Last Updated: 13/02/2025

Severe malaria and microRNAs: A path towards new diagnostic and prevention tools for severe infectious pathologies

Objectives

The aim of this projects is to identify microRNAs suitable to predict pathologies associated with severe malaria (SM) or pneumonia that can be developed into diagnostic/ prognostic biomarkers.

PfEMP1s involved in the sequestration of P. falciparum during SM which constitute targets for the prevention/treatment of SM. To achieve these objectives, miRNAs in plasma of African children with different clinical phenotypes (severe and uncomplicated malaria, bacterial or viral pneumonia; n=50/group) and in postmortem tissue biopsies will be detected by massive parallel sequencing, as well as clinically relevant PfEMP1s expressed by P. falciparum field isolates (n=100).

This research will allow the development of new methods for early diagnosis of diseases such as malaria and pneumonia, as well as innovative tools to prevent the sequestration of the malaria parasite and its adverse consequences

Principal Institution

Barcelona Institute for Global Health (ISGlobal), Spain

Principal Investigators / Focal Persons

Alfredo Mayor

Rationale and Abstract

In paediatrics, and especially in developing countries where diagnostic methods are scarce, some severe infectious diseases such as pneumonia (bacterial or viral) and severe malaria (SM) are difficult to distinguish clinically because of the lack of specificity of their symptoms.

The discovery of biomarkers specific for these severe pathologies is important for the development of new methods for the early identification of critically ill patients and their adequate therapeutic management. This is, therefore, a research area with a high potential for translation to clinical practice able to place Spain in a leading scenario in the fight against diseases of global impact.

Sequestration of Plasmodium falciparum in host organs through cytoadhesion of infected erythrocytes (IEs) to host receptors is a central pathogenic event mediated by parasite proteins expressed on the surface of the IEs (P. falciparum erythrocyte membrane protein 1 [PfEMP1]). The hypothesis of this project is that host tissues damaged by the sequestration of P. falciparum secrete microRNAs (a class of small endogenous RNAs that can regulate genes post-transcriptionally) different to the ones secreted during uncomplicated malaria or pneumonia

External reference

ISGlobal - Severe malaria and microRNAs

Themes

Diagnostics
Genetics and Genomics

Date

Jan 2014 — Mar 2018

Total Project Funding

$220,684

Funding Details
Institute of Health Carlos III (ISCIII), Spain

$220,684
Project Site

Spain

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