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恶性疟原虫转录在疟疾的不同临床特征与感染红细胞的循环时间相关联。

Plasmodium falciparum transcription in different clinical presentations of malaria associates with circulation time of infected erythrocytes.

机构信息

Centre of Infectious Diseases, Parasitology, Heidelberg University Hospital, Heidelberg, Germany.

Max Planck Institute for Infection Biology, Berlin, Germany.

出版信息

Nat Commun. 2021 Jul 30;12(1):4711. doi: 10.1038/s41467-021-25062-z.

Abstract

Following Plasmodium falciparum infection, individuals can remain asymptomatic, present with mild fever in uncomplicated malaria cases, or show one or more severe malaria symptoms. Several studies have investigated associations between parasite transcription and clinical severity, but no broad conclusions have yet been drawn. Here, we apply a series of bioinformatic approaches based on P. falciparum's tightly regulated transcriptional pattern during its ~48-hour intraerythrocytic developmental cycle (IDC) to publicly available transcriptomes of parasites obtained from malaria cases of differing clinical severity across multiple studies. Our analysis shows that within each IDC, the circulation time of infected erythrocytes without sequestering to endothelial cells decreases with increasing parasitaemia or disease severity. Accordingly, we find that the size of circulating infected erythrocytes is inversely related to parasite density and disease severity. We propose that enhanced adhesiveness of infected erythrocytes leads to a rapid increase in parasite burden, promoting higher parasitaemia and increased disease severity.

摘要

在感染疟原虫后,个体可能无症状,在无并发症的疟疾病例中出现轻度发热,或表现出一种或多种严重疟疾症状。已有几项研究调查了寄生虫转录与临床严重程度之间的关联,但尚未得出广泛的结论。在这里,我们应用了一系列基于疟原虫在其约 48 小时的红细胞内发育周期(IDC)期间严格调控的转录模式的生物信息学方法,对来自多个研究中不同临床严重程度疟疾病例的寄生虫的公开转录组进行分析。我们的分析表明,在每个 IDC 内,未与内皮细胞隔离的感染红细胞的循环时间随着寄生虫血症或疾病严重程度的增加而减少。因此,我们发现循环感染红细胞的大小与寄生虫密度和疾病严重程度呈反比。我们提出,感染红细胞的黏附性增强会导致寄生虫负担的迅速增加,从而导致更高的寄生虫血症和更严重的疾病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f381/8324851/1514ef6068b2/41467_2021_25062_Fig1_HTML.jpg

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