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20 May 2022: Clinical Research  

Importance of Influenza Anti-Hemagglutinin Antibodies During the SARS-CoV-2 Pandemic in the 2019/2020 Epidemic Season in Poland

Lidia B. Brydak1ADEFG, Karol Szymański1BF, Katarzyna Kondratiuk1BF, Anna Poznańska2CDE, Adam Kolondra1B, Ewelina Hallmann1BDEF*

DOI: 10.12659/MSM.936495

Med Sci Monit 2022; 28:e936495

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Abstract

BACKGROUND: The aim of this study was to determine the level of anti-hemagglutinin antibodies in the serum of recovered patients during the SARS-CoV-2 pandemic in the 2019/2020 epidemic season in Poland, and the course of COVID-19.

MATERIAL AND METHODS: The material for the study consisted of the sera of COVID-19 convalescents obtained from the following 9 Regional Blood Donation and Blood Supply Centers located in 8 voivodeships. The hemagglutination inhibition reaction assay (HAI) using 8 viral hemagglutination units was used to determine antibody levels, in accordance with WHO recommendations.

RESULTS: This research confirms that a patient’s declared severity of the course of SARS-CoV-2 infection is influenced by the patient’s age and concomitant diseases. There was no statistically significant correlation between the level of anti-hemagglutinin antibodies and the severity of the course of a SARS-CoV-2 infection. Based on the serological tests conducted, it can be unequivocally concluded that both vaccinated and influenza-infected patients had a response rate in line with the requirements of the European Commission and the Committee for Medicinal Products for Human Use hemagglutinin antibodies for 4 influenza virus antigens tested.

CONCLUSIONS: Patients who confirmed their antibody levels with the Commission of the European Communities and the Committee for Propriety Medicinal Products (CPMP) requirements had a mild COVID-19 course. The results of our research emphasize the role of anti-hemagglutinin antibodies in the course of SARS-CoV-2 infection. COVID-19 convalescents have a higher response rate against all 4 types of anti-hemagglutinin antibodies analyzed.

Keywords: COVID-19, Influenza B virus, Influenza A virus, Antibodies, Viral, Hemagglutinins, Humans, Influenza, Human, Pandemics, Poland, SARS-CoV-2, Seasons

Background

In the 20th century, there were 3 pandemics caused by different subtypes of influenza A virus. Spanish flu, which caused 50–100 million deaths in 1918–1919, was caused by influenza virus subtype A/H1N1/. The 1918 influenza pandemic had an unusually high death rate, especially among adults, and was very widespread, affecting even Alaska. Deciphering this virus has become possible only thanks to the progress in scientific research (ie, molecular biology), as well as scientific expeditions aimed at collecting lung tissue samples of victims of this deadly influenza, which are stored frozen to the present day, as in Alaska. Professor Jeffrey Taubenberger, together with the team of the Department of Molecular Pathology of the Armed Forces Institute of Pathology in Washington, initiated research on the molecular pathology of Spanish flu virus. Then, Professor John Oxford of Barts & London Hospital and his team teamed up to continue the molecular research. Photographs of post-mortem autopsy cases included various descriptions of influenza pneumonia with acute massive alveolar bleeding, influenza pneumonia with severe acute pulmonary edema; bronchopneumonia, and influenza pneumonia with focal bronchiolitis and alveolitis [1].

The isolation of influenza virus in humans in 1933 by English researchers was the cornerstone of multidirectional research into such a highly variable pathogen, which, without exaggeration, can be called the master of metamorphosis. The next pandemic, the 1957–1958 Asian flu pandemic, was caused by the A/H2N2/subtype, but caused far fewer deaths (1–4 million). People who had survived the Spanish flu pandemic saw the value of influenza vaccination and were willing to be vaccinated. The first authorization for use of influenza vaccines in humans was given in 1941, for vaccines sponsored by the United States Armed Forces. These vaccinations had numerous adverse effects, but advances in technology and science contributed to their improvement [2]. The next 20th century flu pandemic was the 1968–1969 Hong Kong flu pandemic, which caused about 1–4 million deaths. In 1947 the World Health Organization (WHO), aware of the effects and threats of influenza infection, proposed a global program for epidemiological and virological research in the form of influenza surveillance at the 4th International Congress of Microbiology in Copenhagen [3], now referred to as the Global Influenza Surveillance and Response System. Poland has participated in it through the National Influenza Center since 1957 and has participated in virological and epidemiological SENTINEL supervision of influenza since 2004/2005 through the cooperation of 16 Voivodeship Sanitary and Epidemiological Stations [4].

