial to show some efficacy, provided more significant acquisition delay. Further over 40 weeks of follow-up, no gp120 immunized macaques met euthanasia criteria in contrast to 7 gp140-immunized and 2 control animals. Although males had higher binding antibodies than females, ADCC and ADCP activities were similar. The complex challenge outcomes may reflect differences in IgG subtypes, Fc glycosylation, Fc-R polymorphisms, and/or the microbiome, key areas for future studies. This first demonstration of a sex-difference in SIV vaccine-induced protection emphasizes the need for sex-balancing in vaccine trials. Our results highlight the importance of mucosal immunity and memory B cells at the SIV exposure site for protection.
许多病毒感染,包括HIV感染,都表现出基于性别的致病差异。然而,很少有研究探讨与疫苗相关的性别差异。在一项临床前恒河猴研究中,我们比较了单体SIV gp120与寡聚体SIV gp140的免疫原性和保护效力,并探讨了疫苗效果中随后出现的性别偏差。每个免疫组(16只雌性,8只雄性)先用编码SIVsmH4env/rev、SIV239gag和SIV239nefΔ1-13的具有复制能力的腺病毒重组体进行两次黏膜初免,然后用MF59佐剂中的SIVmac239单体gp120或寡聚体gp140进行两次肌肉注射加强免疫。对照组(7只雌性,5只雄性)接受空腺病毒和MF59。对猕猴进行多达9次每周一次的低剂量SIVmac251直肠内攻击,直至猕猴被感染。我们评估了疫苗诱导的结合抗体、中和抗体和非中和抗体、Env特异性记忆B细胞以及骨髓和直肠组织中的浆母细胞/浆细胞(PB/PC)、黏膜Env特异性抗体和Env特异性T细胞。攻击后,只有一只猕猴(gp140免疫组)未被感染。然而,接种疫苗的雌性猕猴感染SIV的时间显著延迟,而雄性则没有,这与直肠分泌物中的Env特异性IgA、直肠Env特异性记忆B细胞以及直肠组织中的PC相关。这些结果扩展了先前关于黏膜抗体和记忆B细胞与保护效力之间的相关性。gp140方案具有更强的免疫原性,能刺激产生更高水平的gp140和循环V2结合抗体、ADCC和ADCP活性、骨髓Env特异性PB/PC以及直肠gp140特异性IgG。然而,用gp120免疫(RV144中使用的包膜免疫原形式,是唯一一项显示出一定疗效的疫苗试验)能提供更显著的感染延迟。在超过40周的随访中,没有gp120免疫的猕猴达到安乐死标准,而7只gp140免疫的猕猴和2只对照动物达到了。尽管雄性的结合抗体水平高于雌性,但ADCC和ADCP活性相似。复杂的攻击结果可能反映了IgG亚型、Fc糖基化、Fc-R多态性和/或微生物群的差异,这些是未来研究的关键领域。这首次证明了SIV疫苗诱导的保护存在性别差异,强调了疫苗试验中性别平衡的必要性。我们的结果突出了SIV暴露部位的黏膜免疫和记忆B细胞对保护的重要性。
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