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.

Journal of immune based therapies and vaccines Pub Date : 2008-10-31 DOI:10.1186/1476-8518-6-7

Anna A Herasimtschuk, Samantha J Westrop, Graeme J Moyle, Jocelyn S Downey, Nesrina Imami

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Abstract

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.

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重组人生长激素对 HAART 患者 HIV-1 特异性 T 细胞反应、胸腺输出和病毒 DNA 的影响：48 周随访。

背景：治疗慢性 HIV-1 感染的有效免疫疗法需要诱导病毒特异性 CD4+ T 细胞，以及随后特异性记忆 CD8+ T 细胞的成熟和维持。在患有脂肪营养不良的慢性感染患者中，每天同时服用重组人生长激素（rhGH）和高活性抗逆转录病毒疗法（HAART），试图重建这些病毒特异性T细胞反应：接受HAART治疗的HIV-1慢性感染者参加了一项随机、双盲、安慰剂对照研究，接受rhGH治疗。我们在以下时间点评估了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，量化了胸腺输出和病毒HIV-1 DNA：基线；rhGH 治疗 12 周后；24 周时，随机分为三组[安慰剂第 12-24 周（A 组）、隔日给药第 12-24 周（B 组）和每周两次给药第 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，每天服用rhGH后，增殖性CD4+和产生IFN-gamma的CD8+ HIV-1特异性T细胞反应均明显增加。这种增加主要集中在HIV-1 Gag特异性T细胞反应上。在随后随机分配不同给药方案后，接受较少次数rhGH给药的患者的HIV-1特异性增殖性CD4+ T细胞反应有所下降，而病毒特异性IFN-γ产生的CD8+ T细胞反应则维持了较长时间。胸腺输出量没有明显变化，大多数患者的细胞相关HIV-1 DNA保持稳定。抗 HIV-1 Nef 特异性 CD4+ T 细胞增殖反应的增加与病毒载量的减少相关，而 HIV-1 Gag 特异性 IFN-gamma 产生的 CD8+ T 细胞反应的增加与病毒载量的增加相关：这些数据的意义在于，每天服用rhGH和HAART，除了能改善HIV-1相关的脂肪营养不良外，还能以剂量依赖的方式逆转大多数接受治疗的HIV-1阳性患者的T淋巴细胞功能障碍。这种基于免疫的治疗策略用于治疗慢性 HIV-1 感染，可诱导病毒特异性 CD4+ T 细胞，这对随后 "启动 "和扩增病毒特异性 CD8+ T 细胞至关重要：GH in Lipoatrophy IMP22350。

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Journal of immune based therapies and vaccines

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