The rapid spread of an infectious disease such as influenza is caused, on the one hand, by the rapid movement of people, especially today, and, on the other hand, by the existence of animal reservoirs [5]. Influenza infects people regardless of age, time of year, latitude, political views, and religious beliefs. Prior to the COVID-19 pandemic, the WHO reported that around 5–10% of adults and 20–30% of children are infected with influenza each year; there are reports of 3–5 million acute cases of the disease and about 250 000–630 000 people die due to complications triggered by influenza, including 28–111.5 thousand children under 5 years of age [6]. Currently, there are many types of influenza vaccine and next-generation anti-influenza drugs [2,7–9]. Poland had the lowest influenza vaccination rate in Europe, especially in children under 14 years of age. Influenza vaccination is the most effective and cheapest method of influenza prevention. Influenza complications should be considered not only in health-related, but also in economic terms, which the country needs to pay for using tax revenues [10,11]. Increasing preventive measures (ie, increasing Polish vaccination rates, will consequently reduce the number of post-influenza complications and deaths. Providing concrete examples should be helpful in promoting prevention and encouraging healthcare professionals to protect not only patients, but also their relatives, and to debunk numerous myths related to vaccinations. The Department of Influenza Research, National Influenza Center in NIPH NIH-NRI, in collaboration with clinicians, has published over 200 articles assessing the humoral response after influenza vaccination in high-risk groups [10–14]. In children, determination of the humoral response was performed at 6–35 months of age, 3–8 years of age, 9–12 years of age, and 13–20 years of age, with acute lymphoblastic leukemia (ALL), vaccinated at various times from the end of treatment, with severe and mild hemophilia, with bronchopulmonary dysplasia, with glomerulonephritis, with chronic renal failure, subjected to continuous ambulatory peritoneal dialysis, hemodialysis, and with chronic renal failure, vaccinated once and twice, infected with HIV – after splenectomy: vaccinated in age groups 0–5, 6–10, 11–15, 16 years of age, (doctoral dissertation) with aplastic anemia, with asthma, with inflammatory bowel disease [10]. In adult patients: aged 21–30, 31–40, 41–50, 51–64, >64 years of age, enrolled students of the Military Medical Academy, chronically ill patients, patients with acute lymphoblastic leukemia, patients with chronic renal failure (part of the habilitation thesis), HIV-infected patients with various levels of CD4, with symptomatic and asymptomatic AIDS, patients with breast cancer, patients with thyroid cancer, patients with asthma (part of the doctoral dissertation), patients with chronic obstructive pulmonary disease (COPD) (part of the doctoral dissertation), patients from the group of young people and seniors (doctoral dissertation), patients with acute cardiovascular incidents (part of the habilitation thesis), patients with non-Hodgkin malignant lymphoma (doctoral dissertation), lupus patients (doctoral dissertation), patients with primary systemic vasculitis: Wegner’s granulomatosis, an elite group of athletes vaccinated against influenza in the northern and southern hemispheres, patients with chronic diseases, healthy and sick patients undergoing hemodialysis, people over 55 years of age, vaccinated with quadrivalent influenza vaccine in the 2018/2019 epidemic season, overweight patients (doctoral dissertation) and older patients with a certain level of vitamin D (doctoral dissertation) [10,12–20]. It is noteworthy that the results of Polish studies among cardiological patients vaccinated against influenza were included in the European Cardiological Recommendations for Vaccination Against Influenza. Despite over 200 presented papers published in reputable scientific journals on the effectiveness of influenza vaccination, not only in healthy people, but also in high-risk groups, regardless of age, it is hard to admit that the percentage of vaccinated population in Poland is at an outrageously low level of 6.2% [21]. Therefore, it is not surprising that there is such a large death toll in the Polish population due to SARS-CoV-2 infection. There are no data on the number of deaths caused by influenza in Poland in the analyzed season. Furthermore, mortality caused by influenza complications in Poland is definitely underestimated. Poland has not learned any lessons from the history of influenza pandemics and the SARS-CoV-2 pandemic. The first COVID-19 cases appeared in Wuhan in December 2019, while on March 11, 2020, the epidemic was declared a pandemic by WHO. In Poland, the first disease case was recorded on March 4 in a patient who had returned from Germany. Due to the fact that COVID-19 is a new disease entity, it is very important to determine the relationship between the disease and other viral diseases, including influenza. The aim of this study was to evaluate the response rate of anti-hemagglutinin antibodies in a group of COVID convalescents from the first period of the pandemic. The following questions were raised: What was the level of the response rate and the titer of anti-hemagglutinin antibodies (also compared to peers from the national population)? Do these values depend on the patients’ sex and age? What is the role of influenza vaccination? Is there an impact of the anti-hemagglutinin antibodies detected on the subjectively perceived course of a COVID-19 infection? Both types of infections cause non-specific symptoms, such as fever above 38°C, cough, and muscle ache. Both influenza virus and SARS-CoV-2 are respiratory viruses, and the stimulation of the immune system after influenza vaccination to acquire immunity may affect the course of COVID-19 in the event of a SARS-CoV-2 infection. Therefore, it is worth checking whether there is a correlation between the presence of anti-hemagglutinin antibodies in a patient and the course of COVID-19. Due to the fact that the Department of Influenza Research, National Influenza Center, as the only center in Poland, develops influenza virus antigens for the current epidemic seasons and tests the serum levels of anti-hemagglutinin antibodies, this will be the only study of this type in Poland, resulting in broader knowledge of the novel and little-studied SARS-CoV-2 and the relationship between it and other microorganisms.

