重组人生长激素对接受高效抗逆转录病毒治疗(HAART)患者的HIV-1特异性T细胞反应、胸腺输出及前病毒DNA的影响:48周随访
Effects of recombinant human growth hormone on HIV-1-specific T-cell responses, thymic output and proviral DNA in patients on HAART: 48-week follow-up.
作者信息
Herasimtschuk Anna A, Westrop Samantha J, Moyle Graeme J, Downey Jocelyn S, Imami Nesrina
机构信息
Department of Immunology, Imperial College London, Chelsea and Westminster Hospital, 369 Fulham Road, London, SW10 9NH, UK .
出版信息
J Immune Based Ther Vaccines. 2008 Oct 31;6:7. doi: 10.1186/1476-8518-6-7.
BACKGROUND
Efficacious immune-based therapy in treated chronic HIV-1 infection requires the induction of virus-specific CD4+ T cells and subsequent maturation and maintenance of specific memory CD8+ T cells. Concomitant daily administration of recombinant human growth hormone (rhGH) with highly active antiretroviral therapy (HAART) was used in chronically infected patients with lipodystrophy in an attempt to reconstitute these virus-specific T-cell responses.
METHODS
Individuals with chronic HIV-1 infection on HAART were enrolled on a randomized, double-blinded, placebo-controlled study to receive rhGH therapy. We assessed HIV-1-specific proliferative CD4+ and interferon-gamma (IFN-gamma)-producing CD8+ T-cell responses, quantified thymic output and proviral HIV-1 DNA at the following time points: baseline; after 12 weeks of rhGH therapy; at 24 weeks, after randomization into three groups [placebo weeks 12-24 (Group A), alternate-day dosing weeks 12-24 (Group B), and twice-per-week dosing weeks 12-24 (Group C)]; and at 48 weeks after all patients had received HAART alone for the final 24 weeks.
RESULTS
We found significant increases in both proliferative CD4+ and IFN-gamma-producing CD8+ HIV-1-specific T-cell responses after daily administration of rhGH. This increase was focused on HIV-1 Gag-specific T-cell responses. Following subsequent randomisation into different dosing regimens, HIV-1-specific proliferative CD4+ T-cell responses declined in patients receiving less frequent dosing of rhGH, while virus-specific IFN-gamma-producing CD8+ T-cell responses were maintained for longer periods of time. There was no significant change in thymic output and the cell-associated HIV-1 DNA remained stable in most patients. An increased anti-HIV-1 Nef-specific CD4+ T-cell proliferative response was correlated to a decrease in proviral load, and an increased HIV-1 Gag-specific IFN-gamma-producing CD8+ T-cell response correlated with an increase in proviral load.
CONCLUSION
The implication of these data is that daily dosing of rhGH with HAART, in addition to improving HIV-1-associated lipodystrophy, may reverse some of the T-lymphocyte dysfunction seen in most treated HIV-1-positive patients, in a dose-dependent manner. Such immune-based therapeutic strategies used in treated, chronic HIV-1 infection may enable the induction of virus-specific CD4+ T cells essential for the subsequent 'kick-start' and expansion of virus-specific CD8+ T cells.
TRIAL REGISTRATION
GH in Lipoatrophy IMP22350.
背景
在接受治疗的慢性HIV-1感染中,有效的免疫治疗需要诱导病毒特异性CD4+ T细胞,并随后使特异性记忆CD8+ T细胞成熟和维持。在患有脂肪代谢障碍的慢性感染患者中,将重组人生长激素(rhGH)与高效抗逆转录病毒疗法(HAART)联合每日给药,试图重建这些病毒特异性T细胞反应。
方法
对接受HAART治疗的慢性HIV-1感染者进行一项随机、双盲、安慰剂对照研究,以接受rhGH治疗。我们在以下时间点评估HIV-1特异性增殖性CD4+和产生干扰素-γ(IFN-γ)的CD8+ T细胞反应,量化胸腺输出和前病毒HIV-1 DNA:基线;rhGH治疗12周后;随机分为三组后的24周[安慰剂组第12 - 24周(A组)、隔日给药组第12 - 24周(B组)和每周两次给药组第12 - 24周(C组)];以及所有患者在最后24周单独接受HAART治疗后的48周。
结果
我们发现每日给予rhGH后,增殖性CD4+和产生IFN-γ的CD8+ HIV-1特异性T细胞反应均显著增加。这种增加主要集中在HIV-1 Gag特异性T细胞反应上。在随后随机分为不同给药方案后,接受rhGH给药频率较低的患者中,HIV-1特异性增殖性CD4+ T细胞反应下降,而病毒特异性产生IFN-γ的CD8+ T细胞反应维持较长时间。大多数患者的胸腺输出无显著变化,细胞相关HIV-1 DNA保持稳定。抗HIV-1 Nef特异性CD4+ T细胞增殖反应增加与前病毒载量降低相关,HIV-1 Gag特异性产生IFN-γ的CD8+ T细胞反应增加与前病毒载量增加相关。
结论
这些数据表明,rhGH与HAART联合每日给药,除了改善HIV-1相关脂肪代谢障碍外,可能以剂量依赖的方式逆转大多数接受治疗的HIV-1阳性患者中出现的一些T淋巴细胞功能障碍。在接受治疗的慢性HIV-1感染中使用这种基于免疫的治疗策略,可能能够诱导病毒特异性CD4+ T细胞,这对于随后病毒特异性CD8+ T细胞的“启动”和扩增至关重要。
试验注册
GH in Lipoatrophy IMP22350
Zotero 插件