Kvale Dag, Ormaasen Vidar, Kran Anne-Marte Bakken, Johansson Carl Christian, Aukrust Pål, Aandahl Einar Martin, Frøland Stig S, Taskén Kjetil
Department of Infectious Diseases, Ullevål University Hospital, Oslo, Norway.
AIDS. 2006 Apr 4;20(6):813-20. doi: 10.1097/01.aids.0000218544.54586.f1.
To examine the immune modulating effects of cyclooxygenase type 2 (COX-2) inhibitors (COX-2i) in HIV-infected patients on combination antiretroviral treatment (CART).
In-depth substudy from an approved, open, controlled, randomized study comparing the immune modulating effects of CART in combination with COX-2i after 12 weeks.
Patients (n = 38) on long-term CART with stable viral load (VL) < 50,000 copies/ml and CD4+ T-cell counts > 100/microl were randomized to CART and rofecoxib 25 mg bid (n = 12) or celecoxib 400 mg bid (n = 12), or CART only without placebo (n = 14). Routine clinical chemistry, CD4+ and CD8+ counts and VL were safety parameters. Immunological parameters included C-reactive protein, beta2-microglobulin, Ig isotypes and IgG subclasses as well as several T-lymphocyte subsets. Non-parametric analyses were used throughout.
Prestudy experiments showed higher median intracellular expression of COX-2 in CD4+ (P = 0.048) and possibly CD8+ (P = 0.09) T cells from patients on CART compared with uninfected controls. In the clinical study, increased CD4+ T-cell counts were observed only in patients on COX-2i with VL < 50 copies/ml (P = 0.02). Decreased expression of CD38+ on CD8+ T cells and subsets as well as reductions in IgA and IgM (P < 0.03) were most pronounced in patients on COX-2i who had detectable VL (n = 6). COX-2i treatment enhanced the perforin content particularly in the differentiated CD27-/CD8+ T-cell subsets compared with controls (P = 0.05).
COX-2i together with CART improved markers for persistent immune activation, particularly in patients with viraemia, as well as enhanced perforin expression, and thereby strengthened COX-2 as a potential therapeutic target in HIV infection.
研究环氧化酶2(COX-2)抑制剂(COX-2i)对接受联合抗逆转录病毒治疗(CART)的HIV感染患者的免疫调节作用。
一项经批准的、开放的、对照的、随机研究的深入子研究,比较12周后CART联合COX-2i的免疫调节作用。
38例长期接受CART治疗、病毒载量(VL)稳定<50,000拷贝/ml且CD4+T细胞计数>100/μl的患者被随机分为三组,分别接受CART联合25mg罗非昔布每日两次(n = 12)或400mg塞来昔布每日两次(n = 12),或仅接受CART不使用安慰剂(n = 14)。常规临床化学、CD4+和CD8+计数以及VL为安全参数。免疫参数包括C反应蛋白、β2微球蛋白、免疫球蛋白亚型和IgG亚类以及几个T淋巴细胞亚群。全程采用非参数分析。
研究前实验显示,与未感染对照组相比,接受CART治疗患者的CD4+(P = 0.048)和可能的CD8+(P = 0.09)T细胞中COX-2的细胞内表达中位数更高。在临床研究中,仅在VL<50拷贝/ml的COX-2i治疗患者中观察到CD4+T细胞计数增加(P = 0.02)。在可检测到VL的COX-2i治疗患者(n = 6)中,CD8+T细胞及其亚群上CD38+的表达降低以及IgA和IgM的减少(P<0.03)最为明显。与对照组相比,COX-2i治疗尤其增强了分化的CD27-/CD8+T细胞亚群中的穿孔素含量(P = 0.05)。
COX-2i与CART联合使用可改善持续性免疫激活的标志物,特别是在病毒血症患者中,同时增强穿孔素表达,从而强化了COX-2作为HIV感染潜在治疗靶点的作用。
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