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Malaria Journal
Published in: Malaria Journal 1/2019

Open Access 01-12-2019 | Plasmodium Falciparum | Research

The effects of dyslipidaemia and cholesterol modulation on erythrocyte susceptibility to malaria parasite infection

Authors: Marion Koch, Jaimini Cegla, Ben Jones, Yuning Lu, Ziad Mallat, Andrew M. Blagborough, Fiona Angrisano, Jake Baum

Published in: Malaria Journal | Issue 1/2019

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Abstract

Background

Malaria disease commences when blood-stage parasites, called merozoites, invade human erythrocytes. Whilst the process of invasion is traditionally seen as being entirely merozoite-driven, emerging data suggests erythrocyte biophysical properties markedly influence invasion. Cholesterol is a major determinant of cell membrane biophysical properties demanding its interrogation as a potential mediator of resistance to merozoite invasion of the erythrocyte.

Methods

Biophysical measurements of erythrocyte deformability by flicker spectroscopy were used to assess changes in erythrocyte bending modulus on forced integration of cholesterol and how these artificial changes affect invasion by human Plasmodium falciparum merozoites. To validate these observations in a natural context, either murine Plasmodium berghei or human Plasmodium falciparum merozoites were tested for their ability to invade erythrocytes from a hypercholesterolaemic mouse model or human clinical erythrocyte samples deriving from patients with a range of serum cholesterol concentrations, respectively.

Results

Erythrocyte bending modulus (a measure of deformability) was shown to be markedly affected by artificial modulation of cholesterol content and negatively correlated with merozoite invasion efficiency. In an in vitro infection context, however, erythrocytes taken from hypercholesterolaemic mice or from human clinical samples with varying serum cholesterol levels showed little difference in their susceptibility to merozoite invasion. Explaining this, membrane cholesterol levels in both mouse and human hypercholesterolaemia erythrocytes were subsequently found to be no different from matched normal serum controls.

