Anti‐A isohaemagglutinin titres and SARS‐CoV‐2 neutralization: implications for children and convalescent plasma selection
Daniele Focosi
Abstract
I read with interest the recent article by Li et al.1 detailing the risk for COVID-19 pneumonia and for the different ABO blood groups. After demonstrating that group O healthcare workers were less likely to become infected with SARS-CoV,2 a research group proved that anti-A blood group natural isoagglutinins inhibit SARS-CoV entry into competent cells3 and could opsonize viral particles leading to complement-mediated neutralization.4 Since SARS-CoV-2 uses the same receptor as SARS-CoV, anti-A isoagglutinins are expected to have similar effects against SARS-CoV-2, accordingly, clusters of glycosylation sites exist proximal to the receptor-binding motif of the SARS-CoV and SARS-CoV-2 S protein.5 Several recent publications from China, the USA, Turkey, Spain and Italy have shown that the odd ratio for acquiring COVID-19 is higher in blood group A than in blood group O when compared to healthy controls (Table I), while no statistically significant difference was found for groups B and AB. Most importantly, the Italian–Spanish genome-wide association study identified the rs657152 polymorphism in the ABO locus on chromosome 9q34 (and only one other polymorphism in chromosome 3p21·31) as the only susceptibility locus for respiratory failure in COVID-19,6 suggesting that, in addition to disease acquisition, ABO blood group could also affect disease severity. 25·8% (vs. 32·16%) OR 0·67 37·75% (vs. 24·9%) OR 1·21 25·7% (vs. 33·8%) OR not reported 38% (vs. 32·2%) OR not reported 32·5% (mild), 26·5 (critical) (vs. 33·2%) OR 0·97 (mild) and 0·72 (critical) 35·8% in mild, 39·2% in critical (vs. 28·4%) OR 1·4 (mild) and 1·6 (critical) 45·7% (vs. 51·2%) OR 0·8 34·2% (vs. 27·9%) OR 1·3 Not reported OR 0·65 Not reported OR 1·45 24·8% (vs 37·2%) OR 0·8 57% (vs 38%) OR 2·1 Blood group A and ABO polymorphisms (rs495828, gene promoter, and rs8176746, exon 7) predispose to COVID-19 severity via increased ACE activity7-9 and cardiovascular disorders.10, 11 In a multivariate regression analysis for predicting COVID-19 prevalence, C3 and ACE1 polymorphisms were more important confounders in the spread and outcome of COVID-19 in comparison with the A allele.12 But an alternative explanation should be considered. Enveloped viruses show ABO antigens on the virion’s surface and isoagglutinins act as neutralizing antibodies. Under this model, transmission from group O individuals and between individuals of the same group will always be maximal. High titre isoagglutinins can prevent transmission, while low-titre isoagglutinin could lead to milder disease presentations.13 COVID-19 has more severe clinical presentations and outcome in elderly and in males: intriguingly, elderly males are known to experience greater reductions in isoagglutinin titres than females.14 Studies are hence ongoing to evaluate correlations between isoagglutinin titres and outcome in blood group O and B patients. Since the phenomenon apparently does not benefit group B patients,15 I suggest that only anti-A IgG (which is more prevalent than IgM in group O patients, and occurs at titres >1:16 in about 70%), but not anti-A IgM (which is more prevalent than IgG in group B patients), could confer benefit. Apart from specificity, steric hindrance could affect receptor saturation from different antibody isotypes, making IgM less ideal for masking. Since the A1 subgroup accounts for more than 80% of group A, investigations should specifically focus on anti-A1 IgG. It is known that passively acquired maternal isoagglutinins are rare in infants after the first month of life,16 but levels of anti-A isoagglutinins are already about 25% of the adult levels at month 3 and reach 90% of the adult level at three years, peaking at age 5–10, with individuals of 80 years of age and over showing reduced levels similar to those seen in 6- to 12-month-old infants.17 So the isoagglutinin titre hypothesis does not explain why infants are generally spared by severe COVID-19. A lot of additional co-factors could also explain the association, such as cross-protection from childhood vaccinations, lack of antibody-dependent enhancement (ADE) due to missing original antigenic sin (OAS) for other betacoronaviruses,18 or stable Fc fucosylation.19 If confirmed, this hypothesis will have implications for convalescent plasma therapy, since anti-A1 IgG could confer additional benefit over anti-SARS-CoV-2 neutralizing antibodies: in fact, while preserving ABO match compatibility, it could be wiser to prefer blood group O donors for convalescent plasma (CP) in COVID-19. In the mean time, it seems wiser to titre anti-A isoagglutinins in group O CP donations (or to preserve frozen plasma aliquots for later investigation), and to preferentially choose group O units. In view of the growing worldwide trend to manufacture hyperimmune serum from CP, it should also be considered that hyperimmune serum, arising from pooled diverse ABO groups, contains a far lower anti-A isoagglutinin titre than an average O group convalescent donation. I declare that I have no conflict of interest related to this manuscript.