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威康信托基金会讲座。淋巴丝虫病中的感染与疾病:免疫学视角

The Wellcome Trust Lecture. Infection and disease in lymphatic filariasis: an immunological perspective.

作者信息

Ottesen E A

机构信息

Laboratory of Parasitic Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Md 20892.

出版信息

Parasitology. 1992;104 Suppl:S71-9. doi: 10.1017/s0031182000075259.

Abstract

The basic tenet of the immunological perspective of filarial disease is that differential immune responsiveness among individuals exposed to infection results in the different clinical manifestations that develop. The mechanisms involved in this differential responsiveness appear to reflect different T-cell cytokine response patterns. Asymptomatic patients with the clinically silent presentation of 'asymptomatic microfilaraemia', who have been previously described as being 'immunosuppressed' with respect to their generating pro-inflammatory (Th1-type) immune responses to parasite antigen, are now recognized to be fully responsive to parasite antigen but to produce cytokines and mediators that have primarily anti-inflammatory (Th2-like) effects. Studies with immunodeficient mice have indicated the existence of two alternative pathways to the development of lymphatic pathology: one dependent on the induction of inflammatory reactions by the host immune response, the other entirely independent of the immune system and reflecting the direct actions of the parasite or its products on the lymphatics. As histopathology of affected human lymphatics is consistent with this hypothesis, it may be that the lymphatic pathology seen normally in the amicrofilaraemic, highly immunoresponsive infected patients derives from inflammation induced by immune responses to parasite antigen, whereas the lymphatic pathology sometimes seen coexisting with the 'immunosuppressed' state of asymptomatic microfilaraemia actually reflects lymphatic damage that is not immunologically mediated. Though little information exists about the 'natural history' of lymphatic filariasis, there is no evidence for an inevitable progression from one clinical form to another.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

丝虫病免疫学观点的基本信条是,暴露于感染的个体之间不同的免疫反应导致了所出现的不同临床表现。这种不同反应所涉及的机制似乎反映了不同的T细胞细胞因子反应模式。以前被描述为对寄生虫抗原产生促炎(Th1型)免疫反应“免疫抑制”的无症状“无症状微丝蚴血症”临床无症状患者,现在被认为对寄生虫抗原完全有反应,但产生的细胞因子和介质主要具有抗炎(Th2样)作用。对免疫缺陷小鼠的研究表明,淋巴病理发展存在两种替代途径:一种依赖于宿主免疫反应诱导炎症反应,另一种完全独立于免疫系统,反映寄生虫或其产物对淋巴管的直接作用。由于受影响的人类淋巴管的组织病理学与这一假设一致,可能正常情况下在无微丝蚴血症、免疫反应强烈的感染患者中看到的淋巴病理来自对寄生虫抗原免疫反应诱导的炎症,而有时与无症状微丝蚴血症的“免疫抑制”状态共存的淋巴病理实际上反映的是并非由免疫介导的淋巴损伤。尽管关于淋巴丝虫病“自然史”的信息很少,但没有证据表明会不可避免地从一种临床形式发展为另一种临床形式。(摘要截短于250词)

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