Introduction

WASJ

World Academy of Sciences Journal

2632-2900 2632-2919

D.A. Spandidos

WASJ-7-1-00294

10.3892/wasj.2024.294

Articles

Assessment of COVID‑19 vaccines in building immunity response through the measurement of anti‑spike protein antibodies

Najih

Mouad

1 Boussettine

Rihabe

1 2 El Kehel

Mohamed Salem Sid'ahmed

1 El Ansari

Fatima Zahra

3 Tadlaoui

Kaoutar Anouar

1 Ennaji

Moulay Mustapha

1Research Team of Virology, Oncology and Biotechnologies, Laboratory of Virology, Oncology, Biosciences, Environment and New Energies, Faculty of Sciences and Techniques Mohammedia, University Hassan II of Casablanca, Mohammedia 28806, Morocco 2Team of Health Sciences, Education and Management 2SEM, Laboratory of Health Care Sustainable Development 2S2D, Higher Institute of Nursing and Health Technology Professions, Casablanca 20250, Morocco 3Analyses Laboratory, Anoual, Casablanca 20100, Morocco

Correspondence to: Professor Moulay Mustapha Ennaji, Research Team of Virology, Oncology and Biotechnologies, Laboratory of Virology, Oncology, Biosciences, Environment and New Energies, Faculty of Sciences and Techniques Mohammedia, University Hassan II of Casablanca, P.O. Box 146, Quartier Yasmina, Mohammedia 28806, Morocco m.ennaji@yahoo.fr

Jan-Feb 2025

13 11 2024

7 1

08 05 2024 23 10 2024

2024

This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, reproduction and adaptation in any medium and for any purpose provided that it is properly attributed. For attribution, the original author(s), title, publication source (PeerJ) and either DOI or URL of the article must be cited.

The ongoing COVID-19 crisis, caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has led to illness and loss of life. The primary strategy to change the course of the pandemic is, through vaccination, against SARS-CoV-2. The present cross-sectional study aimed to assess the effectiveness of Sinopharm and AstraZeneca COVID-19 vaccines through an assessment of anti-spike protein antibodies. The rate of antibody response was measured by detecting anti-spike and neutralizing antibodies against SARS-CoV-2 after administering two doses of the vaccines. These antibodies are pivotal indicators of the immune response elicited by vaccines, providing crucial insight into their protective efficacy. The objective was to evaluate the response of the host to the vaccine and determine the necessity of booster doses by examining the longevity and variability of antibody responses post-vaccination. To achieve this, serum and plasma samples were collected from 197 patients that tested positive for SARS-CoV-2, and anti-spike protein antibody levels were measured at 1 month after receiving the second doses of either of the aforementioned vaccines. The samples were analyzed using the Elecsys anti-SARS-CoV-2 S assay on the cobas e411 analyzer, a quantitative test that detects antibodies to the SARS-CoV-2 spike protein receptor binding domain, with results of ≥0.8 U/ml considered positive. The results revealed that 92% of the participants tested positive for anti-spike proteins, with the AstraZeneca vaccine demonstrating a better response (95.45%; 42 out of 44) compared with the Sinopharm vaccine (89,54%; 137 out of 153), exhibiting positive results for anti-spike antibodies (>0.8 U/ml).

COVID-19 severe acute respiratory syndrome coronavirus 2 vaccines anti-spike protein antibodies

Funding: No funding was received.

Introduction

Since the COVID-19 pandemic began in 2019 due to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), nations have faced major challenges. COVID-19 infection typically begins with flu-like symptoms, and can be asymptomatic or progress from mild to severe (1,2). The infection is characterized by marked inflammation. Studies have shown an association between blood count parameters and COVID-19 infection, with the neutrophil/lymphocyte ratio (3) and platelet/lymphocyte ratio linked to infection (4).