Conclusions

Based on these observations, serum cholesterol does not appear to impact on erythrocyte susceptibility to merozoite entry. Indeed, no relationship between serum cholesterol and cholesterol content of the erythrocyte is apparent. This work, nonetheless, suggests that native polymorphisms which do affect membrane lipid composition would be expected to affect parasite entry. This supports investigation of erythrocyte biophysical properties in endemic settings, which may yet identify naturally protective lipid-related polymorphisms.
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Literature
1.
Chabanel A, Flamm M, Sung KL, Lee MM, Schachter D, Chien S. Influence of cholesterol content on red cell membrane viscoelasticity and fluidity. Biophys J. 1983;44:171–6.CrossRef
2.
Meleard P, Gerbeaud C, Pott T, Fernandez-Puente L, Bivas I, Mitov MD, et al. Bending elasticities of model membranes: influences of temperature and sterol content. Biophys J. 1997;72:2616–29.CrossRef
3.
Henriksen J, Rowat AC, Ipsen JH. Vesicle fluctuation analysis of the effects of sterols on membrane bending rigidity. Eur Biophys J. 2004;33:732–41.CrossRef
4.
Cazzola R, Rondanelli M, Trotti R, Cestaro B. Effects of weight loss on erythrocyte membrane composition and fluidity in overweight and moderately obese women. J Nutr Biochem. 2011;22:388–92.CrossRef
5.
Tziakas DN, Kaski JC, Chalikias GK, Romero C, Fredericks S, Tentes IK, et al. Total cholesterol content of erythrocyte membranes is increased in patients with acute coronary syndrome: a new marker of clinical instability? J Am Coll Cardiol. 2007;49:2081–9.CrossRef
6.
Martinez M, Vaya A, Marti R, Gil L, Lluch I, Carmena R, Aznar J. Erythrocyte membrane cholesterol/phospholipid changes and hemorheological modifications in familial hypercholesterolemia treated with lovastatin. Thromb Res. 1996;83:375–88.CrossRef
7.
White NJ, Pukrittayakamee S, Hien TT, Faiz MA, Mokuolu OA, Dondorp AM. Malaria. Lancet. 2014;383:723–35.CrossRef
8.
Cowman AF, Berry D, Baum J. The cellular and molecular basis for malaria parasite invasion of the human red blood cell. J Cell Biol. 2012;198:961–71.CrossRef
9.
Koch M, Baum J. The mechanics of malaria parasite invasion of the human erythrocyte—towards a reassessment of the host cell contribution. Cell Microbiol. 2016;18:319–29.CrossRef
10.
Koch M, Wright KE, Otto O, Herbig M, Salinas ND, Tolia NH, et al. Plasmodium falciparum erythrocyte-binding antigen 175 triggers a biophysical change in the red blood cell that facilitates invasion. Proc Natl Acad Sci USA. 2017;114:4225–30.CrossRef
11.
Sisquella X, Nebl T, Thompson JK, Whitehead L, Malpede BM, Salinas ND, et al. Plasmodium falciparum ligand binding to erythrocytes induce alterations in deformability essential for invasion. Elife. 2017;6:e21083.CrossRef
12.
Genton B, Al-Yaman F, Mgone CS, Alexander N, Paniu MM, Alpers MP, et al. Ovalocytosis and cerebral malaria. Nature. 1995;378:564–5.CrossRef
13.
Ndila CM, Uyoga S, Macharia AW, Nyutu G, Peshu N, Ojal J, et al. Human candidate gene polymorphisms and risk of severe malaria in children in Kilifi, Kenya: a case-control association study. Lancet Haematol. 2018;5:e333–45.CrossRef
14.
Baum J, Ward RH, Conway DJ. Natural selection on the erythrocyte surface. Mol Biol Evol. 2002;19:223–9.CrossRef
15.
Malaria Genomic Epidemiology Network, Band G, Rockett KA, Spencer CC, Kwiatkowski DP. A novel locus of resistance to severe malaria in a region of ancient balancing selection. Nature. 2015;526:253–7.CrossRef
16.
Robert V, Bourgouin C, Depoix D, Thouvenot C, Lombard MN, Grellier P. Malaria and obesity: obese mice are resistant to cerebral malaria. Malar J. 2008;7:81.CrossRef
17.
Elased K, Playfair JH. Hypoglycemia and hyperinsulinemia in rodent models of severe malaria infection. Infect Immun. 1994;62:5157–60.PubMedPubMedCentral
18.
Mancio-Silva L, Slavic K, Grilo Ruivo MT, Grosso AR, Modrzynska KK, Vera IM, et al. Nutrient sensing modulates malaria parasite virulence. Nature. 2017;547:213–6.CrossRef
19.
