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细胞因子通过对血液阶段感染的免疫调节在增强疟疾疫苗效力方面的作用。

A role for cytokines in potentiation of malaria vaccines through immunological modulation of blood stage infection.

作者信息

Taylor-Robinson A W, Smith E C

机构信息

School of Biology, University of Leeds, UK.

出版信息

Immunol Rev. 1999 Oct;171:105-23. doi: 10.1111/j.1600-065x.1999.tb01344.x.

Abstract

Malaria is the world's major parasitic disease, for which effective control measures are urgently needed. One of the difficulties hindering successful vaccine design against Plasmodium is an incomplete knowledge of antigens eliciting protective immunity, the precise types of immune response for which to aim, and how these can be induced. A greater appreciation of the mechanisms of protective immunity, on the one hand, and of immunopathology, on the other, should provide critical clues to how manipulation of the immune system may best be achieved. We are studying the regulation of the balance between T helper 1 (Th1) and T helper 2 (Th2) CD4+ T lymphocytes in immunity to asexual blood stages of malaria responsible for the pathogenicity of the disease. Protective immunity to the experimental murine malarias Plasmodium chabaudi and Plasmodium yoelii involves both Th1 and Th2 cells, which provide protection by different mechanisms at different times of infection characterised by higher and lower parasite densities, respectively. This model therefore facilitates a clearer understanding of the Th1/Th2 equilibrium that appears central to immunoregulation of all host/pathogen relationships. It also permits a detailed dissection in vivo of the mechanisms of antimalarial immunity. Here, we discuss the present state of malaria vaccine development and our current research to understand the factors involved in the modulation of vaccine-potentiated immunity.

摘要

疟疾是世界上主要的寄生虫病,迫切需要有效的控制措施。阻碍成功设计针对疟原虫疫苗的困难之一是,对于引发保护性免疫的抗原了解不全面,不清楚应针对何种精确类型的免疫反应,以及如何诱导这些反应。一方面,更深入地了解保护性免疫机制,另一方面,了解免疫病理学,应该能为如何最好地操纵免疫系统提供关键线索。我们正在研究在针对导致疟疾致病性的无性血液阶段的免疫中,辅助性T细胞1(Th1)和辅助性T细胞2(Th2)CD4 + T淋巴细胞之间平衡的调节。对实验性鼠疟查巴迪疟原虫和约氏疟原虫的保护性免疫涉及Th1和Th2细胞,它们在感染的不同时间通过不同机制提供保护,分别以较高和较低的寄生虫密度为特征。因此,该模型有助于更清楚地理解Th1/Th2平衡,这似乎是所有宿主/病原体关系免疫调节的核心。它还允许在体内详细剖析抗疟免疫机制。在这里,我们讨论疟疾疫苗开发的现状以及我们目前为了解疫苗增强免疫调节所涉及因素而进行的研究。

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