Department of Immunology, IML and IdSSC, Hospital Clínico San Carlos, Madrid, Spain.
Department of Immunology, Ophthalmology and ENT, School of Medicine, Complutense University, Madrid, Spain.
Front Immunol. 2019 Apr 2;10:654. doi: 10.3389/fimmu.2019.00654. eCollection 2019.
The assessment of specific polysaccharide antibody production plays a pivotal role in the diagnosis of humoral primary immunodeficiencies (PID). The response to 23-valent pneumococcal vaccine (PPV) remains the gold standard for the diagnosis of polysaccharide antibodies. However, in Spain, the interpretation of pure polysaccharide 23-valent immunization is hampered by the high endemicity of pneumococcal disease and the generalization of the 13-valent adjuvant pneumococcal vaccination. Specific Typhim Vi vaccination (TV) immunoglobulin G IgG response to immunization is useful in adult PID, but there is no data regarding children. To evaluate the clinical utility of TV IgG production as a diagnostic tool to determine anti-polysaccharide antibody production deficiency in children, when the response to PPV is unclear and isolated determination of serotypes is unfeasible. We conducted a single-institution prospective observational study on 61 children with recurrent infections. Baseline specific antibodies against PPV and TV were evaluated. In 28 children (46%), the response to the production of antibodies confirmed a clinical suspicion of humoral PID, and they were therefore immunized with 23-valent pneumococcal vaccine and Typhim Vi. Both specific antibody responses were measured by ELISA (The Binding Site Group Ltd, Birmingham, UK) using previously published cut-offs. Seventy percent of the 61 children displayed baseline PPV IgG > 27 mg/L, whereas only 8% showed TV IgG > 28 U/mL ( < 0.0001). Twenty-one of 28 children (75%) achieved a 3-fold increase in post-vaccination TV IgG levels, whereas only 3% achieved a 4-fold increase in PPV IgG post vaccination, mainly due to high baseline PPV IgG titers. When we classified children according to their response to TV as responders or non-responders and compared this with the well-known clinical warning signs of the Jeffrey Modell Foundation. The proportions of children with history of pneumonia and the need for intravenous antibiotics were significantly higher in TV IgG non-responders than in TV IgG responders ( = 0.02 and = 0.01, respectively). Response to TV can be considered an ancillary diagnostic tool to determine polysaccharide antibodies in children, particularly when isolated determination of pneumococcal serotypes is not feasible. TV provides a useful asset for clinicians in the era of conjugate PPV vaccination, with clinical relevance. Further research is warranted for validation.
评估特定多糖抗体的产生在体液性原发性免疫缺陷(PID)的诊断中起着关键作用。对 23 价肺炎球菌疫苗(PPV)的反应仍然是诊断多糖抗体的金标准。然而,在西班牙,由于肺炎球菌疾病的高发流行率和 13 价佐剂肺炎球菌疫苗接种的普及,对纯多糖 23 价免疫接种的解释受到了阻碍。特定伤寒 Vi 疫苗(TV)免疫球蛋白 G(IgG)对免疫接种的反应在成人 PID 中是有用的,但针对儿童的数据尚不清楚。为了评估 TV IgG 产生作为诊断工具的临床实用性,以确定儿童对多糖抗体产生的缺陷,当对 PPV 的反应不清楚且无法单独确定血清型时。我们对 61 例复发性感染的患儿进行了单中心前瞻性观察性研究。评估了对 PPV 和 TV 的基线特异性抗体。在 28 名儿童(46%)中,对抗体产生的反应证实了对体液性 PID 的临床怀疑,因此对他们进行了 23 价肺炎球菌疫苗和伤寒 Vi 疫苗接种。使用先前发表的临界值,通过 ELISA(The Binding Site Group Ltd,Birmingham,UK)测量两种特异性抗体反应。61 例患儿中有 70%显示基线 PPV IgG >27mg/L,而仅 8%显示 TV IgG >28U/mL(<0.0001)。28 例儿童中有 21 例(75%)在接种疫苗后 TV IgG 水平增加了 3 倍,而只有 3%在接种疫苗后 PPV IgG 增加了 4 倍,这主要是由于基线 PPV IgG 滴度较高。当我们根据对 TV 的反应将儿童分为应答者和非应答者,并将其与 Jeffrey Modell 基金会的已知临床警告信号进行比较时。与 TV IgG 应答者相比,TV IgG 非应答者中患有肺炎和需要静脉内抗生素的儿童比例明显更高(=0.02 和=0.01,分别)。对 TV 的反应可被视为儿童多糖抗体的辅助诊断工具,尤其是当无法单独确定肺炎球菌血清型时。TV 在结合疫苗接种时代为临床医生提供了有用的资产,具有临床相关性。进一步的研究是必要的,以验证。
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