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间日疟原虫:临床表现、危险因素和发病机制。

Plasmodium vivax: clinical spectrum, risk factors and pathogenesis.

机构信息

Global Health Division, Menzies School of Health Research and Charles Darwin University, Darwin, Australia.

出版信息

Adv Parasitol. 2012;80:151-201. doi: 10.1016/B978-0-12-397900-1.00003-7.

Abstract

Vivax malaria was historically described as 'benign tertian malaria' because individual clinical episodes were less likely to cause severe illness than Plasmodium falciparum. Despite this, Plasmodium vivax was, and remains, responsible for major morbidity and significant mortality in vivax-endemic areas. Single infections causing febrile illness in otherwise healthy individuals rarely progress to severe disease. Nevertheless, in the presence of co-morbidities, P. vivax can cause severe illness and fatal outcomes. Recurrent or chronic infections in endemic areas can cause severe anaemia and malnutrition, particularly in early childhood. Other severe manifestations include acute lung injury, acute kidney injury and uncommonly, coma. Multiorgan failure and shock are described but further studies are needed to investigate the role of bacterial and other co-infections in these syndromes. In pregnancy, P. vivax infection can cause maternal anaemia, miscarriage, low birth weight and congenital malaria. Compared to P. falciparum, P. vivax has a greater capacity to elicit an inflammatory response, resulting in a lower pyrogenic threshold. Conversely, cytoadherence of P. vivax to endothelial cells is less frequent and parasite sequestration is not thought to be a significant cause of severe illness in vivax malaria. With a predilection for young red cells, P. vivax does not result in the high parasite biomass associated with severe disease in P. falciparum, but a four to fivefold greater removal of uninfected red cells from the circulation relative to P. falciparum is associated with a similar risk of severe anaemia. Mechanisms underlying the pathogenesis of severe vivax syndromes remain incompletely understood.

摘要

间日疟在历史上被描述为“良性间日疟”,因为个体临床发作不太可能导致比恶性疟原虫更严重的疾病。尽管如此,间日疟原虫过去和现在仍然是间日疟流行地区主要发病率和显著死亡率的原因。在没有合并症的情况下,导致发热性疾病的单一感染很少进展为严重疾病。然而,在存在合并症的情况下,间日疟原虫可能导致严重疾病和致命后果。在流行地区反复发作或慢性感染可导致严重贫血和营养不良,特别是在儿童早期。其他严重表现包括急性肺损伤、急性肾损伤,罕见情况下出现昏迷。多器官衰竭和休克已有描述,但需要进一步研究以调查细菌和其他合并感染在这些综合征中的作用。在妊娠期间,间日疟原虫感染可导致母亲贫血、流产、低出生体重和先天性疟疾。与恶性疟原虫相比,间日疟原虫更有能力引起炎症反应,导致较低的发热阈值。相反,间日疟原虫对内皮细胞的细胞黏附较少见,寄生虫隔离被认为不是间日疟严重疾病的重要原因。间日疟原虫偏爱年轻的红细胞,不会导致与恶性疟原虫严重疾病相关的高寄生虫生物量,但与恶性疟原虫相比,从循环中去除未感染的红细胞的数量增加四到五倍,与严重贫血的风险相似。严重间日疟综合征发病机制的机制仍不完全清楚。

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