Despite extensive research into diagnosis, treatment and vaccines (5), it remains difficult to fight the virus effectively. The number of rapid and accurate tests is not sufficient, case identification is not always effective, and the human defense mechanism against the virus is still not fully understood. However, scientists have rapidly developed multiple vaccines (5). The origins of vaccination trace back to the late 18th century with development of the smallpox vaccine by Edward Jenner (6). Jenner's groundbreaking research utilized the cowpox virus to confer immunity against smallpox, marking the inaugural successful endeavor in immunization against a targeted disease (6). Since then, progress in vaccine development has continued to evolve. Advancements, such as attenuated viral strains adapted for in vitro growth have facilitated the creation of vaccines for diseases, such as polio, measles, rubella, mumps and varicella (7). Vaccine development has employed several approaches which include the following: i) Assortment which involves mixing RNA segments from different viruses to create vaccines for influenza and rotavirus; ii) inactivation, which involves the use of heat or chemicals to prepare vaccines that contain non-infectious viruses or bacteria; iii) protein-based, which involves utilizing purified proteins as antigens to trigger an immune response; iv) genetic engineering, which involves inserting genes encoding protective antigens into viral or bacterial carriers, innovating vaccine development. During the COVID-19 pandemic, various vaccines with varying approaches have been developed, such as: i) mRNA vaccines, which include BNT162b2 (Pfizer) and mRNA-1273 (Moderna); these vaccines use mRNA to make cells produce a specific protein found in COVID-19, triggering an immune response (8). ii) Viral vector vaccines, which include vaccines, such as AZD1222 (Oxford/AstraZeneca) which use harmless viruses known as adenoviruses as carriers to carry a specific piece of DNA into cells (9). This DNA contains instructions for creating proteins associated with COVID-19, which stimulates the immune system. Inactivated vaccines, including CoronaVac by Sinovac and Covaxin by Bharat Biotech, employ inactivated forms of COVID-19(10). Additionally, certain vaccines, such as NVX-CoV2373 by Novavax use specific protein subunits derived from COVID-19(11). Each vaccine employs a distinct approach to bolster immunity against the virus. However, all of these vaccines focus on the COVID-19 spike protein (12). This protein facilitates viral entry into host cells by binding to angiotensin-converting enzyme 2. Antibodies that specifically target the spike protein have exhibited effective antiviral activity and are associated with potential immunity (13).

Since the introduction of the initial COVID-19 vaccine, ~4.9 billion individuals worldwide have received vaccination. In Morocco, the vaccination campaign commenced on January 29, 2021, initially utilizing the AstraZeneca and Sinopharm vaccines only. Subsequently, Janssen by Johnson & Johnson and Pfizer-BioNTech vaccines were administered. However, Moderna vaccine uptake has been limited. Presently, ~23.5 million individuals in Morocco are fully vaccinated, constituting 65% of the country's population (14). The original COVID-19 vaccine, sold under the name Vaxzevria, was withdrawn from the market by AstraZeneca in 2024, as it caused fatal blood clots and low platelet counts, also known as thrombosis-thrombocytopenia syndrome (15).

The Sinopharm vaccine contains inactive viral particles, while AstraZeneca uses a modified adenovirus to deliver the genetic material. The time-dynamic differences in the anti-spike antibody response between Sinopharm and AstraZeneca vaccines may depend on a number of key factors (the timing of antibody production after vaccination, term immunity, patient clinicopathological factors influencing antibody response, etc.) (16,17).

The present study aimed to examine the efficacy of two vaccines, those by Sinopharm and AstraZeneca in generating long-term immunity against SARS-CoV-2, through the evaluation of factors such as age, sex, previous COVID-19 infections and subsequent infections affecting the immune response to these vaccines. By examining these parameters, the present study aimed to determine the extent to which these vaccines establish and maintain protective immunity against COVID-19.

Subjects and methods <sec> <title>Study population

The present study took place from July, 2021 to July, 2022, spanning the period from the end of the second wave to the end of the fourth wave of COVID-19 in Morocco. A total of 197 individuals between the ages of 18 and 80 years volunteered to participate in the study. In total, 44 individuals received the AstraZeneca vaccine, while 153 individuals received the Sinopharm vaccine. At 1 month after the second dose of the vaccine, blood samples were collected from the Analyses Laboratory Anoual in Casablanca, Morocco, to measure the levels of anti-spike antibodies. Individuals with pre-existing medical conditions, serious allergic reactions to vaccines, pregnant females, and those receiving cancer treatments, radiation therapy, or immune-suppressing medications were excluded from the study.

The research began in July, 2021 with preliminary work that involved the secondary analysis of anonymized data, for which formal ethics approval was not initially required. As the project evolved to include primary data collection, an ethics approval waiver was proactively obtained in March, 2022 to ensure compliance with institutional standards. Following this approval waiver, the experimental phase began by analyzing samples that had been stored in the Analyses Laboratory Anoual in Casablanca since July 2021, as well as collecting new samples. This schedule reflects the study period described in the study, capturing both the preliminary analysis of existing samples and the subsequent collection of new data. Verbal consent was obtained from participants due to several factors, including the illiteracy of some patients and the preference of other patients for oral consent rather than written documentation.