Material and Methods

STATISTICAL ANALYSIS:

A response factor (percentage of respondents) was determined for all antibodies with an appropriate titer of ≥40 (according to the criteria of the Committee for Proprietary Medicinal Products (CPMP). Note for Guidance on Harmonization for Influenza vaccine (CPMP/BWP/214/96, 12 march, 1997, 20–21) people aged 18–60) and the average level of antibodies (their geometric mean in this group of participants – GMT) [24,25]. These values were calculated (with their 95% confidence intervals – 95% CI) for the total number of respondents and in subgroups distinguished based on sex, age, and vaccination against influenza in the 2019/2020 season, as well as for comparative purposes for people aged 15–64 years from the national serological review in the 2019/2020 season. The frequency of occurrence of qualitative variables for the total number of respondents and in the selected subgroups was compared using the chi-square test. Cases with incomplete data (summarized in Table 1) were excluded from the analyses to an appropriate extent (the results are presented without them). The distributions of quantitative variables (age and antibody titers) in the 2 groups were compared using the Mann-Whitney test. A significance level of 0.05 was adopted in all statistical analyses. The analyses were performed using SPSS 12.PL statistical software.

Results

The entire study was concerned with young and middle-aged people aged 18–64 years (their average age was 38) (Table 1). Most of the participants were men (71% men vs 29% women).

Information on influenza vaccination in the 2019/2020 epidemic season was obtained in 912 cases; 266 (29.2%) patients were vaccinated and 646 (79.8%) were unvaccinated.

The level of vaccination of the respondents in individual voivodeships varied significantly (statistically significant differences, P<0.001) and ranged from 68.0% in the Śląskie Voivodeship to 2.6% in the Kujawsko-Pomorskie Voivodeship (Figure 1).

