key: cord-0736323-dx34llps
authors: Häfner, Sophia
title: There Will be Blood
date: 2020-04-28
journal: Microbes Infect
DOI: 10.1016/j.micinf.2020.04.008
sha: c7a9b70356c8aea52c107d192bfa04d664045796
doc_id: 736323
cord_uid: dx34llps

Abstract Article highlight based on “Effects of IgG and IgM autoantibodies on non-infected erythrocytes is related to ABO blood group in Plasmodium vivax malaria and is associated with anemia" by Luiza Carvalho Mourão et al.

things about an individual, notably their susceptibility to certain infections: indeed, blood group components can serve as receptors and co-receptors for various pathogens, or get hijacked for uptake, signalling, and adhesion [1] . Noroviruses for instance, the leading cause for acute gastroenteritis, require the expression of blood group antigens on gut epithelial surfaces for successful infection [5, 6] , the hepatitis B virus seems to have a preference for blood group A [7] , the tastes of the human immunodeficiency virus (HIV) are still under debate [8] , and an extremely detailed list of pathogens and their blood type connection can be found in a review by Laura Cooling [1] . It is noteworthy that this connection exceeds often the stage of simple binding between host and pathogen: some microorganisms have learnt to stimulate antibodies against blood group antigens, in order to manipulate the immune system, while blood group antigens can function as decoy receptors, as to prevent the pathogen from accessing its target tissue [1] .

In terms of infection rates and disease severity however, the best-studied cases are naturally intra-erythrocytic pathogens, first and foremost malaria 7 . At this point, it is important to point out that, although the disease is usually associated with the parasite Plasmodium falciparum as the automatic culprit, the P. vivax variant is geographically more wide-spread and responsible for almost threequarters of malaria cases in the Americas [9, 10] . There are significant differences in regard to disease pathogenesis, elicited immune response, and life cycle of the two species. Notably, P. falciparum merozoites are mainly found in mature RBCs, while P. vivax prefers their immature precursors, reticulocytes. Fittingly, another crucial difference is the requirement of the Duffy antigen specifically for P. vivax infection [9, 11] . To date, most studies, including on ABO groups, have focused on P. falciparum, considered for a long time the more virulent of the two species, and causing most malaria cases on the African continent [9] . A recent meta-analysis by Degarege et al. concluded that non-O blood groups had a higher risk of severe P. falciparum infection, with no further differences between A, B and AB types [12] . One possible molecular mechanism seems to be the process of "rosetting", the adhesion of infected RBCs to uninfected erythrocytes, which is strongly correlated to severe malaria through complications such as microvascular congestion and the ensuing tissue damage and organ failure. Evidence points towards the blood group A trisaccharides and P. falciparum RIFIN molecules as binding partners, with more candidates on the cell surfaces and in the host serum awaiting further investigation for potential therapeutic applications [13] . A few studies also point towards a P. vivax -ABO system connection: one of them found for example that the proportion of blood group O individuals was three times higher in P. vivax compared to P. falciparum infections [14] . Érika M Braga's team addresses in this issue of Microbes & Infection not only the relation of P. vivax with ABO blood groups, confirming the increased susceptibility of group O individuals, but in addition tackles an important yet often neglected complication of malaria infection, which is anaemia [15] . Direct destruction of RBCs upon the release of parasites and perturbed erythropoiesis would be obvious explanations for anaemia, if it weren't for the fact that much more uninfected than infected RBCs are actually removed -in P. vivax infection, the ratio is of 34 [16] . Oxidative stress and lipoperoxidation, leading to 4-hydroxynonenal production, have been invoked as a potential mechanism [17] , but Braga's group speculated already in a concise review from 2014 that host immune mechanisms, and an excessive immune response might play a part in malaria associated anaemia pathogenesis, especially upon P. vivax infection, which elicits strong inflammation. The authors pointed out that complement activation is systematically increased in malaria, and an insufficient upregulation of regulatory elements could lead to autologous complement-mediated lysis. Moreover, autoantibodies can emerge from cross-reactive antigenicity between host and parasite, or molecular mimicry by the pathogen [16] . Before long, Braga's group provided experimental evidence for the presence of high levels of auto-antibodies against RBCs in P. vivax patients with severe anaemia. In addition, they showed that opsonisation with IgG antibodies from anaemic patients of healthy erythrocytes increased their phagocytosis and decreased their membrane flexibility [18] . The study in question did not address yet an additional difference between blood groups regarding the risk to develop anaemic and the involvement of auto-antibodies, as hinted soon by another investigation revealing that P. vivax infected individuals of blood type O showed lower levels of haemoglobin and haematocrit compared to type O patients [19] . Here, Mourão et al. combine all three elements, confirm previous findings, and add a layer of molecular mechanisms to the process. They demonstrate that the IgG antibody response of P. vivax patients in general is greater against type O than type A erythrocytes, and that anaemic patients in particular exhibit more IgM antibodies against type O. Furthermore, IgG antibodies from anaemic individuals also lead to a greater increase in RBC membrane rigidity, and to more phagocytosis especially of type O erythrocytes [15] . This raises a plethora of new intriguing questions: what boosts the auto-immune response specifically against blood group O RBCs, and if it is potentially triggered by P. vivax, and if there is a connection with the patient's blood type, to cite a few.

