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在高效抗逆转录病毒疗法有效治疗的第一年,严重免疫受损儿童和青少年对回忆抗原和新抗原的免疫功能受损。

Impaired immunity to recall antigens and neoantigens in severely immunocompromised children and adolescents during the first year of effective highly active antiretroviral therapy.

作者信息

Rigaud Mona, Borkowsky William, Muresan Petronella, Weinberg Adriana, Larussa Phillip, Fenton Terry, Read Jennifer S, Jean-Philippe Patrick, Fergusson Elaine, Zimmer Bonnie, Smith Dorothy, Kraimer Joyce

机构信息

New York University School of Medicine, New York, NY, USA.

出版信息

J Infect Dis. 2008 Oct 15;198(8):1123-30. doi: 10.1086/592050.

Abstract

BACKGROUND

We studied whether severely immunocompromised, human immunodeficiency virus (HIV)-infected children who were beginning highly active antiretroviral therapy (HAART) or changing HAART regimens could spontaneously respond to a recall antigen (tetanus toxoid [TT] vaccine) or respond to a recall antigen and neoantigen (hepatitis A virus [HAV] vaccine) after 3 vaccinations.

METHODS

A total of 46 children who had CD4 cell percentages <15% and who demonstrated a >0.75-log reduction in plasma HIV RNA levels within 4 weeks of starting HAART were randomized to receive vaccinations with either TT or HAV vaccines during the first 6 months of HAART. Study subjects then received the alternate vaccine during the next 6 months of HAART.

RESULTS

Despite the early decline in viremia and the later increase in the percentage of CD4 T cells, spontaneous recovery of cell-mediated immunity (CMI) was not seen for TT. Serologic responses to TT required 3 vaccinations and were comparable in both groups. Serologic responses to HAV were infrequent and of low titer, although the group that received HAV vaccine after receiving TT vaccine performed somewhat better. CMI to HAV was virtually absent.

CONCLUSIONS

Severely immunocompromised children who are receiving HAART develop CMI and antibody to a recall antigen independent of the timing of vaccination, but they require a primary series of vaccinations. Antibodies to a neoantigen, HAV, developed when vaccination was delayed after initiation of HAART. CMI to a neoantigen was difficult to establish.

TRIAL REGISTRATION

Clinicaltrials.gov identifier: NCT00004735/PACTG P1006 .

摘要

背景

我们研究了开始接受高效抗逆转录病毒治疗(HAART)或改变HAART方案的严重免疫功能低下的人类免疫缺陷病毒(HIV)感染儿童,在接种3次疫苗后是否能对回忆抗原(破伤风类毒素[TT]疫苗)产生自发反应,或对回忆抗原和新抗原(甲型肝炎病毒[HAV]疫苗)产生反应。

方法

共有46名CD4细胞百分比<15%且在开始HAART后4周内血浆HIV RNA水平降低>0.75对数的儿童被随机分为两组,在HAART的前6个月分别接受TT或HAV疫苗接种。研究对象在HAART的接下来6个月接受另一种疫苗接种。

结果

尽管病毒血症早期下降,CD4 T细胞百分比后期增加,但TT并未出现细胞介导免疫(CMI)的自发恢复。对TT的血清学反应需要接种3次疫苗,两组相当。对HAV的血清学反应很少且滴度低,尽管先接受TT疫苗后接受HAV疫苗的组表现稍好。对HAV的CMI几乎不存在。

结论

接受HAART的严重免疫功能低下儿童产生CMI和对回忆抗原的抗体与接种疫苗的时间无关,但他们需要进行一系列基础疫苗接种。在开始HAART后延迟接种疫苗时会产生针对新抗原HAV的抗体。对新抗原的CMI很难建立。

试验注册

Clinicaltrials.gov标识符:NCT00004735/PACTG P1006 。

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