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Natural Regulatory T Cells in Malaria: Host or Parasite Allies?

机译:疟疾中的天然调节性T细胞:宿主还是寄生虫盟友?

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摘要

Plasmodium falciparum malaria causes 500 million clinical cases with approximately one million deaths each year. After many years of exposure, individuals living in endemic areas develop a form of clinical immunity to disease known as premunition, which is characterised by low parasite burdens rather than sterilising immunity. The reason why malaria parasites persist under a state of premunition is unknown but it has been suggested that suppression of protective immunity might be a mechanism leading to parasite persistence. Although acquired immunity limits the clinical impact of infection and provides protection against parasite replication, experimental evidence indicates that cell-mediated immune responses also result in detrimental inflammation and contribute to the aetiology of severe disease. Thus, an appropriate regulatory balance between protective immune responses and immune-mediated pathology is required for a favourable outcome of infection. As natural regulatory T (Treg) cells are identified as an immunosuppressive lineage able to modulate the magnitude of effector responses, several studies have investigated whether this cell population plays a role in balancing protective immunity and pathogenesis during malaria. The main findings to date are summarised in this review and the implication for the induction of pathogenesis and immunity to malaria is discussed.
机译:恶性疟原虫疟疾导致5亿例临床病例,每年约有100万人死亡。经过多年的暴露后,生活在流行地区的人们发展出一种对疾病的临床免疫形式,即免疫,其特征是寄生虫负担低而不是对免疫力进行杀菌。疟疾寄生虫在免疫状态下持续存在的原因尚不清楚,但有人提出抑制保护性免疫可能是导致寄生虫持续存在的机制。尽管获得性免疫限制了感染的临床影响并提供了针对寄生虫复制的保护,但实验证据表明,细胞介导的免疫反应也可导致有害的炎症,并有助于严重疾病的病因。因此,为了获得良好的感染效果,需要在保护性免疫应答和免疫介导的病理之间进行适当的调节。由于天然调节性T(Treg)细胞被鉴定为能够调节效应反应强度的免疫抑制谱系,因此多项研究研究了该细胞群是否在疟疾期间平衡保护性免疫和发病机理中发挥作用。该综述总结了迄今为止的主要发现,并讨论了其诱导发病机理和对疟疾免疫的意义。

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