Without doubt, the overall interest in blood ties with infections is just as topical as ever. Fifteen years ago, some studies associated the ABO system with severe respiratory diseases, and found type O to be more resistant against severe acute respiratory syndrome (SARS) [20] . At the moment of writing (in confinement), a retrospective case study on 2173 patients with COVID-19 and confirmed SARS-CoV2 tests from Wuhan and Shenzen (China) is pending as a pre-print on medRxiv, pointing towards a higher risk for group A, and a lower risk for group O, for contracting COVID-19 [21] . Obviously, the information should be handled not with a pinch, but a handful of salt, in times where rumours and shaky evidence about the effectiveness of the antimalarial drug hydroxychloroquine against COVID-19 prompted people to swallow aquarium cleaner with a fatal outcome 8 . Thus, this is no reason to send out only type O family members to do all the shopping, nor hunt them down for their blood. Just in case.

Dr. Erika Martins Braga is a Full Professor of Parasitology at the Universidade Federal de Minas Gerais (UFMG), Brazil. She received her B.A. degree in biology in 1990 and her Ph.D. in parasitology from the same university in 1997. She has been the head of the Malaria Laboratory of the Parasitology Department at UFMG since 1997. Her research is focused on two distinct approaches: study of the immune response in human malaria and study of the diversity of avian malaria parasites in wild birds. She has spent the last 25 years studying the humoral and cellular immune responses among different populations in the Brazilian endemic Amazon region. Her current research interest includes the study of immunological mechanisms which determine anaemia in patients infected by Plasmodium vivax.

The ABO blood group system has been associated with severe disease in Plasmodium falciparum infections, pointing that individuals with A phenotype are at a higher risk to develop severe illness compared to type O phenotype. However, this protective effect of blood group O observed in falciparum malaria has never been demonstrated in malaria caused by Plasmodium vivax. Since immune response, life cycle and disease pathogenesis are different for both P. vivax and P. falciparum, we postulated that ABO blood groups influence clinical outcomes of Plasmodium infection in different manners. Because anaemia is one of the major complications of P. vivax infection, which is thought to arise from the destruction of both infected and non-infected red blood cells (RBCs), we decided to test in vitro mechanistic evidence in favour of higher susceptibility to healthy RBCs destruction by autoantibodies from P. vivax-infected patients from blood group O compared to patients of the blood group A.

We were very pleased when we evidenced that IgG antibodies purified from anaemic patients can increase nRBCs membrane rigidity, an effect that is most pronounced in O erythrocytes, promoting in vitro phagocytosis. We demonstrated for the first time a possible association between ABO blood groups and the potential removal of nRBCs mediated by autoantibodies in P. vivax malaria.

Although we have demonstrated that IgG has a greater effect on membrane rigidity of O nRBCs, we still do not understand how this immunoglobulin induces such effect. It is possible that the binding of antibodies to O-type erythrocytes induces a strong modification on the cell membrane, impeding cell cytoskeleton distortion and leading to a decrease in membrane deformability. Thus, further investigation should be carried out to assess this issue.

Anti-RBC IgG and IgM are increased in anaemic patients with acute vivax malaria and both antibodies can decrease the deformability of nRBCs, but only IgG can induce in vitro erythrophagocytosis. Such effects are enhanced in type O erythrocytes, suggesting that individuals from this blood group infected with P. vivax malaria may be more susceptible to develop anaemia.

"Nothing is worth more than this day. You cannot relive yesterday. Tomorrow is still beyond your reach." (Goethe)

Ask new and pertinent questions and do quality science. Never give up!

Relax with my family, preparing dinner all together.

It is a hard task to select three most important discoveries because in the last decade, scientists have made extraordinary progress to understand the different phenomena involving micro and macro perspectives, from our body to cosmos. Here are some of those important contributions:

• Editing genes: the identification of Crisp-Cas9 system. • The significant expansion of the human family tree: numerous scientific advances aiming to understand our complex origin story. • A vaccine and new treatments to fight Ebola: a hope for overcoming the Coronavirus global crisis.

As a parasitologist working with Malaria, I would like to meet Dr. Charles Louis Alphonse Laveran during his work in a military hospital in Algeria, which lead to the discovery of the malaria parasite. I would like to assist the microscopic observation of a drop of fresh blood taken from a malaria patient when, in November of 1880, he found inside the red blood cells, numerous pigment-filled moving bodies with flagella-like protrusions.

I really would like to check out a vaccine against malaria and new treatment perspectives that could be used to improve the lives of millions of people in endemic countries.

• In 2018, 228 million cases of malaria and 405 000 deaths were indexed by the Wold Health Organisation (WHO) • Plasmodium vivax causes about ¾ of malaria cases in the Americas • One of the major complications of malaria is anaemia • Several blood groups, including the ABO system, have been associated with the susceptibility to contract severe malaria

• P. vivax malaria patients were sorted into an anaemic and a non-anaemic category based on a 11g/dl haemoglobin level cut-off • Both anaemic and non-anaemic patients display a greater IgG antibody response towards non-infected O than A erythrocytes • Anaemic patients exhibited more IgM antibodies against group O then group A erythrocytes • In vitro, addition of IgG or IgM antibodies from both patient classes increased the rigidity of group A and O erythrocytes • Specifically, addition of IgG antibodies from anaemic patients led to a higher increase in rigidity of O erythrocytes compared to A erythrocytes • Opsonisation by IgG antibodies from anaemic patients only increased the in vitro phagocytosis of both A and O erythrocytes, with a greater increase for type O phagocytosis rates Insert Cartoon Nr. 48

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