Iwajomo Oluwadamilola H, Moons Peter, Nkhata Rose, Mzinza David, Ogunniyi Abiodun D, Williams Neil A, Heyderman Robert S, Finn Adam
School of Cellular and Molecular Medicine, University of Bristol, Bristol, United Kingdom; Malawi Liverpool Wellcome Trust Clinical Research Programme, University of Malawi College of Medicine, Blantyre, Malawi.
Department of Pediatrics, University of Malawi College of Medicine, Blantyre, Malawi.
J Infect. 2015 Jun;70(6):616-23. doi: 10.1016/j.jinf.2014.10.011. Epub 2014 Nov 1.
Despite CD4(+) count restoration and viral load suppression with antiretroviral therapy (ART), HIV-infected children remain at increased risk of life-threatening infections including invasive pneumococcal disease (IPD). We therefore investigated whether persistent susceptibility to IPD following ART is associated with incomplete recovery of B-cell function.
41 HIV-infected Malawian children commencing ART were followed-up for a 1 year period during which time blood samples were collected at 0, 3, 6 and 12 months for comprehensive immunophenotyping and pneumomococcal-specific Memory B-cell Enzyme-Linked Immunospot assays. In addition, nasopharyngeal swab samples were cultured to determine pneumococcal carriage rates.
Normalization of major lymphocyte subsets such as CD4(+) percentages was evident following 3 months of ART. The proportions of mature naïve B cells (CD19(+) CD10(-) CD27(-) CD21(hi)) and resting memory B cells (CD19(+) CD27(+) CD21(hi)) increased and apoptosis-prone mature activated B cells (CD19(+) CD21(lo) CD10(-)) decreased markedly by 12 months. However, in the context of high nasopharyngeal pneumococcal carriage rates (83%), restoration of pneumococcal protein antigen-specific B-cell memory was more delayed.
These data show that, in chronically HIV-infected children receiving ART, improvement in B-cell memory profiles and function is slower than CD4(+) T-cells. This supports early initiation of ART and informs research into optimal timing of immunization with pneumococcal vaccines.
尽管抗逆转录病毒疗法(ART)可使CD4(+)细胞计数恢复正常并抑制病毒载量,但感染HIV的儿童仍面临包括侵袭性肺炎球菌疾病(IPD)在内的危及生命感染的风险增加。因此,我们调查了ART治疗后对IPD的持续易感性是否与B细胞功能未完全恢复有关。
对41名开始接受ART治疗的马拉维HIV感染儿童进行了为期1年的随访,在此期间,分别在0、3、6和12个月采集血样,进行全面的免疫表型分析和肺炎球菌特异性记忆B细胞酶联免疫斑点试验。此外,对鼻咽拭子样本进行培养以确定肺炎球菌携带率。
ART治疗3个月后,主要淋巴细胞亚群如CD4(+)百分比明显恢复正常。到12个月时,成熟幼稚B细胞(CD19(+) CD10(-) CD27(-) CD21(hi))和静息记忆B细胞(CD19(+) CD27(+) CD21(hi))的比例增加,而易于凋亡的成熟活化B细胞(CD19(+) CD21(lo) CD10(-))明显减少。然而,在鼻咽肺炎球菌携带率较高(83%)的情况下,肺炎球菌蛋白抗原特异性B细胞记忆的恢复更为延迟。
这些数据表明,在接受ART治疗的慢性HIV感染儿童中,B细胞记忆谱和功能的改善比CD4(+) T细胞慢。这支持尽早开始ART治疗,并为肺炎球菌疫苗免疫接种的最佳时机研究提供了信息。
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