ISGlobal, Hospital Clínic, Universitat de Barcelona, Catalonia, Spain.
Centro de Investigação em Saúde de Manhiça, Maputo, Mozambique.
Clin Infect Dis. 2019 Aug 16;69(5):820-828. doi: 10.1093/cid/ciy934.
The effect of timing of exposure to first Plasmodium falciparum infections during early childhood on the induction of innate and adaptive cytokine responses and their contribution to the development of clinical malaria immunity is not well established.
As part of a double-blind, randomized, placebo-controlled trial in Mozambique using monthly chemoprophylaxis with sulfadoxine-pyrimethamine plus artesunate to selectively control timing of malaria exposure during infancy, peripheral blood mononuclear cells collected from participants at age 2.5, 5.5, 10.5, 15, and 24 months were stimulated ex vivo with parasite schizont and erythrocyte lysates. Cytokine messenger RNA expressed in cell pellets and proteins secreted in supernatants were quantified by reverse-transcription quantitative polymerase chain reaction and multiplex flow cytometry, respectively. Children were followed up for clinical malaria from birth until 4 years of age.
Higher proinflammatory (interleukin [IL] 1, IL-6, tumor necrosis factor) and regulatory (IL-10) cytokine concentrations during the second year of life were associated with reduced incidence of clinical malaria up to 4 years of age, adjusting by chemoprophylaxis and prior malaria exposure. Significantly lower concentrations of antigen-specific T-helper 1 (IL-2, IL-12, interferon-γ) and T-helper 2 (IL-4, IL-5) cytokines by 2 years of age were measured in children undergoing chemoprophylaxis compared to children receiving placebo (P < .03).
Selective chemoprophylaxis altering early natural exposure to malaria blood stage antigens during infancy had a significant effect on T-helper lymphocyte cytokine production >1 year later. Importantly, a balanced proinflammatory and anti-inflammatory cytokine signature, probably by innate cells, around age 2 years was associated with protective clinical immunity during childhood.
NCT00231452.
儿童早期首次感染恶性疟原虫(Plasmodium falciparum)时接触时间对先天和适应性细胞因子反应的诱导及其对临床疟疾免疫发展的影响尚不清楚。
本研究是莫桑比克一项双盲、随机、安慰剂对照试验的一部分,该试验使用磺胺多辛-乙胺嘧啶加青蒿琥酯每月进行化学预防,以选择性控制婴儿期疟疾暴露的时间,在参与者 2.5、5.5、10.5、15 和 24 个月时采集外周血单个核细胞,体外刺激疟原虫裂殖体和红细胞裂解物。通过逆转录定量聚合酶链反应和多重流式细胞术分别定量细胞沉淀中细胞因子信使 RNA 的表达和上清液中分泌的蛋白。从出生到 4 岁时对儿童进行临床疟疾随访。
在生命的第二年,促炎(白细胞介素[IL]1、IL-6、肿瘤坏死因子)和调节(IL-10)细胞因子浓度较高与 4 岁前临床疟疾发病率降低相关,通过化学预防和先前疟疾暴露进行调整。接受化学预防的儿童在 2 岁时测量到的抗原特异性辅助性 T 细胞(IL-2、IL-12、干扰素-γ)和辅助性 T 细胞 2(IL-4、IL-5)细胞因子浓度显著低于接受安慰剂的儿童(P <.03)。
选择性化学预防改变了婴儿期早期对疟疾血期抗原的自然暴露,对 1 年后的辅助性 T 淋巴细胞细胞因子产生有显著影响。重要的是,在 2 岁左右,先天细胞周围存在平衡的促炎和抗炎细胞因子特征,可能与儿童期保护性临床免疫有关。
NCT00231452。