Hegewald Jana, Gantin Richard G, Lechner Christian J, Huang Xiangsheng, Agosssou Abram, Agbeko Yvon F, Soboslay Peter T, Köhler Carsten
Institute for Tropical Medicine, University Clinics Tübingen, Wilhelmstraße 27, 72074 Tübingen, Germany ; Institut National d'Hygiène - Onchocerciasis Reference Laboratory, Sokodé, Togo.
Institut National d'Hygiène - Onchocerciasis Reference Laboratory, Sokodé, Togo.
J Inflamm (Lond). 2015 Jan 20;12:5. doi: 10.1186/s12950-015-0050-y. eCollection 2015.
In sub-Saharan Africa poly-parasite infections are frequently observed in children, and with poly-parasitism modulating immune mechanisms, mediated by cytokines and chemokines, are required to prevent overwhelming inflammation and host tissue damage. We analyzed in children co-infected with helminthes and protozoan parasites their cellular production of regulatory and pro-inflammatory cytokines and chemokines in response to parasite antigens and allergens.
Intestinal and intravascular parasite infections were detected in stool and urines samples. The in vitro cellular cytokine and chemokine responses of peripheral blood mononuclear cells (PBMC) to parasite antigens and allergens were analysed in children (n = 87) with single and poly-parasite infection, and skin prick test reactivity to fungus and mite allergens was determined in singly and poly-parasitized children (n = 509).
In children Entamoeba histolytica/dispar (62%), Necator americanus (31%), Schistosoma haematobium (28%), S. mansoni (21%), Hymenolepis nana (2%) and Strongyloides stercoralis (1%) were diagnosed. Singly infected were 37%, 47% were positive for 2 or more parasite species and 16% were infection-free. When PBMC were stimulated in vitro with parasite antigens and allergens, regulatory-type cytokine IL-27 and alarmin-type IL-33 enhanced with poly-parasite infections whilst IL-10 and pro-inflammatory MIP3-α/CCL20 and MIG/CXCL9 were produced in similar amounts in singly or poly-parasitized children. The co-stimulation in vitro of PBMC with mite allergens and Ascaris lumbricoides antigens depressed the allergen-induced pro-inflammatory IL-27, IL-33 and MIP3-α/CCL20 responses while regulatory IL-10 remained unaffected. Post albendazole and/or praziquantel treatment, the cellular release of IL-10, IL-33, MIP3-α/CCL20 and MIG/CXCL9 lessened significantly in all children infection groups. Skin prick test (SPT) reactivity to fungus Aspergillus fumigatus and mite Dermatophagoides pteronyssinus allergens was investigated in 509 children, and positive SPT responses were found in 23% of the infection-free, and in 47%, 53% and 56% of the singly, doubly and poly-parasite infected, respectively.
In children co-infected with helminthes and protozoan parasites a mixed cellular response profile of both inflammatory and regulatory chemokines and cytokines was stimulated by individual antigens and allergens, pro-inflammatory cytokines and chemokines enhanced with an increasing number of parasite infections, and in poly-parasitized children skin prick test reactivity to allergens extracts was highest.
在撒哈拉以南非洲地区,儿童中经常观察到多寄生虫感染,并且多寄生虫感染会调节免疫机制,由细胞因子和趋化因子介导,以防止过度炎症和宿主组织损伤。我们分析了同时感染蠕虫和原生动物寄生虫的儿童对寄生虫抗原和过敏原的调节性和促炎性细胞因子及趋化因子的细胞产生情况。
在粪便和尿液样本中检测肠道和血管内寄生虫感染。分析了单寄生虫感染和多寄生虫感染儿童(n = 87)外周血单核细胞(PBMC)对寄生虫抗原和过敏原的体外细胞因子和趋化因子反应,并测定了单寄生虫感染和多寄生虫感染儿童(n = 509)对真菌和螨虫过敏原的皮肤点刺试验反应性。
在儿童中诊断出溶组织内阿米巴/非致病性阿米巴(62%)、美洲板口线虫(31%)、埃及血吸虫(28%)、曼氏血吸虫(21%)、微小膜壳绦虫(2%)和粪类圆线虫(1%)。单感染的占37%,47%的儿童感染2种或更多寄生虫种类呈阳性,16%未感染。当用寄生虫抗原和过敏原体外刺激PBMC时,调节性细胞因子IL-27和警报素型IL-33在多寄生虫感染时增强,而IL-10以及促炎性MIP3-α/CCL20和MIG/CXCL9在单寄生虫感染或多寄生虫感染儿童中的产生量相似。PBMC与螨虫过敏原和蛔虫抗原的体外共刺激抑制了过敏原诱导的促炎性IL-27、IL-33和MIP3-α/CCL20反应,而调节性IL-10不受影响。在使用阿苯达唑和/或吡喹酮治疗后,所有儿童感染组中IL-10、IL-33、MIP3-α/CCL20和MIG/CXCL9的细胞释放显著减少。在509名儿童中研究了对烟曲霉和粉尘螨过敏原的皮肤点刺试验(SPT)反应性,未感染儿童中有23%的SPT反应呈阳性,单寄生虫感染、双寄生虫感染和多寄生虫感染儿童中的阳性率分别为47%、53%和56%。
在同时感染蠕虫和原生动物寄生虫的儿童中,个体抗原和过敏原刺激了炎性和调节性趋化因子及细胞因子的混合细胞反应谱,促炎性细胞因子和趋化因子随着寄生虫感染数量的增加而增强,并且在多寄生虫感染儿童中对过敏原提取物的皮肤点刺试验反应性最高。
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