疫苗诱导的CD107a+ CD4+ T细胞在感染艾滋病病毒后对耗竭具有抗性。
Vaccine-induced CD107a+ CD4+ T cells are resistant to depletion following AIDS virus infection.
作者信息
Terahara Kazutaka, Ishii Hiroshi, Nomura Takushi, Takahashi Naofumi, Takeda Akiko, Shiino Teiichiro, Tsunetsugu-Yokota Yasuko, Matano Tetsuro
机构信息
Department of Immunology, National Institute of Infectious Diseases, Tokyo, Japan.
AIDS Research Center, National Institute of Infectious Diseases, Tokyo, Japan.
出版信息
J Virol. 2014 Dec;88(24):14232-40. doi: 10.1128/JVI.02032-14. Epub 2014 Oct 1.
UNLABELLED
CD4(+) T-cell responses are crucial for effective antibody and CD8(+) T-cell induction following virus infection. However, virus-specific CD4(+) T cells can be preferential targets for human immunodeficiency virus (HIV) infection. HIV-specific CD4(+) T-cell induction by vaccination may thus result in enhancement of virus replication following infection. In the present study, we show that vaccine-elicited CD4(+) T cells expressing CD107a are relatively resistant to depletion in a macaque AIDS model. Comparison of virus-specific CD107a, macrophage inflammatory protein-1β, gamma interferon, tumor necrosis factor alpha, and interleukin-2 responses in CD4(+) T cells of vaccinated macaques prechallenge and 1 week postchallenge showed a significant reduction in the CD107a(-) but not the CD107a(+) subset after virus exposure. Those vaccinees that failed to control viremia showed a more marked reduction and exhibited significantly higher viral loads at week 1 than unvaccinated animals. Our results indicate that vaccine-induced CD107a(-) CD4(+) T cells are depleted following virus infection, suggesting a rationale for avoiding virus-specific CD107a(-) CD4(+) T-cell induction in HIV vaccine design.
IMPORTANCE
Induction of effective antibody and/or CD8(+) T-cell responses is a principal vaccine strategy against human immunodeficiency virus (HIV) infection. CD4(+) T-cell responses are crucial for effective antibody and CD8(+) T-cell induction. However, virus-specific CD4(+) T cells can be preferential targets for HIV infection. Here, we show that vaccine-induced virus-specific CD107a(-) CD4(+) T cells are largely depleted following infection in a macaque AIDS model. While CD4(+) T-cell responses are important in viral control, our results indicate that virus-specific CD107a(-) CD4(+) T-cell induction by vaccination may not lead to efficient CD4(+) T-cell responses following infection but rather be detrimental and accelerate viral replication in the acute phase. This suggests that HIV vaccine design should avoid virus-specific CD107a(-) CD4(+) T-cell induction. Conversely, this study found that vaccine-induced CD107a(+) CD4(+) T cells are relatively resistant to depletion following virus challenge, implying that induction of these cells may be an alternative approach toward HIV control.
未标记
CD4(+) T细胞反应对于病毒感染后有效诱导抗体和CD8(+) T细胞至关重要。然而,病毒特异性CD4(+) T细胞可能是人类免疫缺陷病毒(HIV)感染的优先靶标。因此,通过疫苗接种诱导HIV特异性CD4(+) T细胞可能会导致感染后病毒复制增强。在本研究中,我们表明在猕猴艾滋病模型中,表达CD107a的疫苗诱导的CD4(+) T细胞对耗竭相对具有抗性。比较接种疫苗的猕猴在攻毒前和攻毒后1周时CD4(+) T细胞中病毒特异性CD107a、巨噬细胞炎性蛋白-1β、γ干扰素、肿瘤坏死因子α和白细胞介素-2的反应,结果显示病毒暴露后CD107a(-)亚群而非CD107a(+)亚群显著减少。那些未能控制病毒血症的疫苗接种者显示出更明显的减少,并且在第1周时病毒载量显著高于未接种疫苗的动物。我们的结果表明,疫苗诱导的CD107a(-) CD4(+) T细胞在病毒感染后会被耗竭,这为在HIV疫苗设计中避免诱导病毒特异性CD107a(-) CD4(+) T细胞提供了理论依据。
重要性
诱导有效的抗体和/或CD8(+) T细胞反应是对抗人类免疫缺陷病毒(HIV)感染的主要疫苗策略。CD4(+) T细胞反应对于有效诱导抗体和CD8(+) T细胞至关重要。然而,病毒特异性CD4(+) T细胞可能是HIV感染的优先靶标。在这里,我们表明在猕猴艾滋病模型中,疫苗诱导的病毒特异性CD107a(-) CD4(+) T细胞在感染后大部分被耗竭。虽然CD4(+) T细胞反应在病毒控制中很重要,但我们的结果表明,通过疫苗接种诱导病毒特异性CD107a(-) CD4(+) T细胞可能不会导致感染后有效的CD4(+) T细胞反应,反而可能有害并加速急性期的病毒复制。这表明HIV疫苗设计应避免诱导病毒特异性CD107a(-) CD4(+) T细胞。相反,本研究发现疫苗诱导的CD107a(+) CD4(+) T细胞在病毒攻击后对耗竭相对具有抗性,这意味着诱导这些细胞可能是控制HIV的另一种方法。
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