Both groups of respondents (vaccinated and unvaccinated) had a significantly higher proportion of men (77.1% and 69.1%, respectively), and the difference is statistically significant (P=0.016). These groups did not significantly differ in terms of age distribution; the mean age of vaccinated subjects was 38.0±0.6 years, the mean age of unvaccinated subjects was 37.3±0.4 years, while the median age was 38 and 36 years, respectively. It is noteworthy that people vaccinated in the 2019/2020 season were much more likely to have also been vaccinated in previous epidemic seasons – 63.3% vs 25.6% (statistically significant difference, P<0.001). Chronic diseases were reported more than twice as often in vaccinated patients – 11.7% vs 5.4% (statistically significant difference, P=0.002). In both groups, the level of each of the analyzed anti-A/H1N1/pdm09, anti-A/H3N2/, anti-B/Victoria lineage, and anti-B/Yamagata lineage antibodies ranged from 0 to 640, but the vaccinated subjects had a significantly higher response rate for each of the antibodies; the percentage of people with an antibody titer ≥40 for (P<0.001 in all cases) as well as the mean level of 3 antibodies, and the only exception was anti-B/Victoria with similar GMT in both compared groups (Table 3).

As can be seen from the data presented in Table 3, in the case of the A/Brisbane/02/2018 (H1N1)pdm09-like virus, people vaccinated significantly more often (P<0.001) had anti-A/H1N1/pdm09 antibody levels of 40 or more (56.0 [50.0–62.0]% vs 30.0 [26.5–33.6]%).

When it comes to the A/Kansas/14/2017 (H3N2) virus, vaccinated subjects significantly more often (P<0.001) had the anti-A/Kansas/114/2017/H3N2 antibody level of 40 or more (72.9 [67.6–78.3]% vs 60.4 [56.6–64.1]%).

On the other hand, in the case of the B/Colorado/06/2017 Victoria lineage virus, vaccinated persons significantly more often (P<0.001) had the anti-B/Colorado/06/2017 Victoria lineage antibody level of 40 or more (48.9 [42.9–54.9]% vs 25.4 [22.0–28.7]%).

People vaccinated against the B/Phuket/3073/2013 Yamagata lineage virus significantly more often (P<0.001) had a level of anti-B/Phuket/3073/2013-Yamagata lineage antibodies of 40 or more (77.1 [72.0–82.1]% vs 55, 4 [51.6–59.3]%).

The response rate did not depend on the sex of the subjects for the 3 types of antibodies, and only for the anti-B/Colorado/06/2017 (Victoria lineage) was it significantly higher in men than in women (34.5 [30.9–38.2]% vs 26.7 [21.4–32.0]%, P=0.021).

Influenza vaccination raises the levels of antibodies against all 4 viruses in the quadrivalent vaccine, but the levels depend on age as well as the patient’s immune memory.

In our study of people up to 40 years of age, the anti-A/Brisbane/02/2018 (H1N1)pdm09 antibody levels ≥40 were recorded in 65.1 [57.9–72.3]% of the vaccinated and 37.2 [32.4–42.1]% of unvaccinated persons (P<0.001), while at the age of 40 or more – in 39.6 [29.8–49.4]% and 19.2 [14.4–23.9]%, respectively (P<0.001) (Figure 2).

In people up to 40 years of age, the anti-A/Kansas/14/2017 (H3N2) antibodies at a level of ≥40 were recorded in 75.1 [68.6–81.7]% of the vaccinated and 59.6 [54.7–64.5]% of the unvaccinated subjects (P<0.001), while at the age of 40 or more – in 69.8 [60.6–79.0]% and 61.7 [55.8–67.6]% (the difference was not statistically significant) (Figure 3).

In people up to 40 years of age, the anti-B/Colorado/06/2017 (B/Victoria lineage) antibodies at a level ≥40 were detected in 40.8 [33.4–48.2]% of the vaccinated and 17.7 [13.9–21.5]% of the unvaccinated subjects (P<0.001), while at the age of 40 or more, in 62.5 [52.8–72.2]% of the vaccinated and 36.8 [30.9–42.6]% (P<0.001) (Figure 4).

