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白细胞介素-12和CD40配体活性增强,但金黄色葡萄球菌Cowan 1诱导的反应减弱,提示人类血吸虫病存在全身性且逐渐受损的1型细胞因子模式。

Enhanced interleukin-12 and CD40 ligand activities but reduced Staphylococcus aureus Cowan 1-induced responses suggest a generalized and progressively impaired type 1 cytokine pattern for human schistosomiasis.

作者信息

Montenegro Silvia M L, Abath Frederico G C, Domingues Ana Lúcia C, Melo Wlademir G, Morais Clarice N L, Coutinho Eridan M, Mahanty Siddhartha, Wynn Thomas A

机构信息

Departamento de Imunologia, Centro de Pesquisas Aggeu Magalhães-FIOCRUZ. Universidade Federal de Pernambuco, Recife, Brazil.

出版信息

Infect Immun. 2002 Nov;70(11):5903-12. doi: 10.1128/IAI.70.11.5903-5912.2002.

Abstract

Whole-blood-cell cultures from schistosomiasis patients were stimulated with a variety of T-cell-dependent and T-cell-independent stimuli to determine whether the defect in type 1 cytokine expression observed following helminth infection is associated with alterations in interleukin-12 (IL-12) or CD40 ligand (CD40L) responsiveness. Cultures from uninfected individuals produced abundant gamma interferon in response to Staphylococcus aureus Cowan 1 (SAC), while patients with intestinal and hepatosplenic disease displayed intermediate and weak responses, respectively. Importantly, the decrease in type 1 cytokine expression was not attributed to defects in IL-12- or CD40L-induced activity. Indeed, schistosomiasis patients displayed heightened responses and even produced more biologically active IL-12 when stimulated with SAC and CD40L than did uninfected controls. Finally, additional studies suggested only a partial role for IL-10, since intestinal patients were the only group that overproduced this downregulatory cytokine. Together, these studies demonstrate that the type 1 deficiency in chronic hepatosplenic schistosomiasis is not related to specific defects in IL-12, IL-10, or CD40L activity, although changes in the functional status of antigen-presenting cells appear to be involved.

摘要

用多种T细胞依赖性和T细胞非依赖性刺激物刺激血吸虫病患者的全血细胞培养物,以确定蠕虫感染后观察到的1型细胞因子表达缺陷是否与白细胞介素-12(IL-12)或CD40配体(CD40L)反应性的改变有关。来自未感染个体的培养物对金黄色葡萄球菌考恩1株(SAC)产生大量γ干扰素,而患有肠道和肝脾疾病的患者分别表现出中等和微弱的反应。重要的是,1型细胞因子表达的降低并非归因于IL-12或CD40L诱导活性的缺陷。事实上,与未感染的对照组相比,血吸虫病患者在用SAC和CD40L刺激时表现出更高的反应,甚至产生更多具有生物活性的IL-12。最后,进一步的研究表明IL-10仅起部分作用,因为肠道疾病患者是唯一过度产生这种下调细胞因子的群体。总之,这些研究表明,慢性肝脾血吸虫病中的1型缺陷与IL-12、IL-10或CD40L活性的特定缺陷无关,尽管抗原呈递细胞的功能状态变化似乎也参与其中。

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