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疟疾疫苗的进展:有效诱导保护性抗疟疾免疫力。

Progress toward a malaria vaccine: efficient induction of protective anti-malaria immunity.

作者信息

Tsuji M, Rodrigues E G, Nussenzweig S

机构信息

Department of Medical and Molecular Parasitology, New York University School of Medicine, NY 10010, USA.

出版信息

Biol Chem. 2001 Apr;382(4):553-70. doi: 10.1515/BC.2001.069.

Abstract

Malaria can be a very severe disease, particularly in young children, pregnant women (mostly in primipara), and malaria naïve adults, and currently ranks among the most prevalent infections in tropical and subtropical areas throughout the world. The widespread occurrence and the increased incidence of malaria in many countries, caused by drug-resistant parasites (Plasmodium falciparum and P. vivax) and insecticide-resistant vectors (Anopheles mosquitoes), indicate the need to develop new methods of controlling this disease. Experimental vaccination with irradiated sporozoites can protect animals and humans against the disease, demonstrating the feasibility of developing an effective malaria vaccine. However, developing a universally effective, long lasting vaccine against this parasitic disease has been a difficult task, due to several problems. One difficulty stems from the complexity of the parasite's life cycle. During their life cycle, malaria parasites change their residence within the host, thus avoiding being re-exposed to the same immunological environment. These parasites also possess some distinct antigens, present at different life stages of the parasite, the so-called stage-specific antigens. While some of the stage-specific antigens can induce protective immune responses in the host, these responses are usually genetically restricted, this being another reason for delaying the development of a universally effective vaccine. The stage-specific antigens must be used as immunogens and introduced into the host by using a delivery system that should efficiently induce protective responses against the respective stages. Here we review several research approaches aimed at inducing protective anti-malaria immunity, overcoming the difficulties described above.

摘要

疟疾可能是一种非常严重的疾病,尤其在幼儿、孕妇(主要是初产妇)和初次感染疟疾的成年人中,目前它位列全球热带和亚热带地区最普遍的感染疾病之中。许多国家疟疾的广泛流行和发病率上升,是由耐药寄生虫(恶性疟原虫和间日疟原虫)和耐杀虫剂媒介(按蚊)引起的,这表明需要开发控制这种疾病的新方法。用辐照子孢子进行实验性疫苗接种可以保护动物和人类免受该疾病侵害,这证明了开发有效疟疾疫苗的可行性。然而,由于几个问题,开发一种针对这种寄生虫病的普遍有效、持久的疫苗一直是一项艰巨的任务。一个困难源于寄生虫生命周期的复杂性。在其生命周期中,疟原虫会改变在宿主体内的寄生部位,从而避免再次暴露于相同的免疫环境中。这些寄生虫还拥有一些独特的抗原,存在于寄生虫的不同生命阶段,即所谓的阶段特异性抗原。虽然一些阶段特异性抗原可以在宿主体内诱导保护性免疫反应,但这些反应通常受到基因限制,这是延迟开发普遍有效疫苗的另一个原因。阶段特异性抗原必须用作免疫原,并通过一种递送系统引入宿主体内,该系统应能有效诱导针对各个阶段的保护性反应。在此,我们综述了几种旨在诱导保护性抗疟疾免疫、克服上述困难的研究方法。

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