In people under the age of 40, the anti-B/Phuket/3073/2013 (B/Yamagata lineage) antibodies at a level of ≥40 were recorded in 82.8 [77.2–88.5]% of the vaccinated and 60.9 [56.1–65.8]% of the unvaccinated (P<0.001), while at the age of 40 or more, in 66.7 [57.2–76.1]% and 47.1% [41.1–53.2], respectively (P=0.001) (Figure 5).

Among both vaccinated and unvaccinated subjects, the response rate did not show any relationship with their sex. The only exception was the anti-B/Colorado/06/2017 (Victoria lineage) antibodies among unvaccinated people – at a level of ≥40, they were found in 27.9 [23.7–32.0]% of men and 19.6 [14.1–25.1]% of women (P=0.026). This means that the sex-dependence of the response rate for this strain, shown above, comes from unvaccinated individuals. Neither influenza vaccination in the 2019/2020 season (also in previous seasons) nor the level of any of the analyzed antibodies showed a statistically significant relationship with the subjective assessment of the COVID-19 severity in convalescents. This assessment was influenced by age and its consequences (ie, the incidence of chronic diseases was 3.3% of subjects under age 40 and by 13.2% of subjects over age 40, P<0.001). Persons assessing the course of the disease as asymptomatic or mild were on average younger than those suffering more severely (median age 36 vs 39 years, P<0.001). In the first group, 6.3% declared chronic diseases, in the second it was10.1% (P<0.05). The results of the comparison of parameters of people aged 15–64 based on the serological review of the 2019/2020 epidemic season (paper prepared for publication), 3 combined age groups (15–25, 26–44, 45–64), and those of COVID-19 convalescents are presented in Table 4.

COVID-19 convalescents had a higher response rate for all the 4 analyzed antibodies; in 2 cases (type B), the differences are statistically significant: for B/Colorado/06/2017-Victoria lineage (32.3 [29.3–35.3]% vs 4.3 [2.0–6.6]%) and for B/Phuket-Yamagata lineage (61.6 [58.4–64.7]% vs 31.7 [26.4–36.9]%). The mean antibody titer (geometric mean) was higher in convalescents for 3 antigens; in 2 cases, the differences were statistically significant: for A/H1N1/pdm09 (99.7 [90.6–108.7] vs 69.0 [58.4–79.5]) and for B/Colorado/06/2017-Victoria lineage (80.7 [74.1–87.3] vs 52.2 [38.4–66.1]). For B/Phuket/3073/2013-Yamagata lineage, the antibody titers in both groups were almost equal.

