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细胞因子/趋化因子网络对阿米巴病炎症免疫反应的调节

Regulation of the inflammatory immune response by the cytokine/chemokine network in amoebiasis.

作者信息

García-Zepeda E A, Rojas-López A, Esquivel-Velázquez M, Ostoa-Saloma P

机构信息

Departamento de Inmunología, Instituto de Investigaciones Biomédicas, Universidad Nacional Autónoma de México, México DF, Mexico.

出版信息

Parasite Immunol. 2007 Dec;29(12):679-84. doi: 10.1111/j.1365-3024.2007.00990.x.

Abstract

Amoebiasis is caused by the protozoa Entamoeba histolytica and persists as one of the leading parasitic diseases affecting millions worldwide. This parasite invades the intestinal mucosa, causing amoebic colitis and ulcers. It may also spread to other organs, mainly the liver, causing amoebic liver abscess (ALA). Current research efforts have focused on the development of specific diagnostic tests and animal models searching for a better understanding of the complex physiopathology of this disease. Analysis of the inflammatory immune response during intestinal amoebiasis in both human disease and animal murine models has revealed an important regulatory role for chemokines and cytokines. Recruitment and activation of inflammatory cells can also be modulated by specific protease-mediated cleavage of cytokines and by secreted amoebic factors such as amoebapores and monocyte locomotion inhibitory factor (MLIF). Unlike intestinal amoebiasis, analysis of the immune response in ALA has mainly been done in the hamster model. This has limited our information regarding the immune response during this phase of the disease. However, even with these limitations, several Th1/2 cytokines, such as IL-6 and IL-4, and regulatory cytokines, like IL-10 and TGFbeta, have been associated to the development of this disease.

摘要

阿米巴病由原生动物溶组织内阿米巴引起,仍是影响全球数百万人的主要寄生虫病之一。这种寄生虫侵入肠道黏膜,导致阿米巴性结肠炎和溃疡。它还可能扩散到其他器官,主要是肝脏,引起阿米巴肝脓肿(ALA)。目前的研究工作集中在开发特定的诊断测试和动物模型,以更好地理解这种疾病复杂的生理病理学。对人类疾病和动物小鼠模型中肠道阿米巴病期间炎症免疫反应的分析揭示了趋化因子和细胞因子的重要调节作用。炎症细胞的募集和激活也可通过细胞因子的特定蛋白酶介导的裂解以及由分泌的阿米巴因子如阿米巴穿孔素和单核细胞移动抑制因子(MLIF)来调节。与肠道阿米巴病不同,对ALA中免疫反应的分析主要在仓鼠模型中进行。这限制了我们关于疾病这一阶段免疫反应的信息。然而,即使有这些限制,几种Th1/2细胞因子,如IL-6和IL-4,以及调节性细胞因子,如IL-10和转化生长因子β,已与这种疾病的发展相关联。

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