Abstract
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. 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. 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. This is the first report showing an association of severe noncerebral malaria from Brazil with particular DBL1 alpha sequences.
Highlights
Plasmodium falciparum is the most virulent and devastating human malarial parasite and is responsible for approximately 300 million annual clinical cases and 1 million deaths, mostly in children under 5 years old
These 8 sequences represent 3 sequences from patient G2 and one sequence from each severe patient (G3, G23, G29, G33, and G34). These sequences were the most abundantly expressed in each patient as reflected by the large percentage (Ͼ33%) of identical clones sequences from each sample. These data demonstrate that there are P. falciparum DBL1␣ sequences lacking 1–2 cysteine residues that are predominantly expressed in parasites obtained from all patients with severe malaria included in this study
Having identified DBL1␣ var sequences lacking 1–2 cysteine residues predominantly expressed in all patients with severe malaria from the Brazilian Amazon, we examined DBL1␣ var sequences expressed in parasites obtained from patients with mild malaria
Summary
Plasmodium falciparum is the most virulent and devastating human malarial parasite and is responsible for approximately 300 million annual clinical cases and 1 million deaths, mostly in children under 5 years old. Falciparum infections are characterized by removal from the peripheral circulation of red blood cells infected with mature parasites This sequestration occurs by adhesion of infected erythrocytes to host receptors in the microvasculature of several organs. PfEMP1 plays a major role in cytoadherence and rosetting Both phenomena are directly associated with severe falciparum malaria. We analyzed parasites of Brazilian patients with severe malaria to determine whether there were particular DBL1␣ var sequences predominantly expressed in such patients. Materials and Methods: DBL1␣ 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␣ 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. Conclusion: This is the first report showing an association of severe noncerebral malaria from Brazil with particular DBL1␣ sequences
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