Discussion

The scientific objective of this study was to assess the relationship between the presence of anti-hemagglutinin antibodies in the serum of convalescents and parameters such as: sex and age, vaccination against influenza, as well as the influence of detected anti-hemagglutinin antibodies on the subjectively perceived course of a COVID-19 infection. Anti-hemagglutinin antibodies are antibodies produced in the body following influenza vaccination or exposure to influenza virus. So far, research on the anti-hemagglutinin antibody level has been conducted in healthy and high-risk patients [10,2–20]. Due to the fact that SARS-CoV-2 is a new respiratory virus attacking humans, it is worth investigating the issue of the presence of anti-hemagglutinin antibodies in COVID-19 convalescents. SARS-CoV-2 appeared in Poland during the peak of the 2019/2020 flu epidemic season. Circulation of respiratory viruses in the population requires the use of effective diagnostic methods to confirm infections not only with influenza viruses, but also with influenza-like viruses. Apart from molecular biology methods, monitoring the level of anti-hemagglutinin antibodies in patients’ sera is also important for diagnostic purposes. When an infection is caused by influenza virus, the body produces antibodies against the virus surface glycoproteins (ie, hemagglutinin (HA) and neuraminidase [NA]). These antigens are different for type A viruses and type B viruses. Hemagglutinin is responsible for the adsorption of a viral particle to a cell receptor in the host body. This glycoprotein is capable of fusing cell membranes, thus enabling the integration of the viral envelope with the membranes of the attacked cell, which, as a result, leads to the penetration of the virion into the cytoplasm of the cell and its release within the internal structures. Haemagglutinin makes up 80% of the viral envelope proteins, is encoded by segment 4 of the genome, and takes the form of a trimer, with each monomer consisting of a spherical main domain and a stem. The host’s respiratory proteases are capable of cleaving HA into HA1 and HA2 subunits, rendering the virus infectious. The HA1 and HA2 subunits are linked to each other by disulfide bonds. The HA1 subunit is a sialic acid binding site. Proteins are found in this part. There are antigenic determinants (epitopes) against which the host’s immune system produces immunoglobulins during an infection. The HA2 subunit, on the other hand, forms a transmembrane part that anchors the protein in the viral lipid envelope and participates in fusion between the viral envelope and the endosome membrane. The hemagglutinin cleavage site is amino acid sequence-dependent and is only mediated by extracellular trypsin-like proteases in the upper respiratory tract or in the gastrointestinal tract, resulting in only a local infection. Located on the surface, the HA virus membrane is inactive (referred to as HA0). The activation of HA takes place inside the endosome, thanks to lower pH that changes the structure of the protein. X-ray studies have shown that, inside the endosome, each of the 3 HA0 polypeptide chains is cleaved into 2 fragments by host proteases present in the endosome. After the cleavage, 2 HA1 and HA2 protein fragments are formed, linked by a disulfide bridge. One of the HA2 fragments is referred to as the fusion peptide because it has the ability to bind to the endosome membrane. Under favorable conditions, the HA2 fusion fragment becomes exposed and migrates about 10 nm toward the endosome membrane. Studies have shown that acidification of the endosome and the rate of changes in the structure of hemagglutinin and the exposure of the fusion peptide are temperature-dependent and take place faster with increasing temperature. Therefore, the body’s usual response to an infection is a factor contributing to its faster elimination. The administration of an influenza vaccine produces specific influenza vaccine antibodies. The level of these antibodies is measured using the staining inhibition of hemagglutination (HAI). In this study, turkey blood or dust was used [22]. There are antibodies in the environment that bind to the shaft of the HA glycoprotein, but they are rare in humans, and there is no way of detecting them and their titer using the NI test. These immunoglobulins prevent changes in the conformation of the hemagglutinin structure caused by a change in endosome pH, which prevents the virus from attaching to the cell. The ability of anti-hemagglutinin antibodies to cross-react is important, blocking the proliferation and release from respiratory epithelial cells of a different subtype of influenza virus. For this reason, it is important to perform flu vaccinations every season, which contributes to increased immunity and thus reduces the risk of post-influenza complications. The obtained results will allow us to learn about the SARS-CoV-2 virus, which in many respects is still unknown. This type of research is also important for developing influenza vaccination recommendations with people at a higher risk in mind, such as healthcare professionals, patients with comorbidities, or the elderly, as these recommendations may reduce the mortality caused by COVID-19. In Poland, in the 2019/2020 epidemic season, only 65 deaths were recorded due to influenza complications, which is clearly an underestimation. Numerous studies by multiple authors support the role of influenza vaccination in children and people aged 65 regarding decreased spread of clinical expression of COVID-19 [26–31].

A study by Green et al showed structural similarities between influenza viruses and coronaviruses in their binding receptors and concluded that influenza vaccine could induce cross-resistance [27]. Based on the research they conducted in 2 subsequent epidemic seasons, 2018/2019 and 2019/2020, the authors indicate a relationship between earlier influenza vaccinations and reduced susceptibility to a SARS-CoV-2 infection, a milder form of COVID-19 disease. These studies were conducted using the computerized patient database of Leumit Health Services, a large health maintenance organization (HMO), from demographic data of 715 164 patients dispersed throughout the country, including medical visits, medical diagnoses, hospitalizations, and diagnostic tests. The authors also, based on their research, emphasized the importance of vaccination recommendation against influenza, especially in light of the current SARS-CoV-2 pandemic. Although Italian research by Amato et al [29] concerned the population of people aged 65 and over, influenza vaccination was shown to play a role in preventing and minimizing the spread of COVID-19 cases. Studies by Zanettini et al confirmed that COVID-19-related mortality is higher in the elderly and people with pre-existing chronic conditions [30]. It is also known that it is associated with increased morbidity and mortality in the elderly due to seasonal influenza infection; therefore, seasonal influenza vaccination is recommended for them, which was also confirmed by Polish studies [10]. Research conducted by American authors, based on analyses of various periods, suggests that influenza vaccination protects against COVID-19 mortality.

