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巴西严重非脑型恶性疟原虫疟疾与缺乏半胱氨酸残基的表达型PfEMP1 DBL1α序列的关联。

Association of severe noncerebral Plasmodium falciparum malaria in Brazil with expressed PfEMP1 DBL1 alpha sequences lacking cysteine residues.

作者信息

Kirchgatter Karin, Portillo Hernando del A

机构信息

Departmento de Parasitologia, Instituto de Ciências Biomédicas, Universidade de São Paulo, Brazil.

出版信息

Mol Med. 2002 Jan;8(1):16-23.

PMID:11984002
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2039937/
Abstract

BACKGROUND

Cytoadherence and rosetting contribute to the development of severe Plasmodium falciparum malaria. In Brazil,severe falciparum malaria is mostly associated with renal or pulmonary complications and very rarely with cerebral malaria. The most N-terminal DBL1 alpha domain of PfEMP1, a protein encoded by the var multigene family mediates rosetting. We analyzed parasites of Brazilian patients with severe malaria to determine whether there were particular DBL1 alpha var sequences predominantly expressed in such patients.

MATERIALS AND METHODS

DBL1 alpha var sequences were obtained from parasites of Brazilian patients with severe and mild malaria and were analyzed by standard bioinformatic programs. Three hundred twenty var DBL1 alpha sequences obtained from 80 Brazilian patients with mild malaria were spotted in high-density filters and hybridized to probes representing predominantly expressed sequences in parasites from patients with severe malaria. A DBL1 alpha domain was expressed in bacteria and used to demonstrate its binding capacity to erythrocytes by immunofluorescence.

RESULTS

Forty-three different and unreported DBL1 alpha amino acid sequences were obtained. Sequences predominantly expressed in patients with severe malaria could be subgrouped due to deletions of 1-2-cysteine residues. These sequences were commonly found in the var gene repertoire of parasites from patients with mild malaria, yet they were rarely expressed in these patients. A recombinant protein representing the most abundantly expressed sequence detected in one patient with severe malaria bound directly to uninfected erythrocytes.

CONCLUSIONS

This is the first report showing an association of severe noncerebral malaria from Brazil with particular DBL1 alpha sequences.

摘要

背景

细胞粘附和红细胞凝聚有助于恶性疟原虫严重疟疾的发展。在巴西,严重恶性疟疾主要与肾脏或肺部并发症相关,很少与脑型疟疾相关。由var多基因家族编码的蛋白质PfEMP1的最N端DBL1α结构域介导红细胞凝聚。我们分析了巴西重症疟疾患者的疟原虫,以确定在这些患者中是否有特定的DBL1α var序列主要表达。

材料与方法

从巴西重症和轻症疟疾患者的疟原虫中获得DBL1α var序列,并通过标准生物信息学程序进行分析。将从80例巴西轻症疟疾患者中获得的320个var DBL1α序列点样于高密度滤膜上,并与代表重症疟疾患者疟原虫中主要表达序列的探针杂交。在细菌中表达一个DBL1α结构域,并通过免疫荧光证明其与红细胞的结合能力。

结果

获得了43种不同的、未报道的DBL1α氨基酸序列。由于1-2个半胱氨酸残基的缺失,在重症疟疾患者中主要表达的序列可分为亚组。这些序列在轻症疟疾患者疟原虫的var基因库中常见,但在这些患者中很少表达。代表在一名重症疟疾患者中检测到的最丰富表达序列的重组蛋白直接与未感染的红细胞结合。

结论

这是第一份显示巴西严重非脑型疟疾与特定DBL1α序列相关的报告。