Methods to Investigate the Deformability of RBC During Malaria

Despite a 30% decline in mortality since 2000, malaria still affected 219 million subjects and caused 435,000 deaths in 2017. Red blood cells (RBC) host parasites that cause malaria, of which is the most pathogenic. The deformability of RBC is markedly modified by invasion and development of . Surfa...

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Published inFrontiers in physiology Vol. 10; p. 1613
Main Authors Depond, Mallorie, Henry, Benoit, Buffet, Pierre, Ndour, Papa Alioune
Format Journal Article
LanguageEnglish
Published Switzerland Frontiers Media S.A 21.01.2020
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Summary:Despite a 30% decline in mortality since 2000, malaria still affected 219 million subjects and caused 435,000 deaths in 2017. Red blood cells (RBC) host parasites that cause malaria, of which is the most pathogenic. The deformability of RBC is markedly modified by invasion and development of . Surface membrane area is potentially impacted by parasite entry and development, the cytoskeleton is modified by parasite proteins and cytosol viscosity is altered by parasite metabolism. RBC hosting mature parasites (second half of the asexual erythrocytic cycle) are abnormally stiff but the main reason for their absence from the circulation is their adherence to endothelial cells, mediated by parasite proteins exposed at the infected-RBC surface. By contrast, the circulation of non-adherent rings and gametocytes, depends predominantly on deformability. Altered deformability of rings and of uninfected-RBC altered by malaria infection is an important determinant of malaria pathogenesis. It also impacts the response to antimalarial therapy. Unlike conventional antimalarials that target mature stages, currently recommended first-line artemisinin derivatives and the emerging spiroindolones act on circulating rings. Methods to investigate the deformability of RBC are therefore critical to understand the clearance of infected- and uninfected-RBC in malaria. Herein, we review the main methods to assess the deformability of infected-RBC, and their contribution to the understanding of how infection causes disease, how the parasite is transmitted and how antimalarial drugs induce parasite clearance.
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Edited by: Gregory Barshtein, The Hebrew University of Jerusalem, Israel
This article was submitted to Red Blood Cell Physiology, a section of the journal Frontiers in Physiology
Reviewed by: Dmitry A. Fedosov, Jülich Research Centre, Germany; Pietro Alano, Istituto Superiore di Sanità (ISS), Italy
These authors have contributed equally to this work
ISSN:1664-042X
1664-042X
DOI:10.3389/fphys.2019.01613