不要杀死寄生虫,要控制疾病。

Acta Leidensia Pub Date : 1991-01-01
J H Playfair, J Taverne, C A Bate
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引用次数: 0

摘要

从实验室和临床研究可以清楚地看出,血液期疟疾寄生虫本身并不直接引起该病的大多数严重并发症,可能贫血除外。例如,受到致命感染的T细胞被剥夺的小鼠存活时间更长,而且似乎对寄生虫病没有影响的疫苗可以保护小鼠免于过早死亡。在某些情况下,TNF抗体具有相同的效果。在临床上,50多年来人们都知道,在疟疾流行地区,儿童在寄生虫病开始下降前几年就会对疟疾的严重毒性方面产生免疫力。最近关于血期寄生虫的外抗原诱导肿瘤坏死因子(TNF)等细胞因子以及细胞因子在这种疾病和其他毒性疾病中的作用的研究表明,适当的疫苗可能诱导抗体阻断外抗原的作用,从而赋予幼儿通常需要数年才能出现的抗疾病免疫力。这种疫苗可能较少受到抗原变异的阻碍,而抗原变异使得抗寄生虫免疫的发展缓慢。表征所涉及的分子是一个高度优先。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Don't kill the parasite: control the disease.

It is clear from both laboratory and clinical studies that the blood-stage malaria parasite does not itself directly cause most of the serious complications of the disease, with the possible exception of anaemia. For example, T cell- deprived mice with lethal infections survive longer and mice can be protected against early death by vaccines that appear not to affect parasitaemia. In certain cases antibodies to TNF have the same effect. Clinically it has been known for over 50 years that children in endemic areas develop immunity to the serious toxic aspects of malaria several years before their parasitaemias start to fall. Recent work on the induction of cytokines such as tumour necrosis factor (TNF) by exoantigens of the blood-stage parasite and on the role of cytokines in this and other toxic diseases suggests that an appropriate vaccine might induce antibody that blocks the effect of the exoantigens, thus conferring on young children the anti-disease immunity that normally takes years to appear. Such vaccines might be less hampered by the antigenic variation that makes anti-parasite immunity slow to develop. Characterisation of the molecules involved is a high priority.

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