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Epstein-Barr virus genome load is increased by therapeutic vaccination in HIV-1 carriers, and further enhanced in patients with a history of symptomatic primary infection

机译:在HIV-1携带者中进行治疗性疫苗接种会增加爱泼斯坦-巴尔病毒的基因组负荷,在有症状的原发感染史患者中进一步增加

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Objective Epstein–Barr virus (EBV) infection is an established risk factor for B-cell lymphomas in Human Immunodeficiency virus (HIV)-1 infected patients. A disturbed EBV-host relationship is seen in patient groups with a high risk for EBV-associated lymphomas. We have analysed this relationship by measuring EBV-DNA in the blood of HIV-1 carriers. Method EBV-DNA load in B-cells was monitored by PCR in non- or insufficiently antiretroviral treated and rgp160-vaccinated HIV-patients. Results Both asymptomatic HIV-infected and AIDS-patients showed a 25–40-fold increase in the number of B cell associated EBV-DNA copies compared to healthy controls. Patients included in a vaccine trial with recombinant HIV gp160 showed a 5-fold increase of EBV load compared to non-immunised patients and a 50-fold increase compared to healthy controls. There was no difference whether they received vaccine or “placebo”. Vaccinated patients with a history of symptomatic primary HIV-1 infection (PHI) had a 280-fold increase in median EBV load compared to healthy controls, thus suggesting a synergistic effect between the vaccination and PHI, which hypothetically could affect lymphoma risk. Conclusions We recommend analysis of EBV-load and long term follow up of lymphoma risk in all therapeutic HIV-1 vaccination trials.
机译:客观爱泼斯坦-巴尔病毒(EBV)感染是人类免疫缺陷病毒(HIV)-1感染患者B细胞淋巴瘤的既定危险因素。在患有EBV相关淋巴瘤的高风险患者组中发现EBV宿主关系受到干扰。我们通过测量HIV-1携带者血液中的EBV-DNA分析了这种关系。方法通过PCR监测未经抗逆转录病毒治疗或未经rgp160接种的HIV患者的B细胞EBV-DNA负载。结果与健康对照组相比,无症状HIV感染者和AIDS患者的B细胞相关EBV-DNA拷贝数均增加了25-40倍。与未免疫的患者相比,参与重组HIV gp160疫苗试验的患者的EBV负荷增加了5倍,与健康对照相比增加了50倍。他们接受疫苗还是“安慰剂”没有区别。有症状的原发性HIV-1感染病史(PHI)的疫苗接种患者的EBV负荷中位数比健康对照组高280倍,因此表明疫苗接种与PHI有协同作用,假设可能影响淋巴瘤的风险。结论我们建议在所有治疗性HIV-1疫苗接种试验中分析EBV载量和长期随访淋巴瘤的风险。

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