诺氏疟疾:人类危险因素、临床谱和病理生理学。

3区 医学 Q1 Immunology and Microbiology
Advances in Parasitology Pub Date : 2021-01-01 Epub Date: 2021-08-28 DOI:10.1016/bs.apar.2021.08.001
Nicholas M Anstey, Matthew J Grigg, Giri S Rajahram, Daniel J Cooper, Timothy William, Steven Kho, Bridget E Barber
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引用次数: 12

摘要

诺氏疟原虫在东南亚流行,是人畜共患疟疾的最常见病因。诺氏疟原虫感染的临床疾病范围从无症状感染到严重疟疾和死亡。超过90%的临床疾病发生在成年人身上,大多数生活在经历土地利用集约化变化的森林边缘地区。由于人类的无性生活周期为24小时,因此寄生虫数量可能很高,但大多数诺氏疟疾的临床病例并不伴有低寄生虫血症。在共流行地区,诺氏疟疾的中位寄生虫率低于间日疟疾和恶性疟疾,表明发热阈值较低。有症状的成年人中有6-9%发生严重疟疾。诺氏疟原虫引起的严重疟疾的表现与恶性疟疾相似,但明显没有昏迷。年龄、寄生虫病、心血管合并症和延迟诊断是严重疾病和死亡的危险因素,仅在成人中可见。血小板减少症在成人中几乎是普遍的,可能与血小板红细胞结合和清除有关。在非天然灵长类宿主的致命疾病中看到的微血管污泥和在人类致命疾病中寄生虫的微血管积聚的机制尚不清楚。在人类和其他非自然灵长类宿主中,受感染和未受感染的红细胞变形能力的显著降低与疾病严重程度有关,可能导致微血管灌注受损和器官功能障碍。内皮活化、内皮功能障碍、糖萼降解和溶血也与严重疾病和器官功能障碍有关,并可能导致严重疾病和器官功能障碍,特别是急性肾损伤。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Knowlesi malaria: Human risk factors, clinical spectrum, and pathophysiology.

Plasmodium knowlesi is endemic across Southeast Asia, and is the commonest cause of zoonotic malaria. The spectrum of clinical disease from P. knowlesi infection ranges from asymptomatic infection, through to severe malaria and death. Over 90% of clinical disease occurs in adults, mostly living in forest edge areas undergoing intensive land use change. With a 24-h asexual life cycle in humans, high parasite counts are possible, but most clinical cases of knowlesi malaria are uncomplicated with low parasitaemia. In co-endemic areas, median parasitaemia in knowlesi malaria is lower than that seen in vivax and falciparum malaria, suggesting a lower fever threshold. Severe malaria occurs in 6-9% of symptomatic adults. Manifestations of severe malaria from P. knowlesi are similar to those seen with falciparum malaria, with the notable absence of coma. Age, parasitaemia, cardiovascular comorbidities and delayed diagnosis are risk factors for severe disease and death, which are only seen in adults. Thrombocytopenia is near-universal in adults, likely related to platelet-red cell binding and clearance. Mechanisms underlying the microvascular sludging seen in fatal disease in non-natural primate hosts and the microvascular accumulation of parasites in fatal human disease are not clear. Marked reductions in deformability of both infected and uninfected red blood cells are associated with disease severity in both humans and other non-natural primate hosts, likely contributing to impaired microvascular perfusion and organ dysfunction. Endothelial activation, endothelial dysfunction, glycocalyx degradation and haemolysis are also associated with, and likely contribute to, severe disease and organ dysfunction, particularly acute kidney injury.

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来源期刊
Advances in Parasitology
Advances in Parasitology 医学-寄生虫学
CiteScore
9.00
自引率
0.00%
发文量
28
审稿时长
>12 weeks
期刊介绍: Advances in Parasitology is recognised as a leading review serial which is consistently well placed in terms of impact factor and citations. Major reviews on all aspects of medical, veterinary and wild-life parasitology are considered. The journal provides an outlet for authoritative reviews from experts in the field. While emphasis is given to modern molecular approaches contributions across all disciplines are encouraged including traditional areas such as ecology and taxonomy. Eclectic volumes are supplemented by thematic volumes dedicated to a particular topic of recognised interest and importance.
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