Chukwuocha UM, Eke KN. Malaria parasite status and cholesterol level of malaria patients in parts of the IMO River Basin of Nigeria. Asian Pac J Trop Med. 2011;4:993–6.CrossRef
20.
Wilson DW, Crabb BS, Beeson JG. Development of fluorescent Plasmodium falciparum for in vitro growth inhibition assays. Malar J. 2010;9:152.CrossRef
21.
Trager W, Jensen JB. Human malaria parasites in continuous culture. Science. 1976;193:673–5.CrossRef
22.
Boyle MJ, Wilson DW, Richards JS, Riglar DT, Tetteh KK, Conway DJ, et al. Isolation of viable Plasmodium falciparum merozoites to define erythrocyte invasion events and advance vaccine and drug development. Proc Natl Acad Sci USA. 2010;107:14378–83.CrossRef
23.
Zuccala ES, Satchwell TJ, Angrisano F, Tan YH, Wilson MC, Heesom KJ, et al. Quantitative phospho-proteomics reveals the Plasmodium merozoite triggers pre-invasion host kinase modification of the red cell cytoskeleton. Sci Rep. 2016;6:19766.CrossRef
24.
Salmon BL, Oksman A, Goldberg DE. Malaria parasite exit from the host erythrocyte: a two-step process requiring extraerythrocytic proteolysis. Proc Natl Acad Sci USA. 2001;98:271–6.CrossRef
25.
Zidovetzki R, Levitan I. Use of cyclodextrins to manipulate plasma membrane cholesterol content: evidence, misconceptions and control strategies. Biochim Biophys Acta. 2007;1768:1311–24.CrossRef
26.
Lyth O, Vizcay-Barrena G, Wright KE, Haase S, Mohring F, Najer A, et al. Cellular dissection of malaria parasite invasion of human erythrocytes using viable Plasmodium knowlesi merozoites. Sci Rep. 2018;8:10165.CrossRef
27.
Lelliott PM, Lampkin S, McMorran BJ, Foote SJ, Burgio G. A flow cytometric assay to quantify invasion of red blood cells by rodent Plasmodium parasites in vivo. Malar J. 2014;13:100.CrossRef
28.
Wilson DW, Langer C, Goodman CD, McFadden GI, Beeson JG. Defining the timing of action of antimalarial drugs against Plasmodium falciparum. Antimicrob Agents Chemother. 2013;57:1455–67.CrossRef
29.
Carter CP, Howles PN, Hui DY. Genetic variation in cholesterol absorption efficiency among inbred strains of mice. J Nutr. 1997;127:1344–8.CrossRef
30.
Zadelaar S, Kleemann R, Verschuren L, de Vries-Van der Weij J, van der Hoorn J, Princen HM, et al. Mouse models for atherosclerosis and pharmaceutical modifiers. Arterioscler Thromb Vasc Biol. 2007;27:1706–21.CrossRef
31.
Sengupta A, Ghosh M. Integrity of erythrocytes of hypercholesterolemic and normocholesterolemic rats during ingestion of different structured lipids. Eur J Nutr. 2011;50:411–9.CrossRef
32.
Dwight JF, Mendes Ribeiro AC, Hendry BM. Effects of HMG-CoA reductase inhibition on erythrocyte membrane cholesterol and acyl chain composition. Clin Chim Acta. 1996;256:53–63.CrossRef
33.
D’Alessandro A, Righetti PG, Zolla L. The red blood cell proteome and interactome: an update. J Proteome Res. 2010;9:144–63.CrossRef
34.
Quarfordt SH, Hilderman HL. Quantitation of the in vitro free cholesterol exchange of human red cells and lipoproteins. J Lipid Res. 1970;11:528–35.PubMed
35.
Gold JC, Phillips MC. Effects of membrane lipid composition on the kinetics of cholesterol exchange between lipoproteins and different species of red blood cells. Biochim Biophys Acta. 1990;1027:85–92.CrossRef
36.
Lingwood D, Binnington B, Rog T, Vattulainen I, Grzybek M, Coskun U, et al. Cholesterol modulates glycolipid conformation and receptor activity. Nat Chem Biol. 2011;7:260–2.CrossRef
37.
Davis S, Davis BM, Richens JL, Vere KA, Petrov PG, Winlove CP, et al. Alpha-Tocopherols modify the membrane dipole potential leading to modulation of ligand binding by P-glycoprotein. J Lipid Res. 2015;56:1543–50.CrossRef
Metadata
Title
The effects of dyslipidaemia and cholesterol modulation on erythrocyte susceptibility to malaria parasite infection
Authors
Marion Koch
Jaimini Cegla
Ben Jones
Yuning Lu
Ziad Mallat
Andrew M. Blagborough
Fiona Angrisano
Jake Baum
Publication date
01-12-2019
Publisher
BioMed Central
Published in
Malaria Journal / Issue 1/2019
Electronic ISSN: 1475-2875
DOI
https://doi.org/10.1186/s12936-019-3016-3

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