Research by Conlon et al in 27–201 people demonstrated that influenza vaccination was associated with a reduced number of positive results of COVID-19 molecular biology tests in people who were vaccinated against influenza [28]. The obtained results clearly indicate that influenza vaccinations should be recommended to reduce mortality, length of hospitalization, need for intensive care, and the use of mechanical ventilation. Patwardhan and Ohler conducted research on over 900 children who were tested positive for SARS-CoV-2 between February and August 2020 [26]. To quote the authors’ statement: “The twindemic of influenza and SARS-CoV-2 may become a public health nightmare because of the same seasonal occurrence and similarity in symptoms apart from interactions between the viruses and their host responses”, as long as we confirm the infection using molecular biology methods. The authors’ research showed that children who had a positive SARS-CoV-2 result in the analyzed influenza season had a lower chance of developing symptoms, especially breathing problems or severe disease symptoms. The authors concluded that SARS-CoV-2-positive children who were vaccinated against pneumococci were also less likely to develop the disease. For decades, children have been regarded as superspreaders, especially for respiratory viruses [9]. Unexpectedly, the correlation of the level of anti-hemagglutinin antibodies with the severity of the SARS-CoV-2 course has not been statistically confirmed. It could be associated with the age-limited group of patients, including prime-aged people (on average 38 years), analyzed in the 2019/2020 epidemic season. The study group did not include the elderly and fatal cases. Please note that this was the beginning of a pandemic, with fewer coronavirus variants occurring. Furthermore, the patients enrolled in the study subjectively assessed the severity of the disease course. Based on serological studies, it can be unequivocally concluded that both vaccinated patients and those who contracted influenza infection had a response rate of ≥40 in accordance with the requirements of the European Commission and the Committee for Medicinal Products for Human Use [24,25].

Vaccination significantly increased the response rate against all 4 types of anti-hemagglutinin antibodies analyzed (anti-A/Brisbane (H1N1)pdm09, anti-A/Kansas/14/2017 (H3N2), anti-B/Colorado/06/2017 Victoria lineage, and anti-B/Phuket/3073/2013 Yamagata lineage) as well as the level of anti-haemagglutinin antibodies in the subjects for 3 of them.

In addition, a study carried out in the Netherlands in 2020 by Debisarun et al showed that quadrivalent influenza vaccine induces a better cytokine response after stimulating immune cells with SARS-CoV-2 [31].

Conclusions

The serum level of anti-hemagglutinin antibodies in convalescents showed values greater than ≥40 the response levels as required by the Commission of the European Communities and the Committee for Propriety Medicinal Products (CPMP).

Patients who had their antibody levels confirmed with the EC and CPMP requirements had a mild COVID-19 course. There were no deaths among the studied group of patients.

Influenza vaccination helped all patients, regardless of age.

The results of our research emphasize the role of anti-hemagglutinin antibodies in the course of SARS-CoV-2 infection. It would be worth extending the study to a group of patients with a physician-confirmed, severe course of COVID-19 because, despite the proven effect of vaccination on the response rate, due to patients’ subjective assessments of the infection course, its influence on the infection severity was not statistically confirmed.

COVID-19 convalescents have a higher response rate against all 4 types of anti-hemagglutinin antibodies analyzed.

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Medical Science Monitor eISSN: 1643-3750
Medical Science Monitor eISSN: 1643-3750