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Age-Stratified Profiles of Serum IL-6 IL-10 and TNF-α Cytokines among Kenyan Children with Schistosoma haematobium Plasmodium falciparum and Other Chronic Parasitic Co-infections

机译:肯尼亚血吸虫恶性疟原虫和其他慢性寄生虫共感染儿童的血清IL-6IL-10和TNF-α细胞因子的年龄分层特征

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摘要

In a study of children having polyparasitic infections in a Schistosoma haematobium–endemic area, we examined the hypothesis that S. haematobium–positive children, compared with S. haematobium–negative children (anti-soluble worm antigen preparation [SWAP] negative and egg negative) have increased systemic production of pro-inflammatory cytokines (interleukin [IL]-6, tumor necrosis factor [TNF]-α) and decreased down-regulatory IL-10. A total of 804 children, 2–19 years of age, were surveyed between July and December 2009 and tested for S. haematobium, Plasmodium falciparum, filariasis, and soil-transmitted helminth infections. Plasma levels of IL-6, TNF-α, and IL-10 were compared for S. haematobium–positive and S. haematobium–negative children, adjusting for malaria, filaria, and hookworm co-infections, and for nutritional status, age group, sex, and geographic location. IL-10 was significantly elevated among children infected with S. haematobium, showing bimodal peaks in 7–8 and 13–14 years age groups. IL-10 was also higher among children who were acutely malnourished, whereas IL-10 levels were lower in the presence of S. haematobium–filaria co-infection. After adjustment for co-factors, IL-6 was significantly elevated among children of 5–6 years and among those with P. falciparum infection. Lower levels of IL-6 were found in malaria–hookworm co-infection. High levels of TNF-α were found in children aged 11–12 years regardless of infection status. In addition, village of residence was a strong predictor of IL-6 and IL-10 plasma levels. In adolescent children infected with S. haematobium, there is an associated elevation in circulating IL-10 that may reduce the risk of later morbidity. Although we did not find a direct link between S. haematobium infection and circulating pro-inflammatory IL-6 and TNF-α levels, future T-cell stimulation studies may provide more conclusive linkages between infection and cytokine responses in settings that are endemic for multiple parasites and multiple co-infections.
机译:在一项针对血吸虫血吸虫病流行地区多寄生虫感染儿童的研究中,我们检验了以下假设:血吸虫血吸虫阳性儿童与血吸虫血吸虫阴性儿童相比(抗可溶性蠕虫抗原制剂[SWAP]阴性和卵阴性) )可增加促炎性细胞因子(白介素[IL] -6,肿瘤坏死因子[TNF]-α)的系统生成,并降低IL-10的下调。在2009年7月至2009年12月之间,共对804名2-19岁的儿童进行了调查,并对其进行了血球链球菌,恶性疟原虫,丝虫病和土壤传播的蠕虫感染的检测。比较了血生链球菌阳性和血生链球菌阴性儿童的血浆IL-6,TNF-α和IL-10的水平,并调整了疟疾,丝虫和钩虫的合并感染,并调整了营养状况,年龄组,性别和地理位置。在感染链球菌的儿童中,IL-10显着升高,在7-8岁和13-14岁年龄组中出现双峰峰值。在急性营养不良的儿童中,IL-10含量也较高,而存在血生链球菌-丝虫病合并感染时,IL-10含量较低。调整辅助因子后,在5-6岁的儿童和恶性疟原虫感染的儿童中,IL-6明显升高。在疟疾-钩虫感染中发现较低水平的IL-6。无论感染状况如何,在11至12岁的儿童中都发现高水平的TNF-α。此外,居住村庄是IL-6和IL-10血浆水平的有力预测指标。在感染了链球菌的青春期儿童中,循环中的IL-10升高,可能会降低以后发病的风险。尽管我们并未发现血球链球菌感染与循环性促炎性IL-6和TNF-α水平之间存在直接联系,但未来的T细胞刺激研究可能会在多发性地方性流行的环境中提供感染和细胞因子反应之间的更多结论性联系。寄生虫和多种合并感染。

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