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疟原虫感染中寄生虫年龄和同步状态的估计。

Estimation of parasite age and synchrony status in Plasmodium falciparum infections.

机构信息

Institute of Infection, Immunity and Inflammation, College of Medical, Veterinary and Life Sciences, University of Glasgow, Glasgow, UK.

Department of Epidemiology Noguchi Memorial Institute for Medical Research, College of Health Sciences, University of Ghana, P.O. Box LG581, Legon, Ghana.

出版信息

Sci Rep. 2020 Jul 2;10(1):10925. doi: 10.1038/s41598-020-67817-6.

Abstract

Human malaria parasites have complex but poorly understood population dynamics inside their human host. In some but not all infections, parasites progress synchronously through the 48 h lifecycle following erythrocyte invasion, such that at any one time there is a limited spread of parasites at a particular time (hours) post-invasion. Patients presenting with older parasites, and with asynchronous infections, have been reported to have higher risks of fatal outcomes, associated with higher parasite biomass and multiplication rates respectively. However, practical tools to assess synchrony and estimate parasite age post-invasion in patient samples are lacking. We have developed a novel method based on three genes differentially expressed over the parasite intra-erythrocytic lifecycle, and applied it to samples from patients with uncomplicated malaria attending two health clinics in Ghana. We found that most patients presented with synchronous infections, and with parasites within 12 h of erythrocyte invasion. Finally we investigated if clinical features such as fever and parasite density could act as predictors of parasite age and synchrony. The new method is a simple and practicable approach to study parasite dynamics in naturally-infected patients, and is a significant improvement on the subjective microscopical methods for parasite staging in vivo, aiding patient management.

摘要

人类疟原虫在其人体宿主内的种群动态十分复杂,但人们对其了解甚少。在某些但不是所有的感染中,寄生虫在被红细胞入侵后的 48 小时生命周期中同步进展,因此在任何一个时间点,在特定的(小时)入侵后,寄生虫的传播范围有限。据报道,具有较老寄生虫和不同步感染的患者具有更高的致命结局风险,分别与更高的寄生虫生物量和倍增率相关。然而,评估患者样本中同步性和估计入侵后寄生虫年龄的实用工具仍然缺乏。我们开发了一种基于寄生虫在红细胞内生命周期中差异表达的三个基因的新方法,并将其应用于在加纳两个卫生诊所就诊的患有无并发症疟疾的患者样本。我们发现大多数患者的感染是同步的,并且寄生虫在红细胞入侵后 12 小时内。最后,我们研究了发热和寄生虫密度等临床特征是否可以作为寄生虫年龄和同步性的预测因子。该新方法是一种简单可行的方法,可用于研究自然感染患者中的寄生虫动力学,并且比体内寄生虫分期的主观显微镜方法有了显著的改进,有助于患者管理。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8b9a/7331735/774a58f8341d/41598_2020_67817_Fig1_HTML.jpg

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