Viral RNA extraction

The Genrui 48 automated platform was used to isolate RNA from nasopharyngeal and pharyngeal swabs using the Genrui nucleic acid extraction assay (Genrui Biotech Inc.), according to the manufacturer's guidelines. The extracted RNA samples were then stored at -80˚C until analysis.

Reverse transcription-quantitative PCR (RT-qPCR)

The GeneFinder^™ COVID-19 Plus RealAmp kit (OSANG Healthcare Co., Ltd.) was used for RT-PCR according to the instructions provided with the kit (EUA-OSANG-gene-ifu, REF IFMR-45). Thus, RT-PCR was carried out in a total volume of 20 µl, containing 15 µl of the GeneFinder^™ COVID-19 Plus RealAmp master mixture (containing 10 µl of COVID-19 Plus Reaction mixture and 5 µl of COVID-19 Plus Probe mixture), and 5 µl of RNA extracted from patient samples, using the croBEE^® Real-Time PCR System (18). The reaction mixture was incubated at 50˚C for 20 min, followed by a pre-denaturation at 95˚C for 5 min, then 45 cycles of denaturation at 95˚C for 15 sec and annealing at 58˚C for 60 sec. The human housekeeping gene RNAse P was used for the internal control for normalizing gene expression. The primer sequences for the ORF1ab target and RNAse P are proprietary and confidential to OSANG Healthcare Co., Ltd., the kit's manufacturer, and therefore cannot be disclosed. The relative expression level of SARS-CoV-2 was calculated using the 2^-ΔΔCq value, based on the threshold cycle (Cq) method (19).

Measurement of antibodies

Blood samples were tested for antibodies against SARS-CoV-2 using the Elecsys anti-SARS-CoV-2 S assay (Roche Diagnostics), which runs on the Cobas e411 system from Roche Diagnostics. This test measures antibodies that bind to a specific part of the spike protein of the virus. It uses a technique known as electrochemiluminescence to detect the antibodies, and it is designed to quantify their levels. The test can detect antibody concentrations ranging from 0.40 to 250 U/ml, and it can be diluted 1:10 to measure concentrations up to 2,500 U/ml. Concentrations <0.80 U/ml are considered negative, while concentrations at or above ≥0.80 U/ml are classified as positive (20).

Statistical analysis

Statistical data were processed using IBM SPSS Statistics 28.0 software for Windows. The analysis of the association between the response to the vaccines and data from COVID-19-infected patients was performed using the Chi-squared test or Fisher's exact test (when one of the theoretical numbers was ≤5). A P-value ≤0.05 was considered to indicate a statistically significant difference.

Results

The present study included 197 participants with an average age of 52.6 years, ranging from 18 to 80 years. The age breakdown revealed that 27% of the subjects were <40 years of age, 42% were between 40 and 60 years of age, and 31% were >60 years of age. As regards the type of vaccine received, the majority (78%) received two doses of the Sinopharm vaccine, while the remaining 22% were vaccinated with the AstraZeneca vaccine (Table I).

After completing the second dose of vaccination, at the 14-day mark, the levels of antibodies against the spike protein of the virus were measured. The majority of the participants (92%) had detectable levels (>0.8 U/ml) of these antibodies (181 out of 197 subjecdts). Of these, 45% had high antibody responses (>200 U/ml), 11% had intermediate responses (>100 U/ml), 36% had low responses (<100 U/ml), and 8.1% had no detectable antibody response (Table I).

At 1 year following vaccination, 67.51% of the study subjects remained fully protected and had not been ill, 16% of the subjects had been ill within the first 6 months, and 16% of the subjects had been ill after the first 6 months (Table I).

A statistical analysis found no clear association between age, sex, or previous COVID-19 infection and the effectiveness of the AstraZeneca vaccine. However, there was a noticeable trend in the response based on age. Younger patients (<40 years of age) had a higher response rate (88%) compared to those aged 40-60 years (59.1%) and those >60 years of age (38.5%). However, these differences were not statistically significant (P=0.31; Table II).

By contrast, a notable association was detected between the response to the Sinopharm vaccine and age. A high response rate was noted in 43 and 49% of cases in the age group <40 years and in the age group between 40-60 years, respectively, compared to 31% in cases >60 years of age (P=0.018; Table III). However, no significant associations were found between the response to the Sinopharm vaccine and sex (P=0.22) or a history of COVID-19 infection (P=0.48; Table III).

When comparing the two vaccines, there was no noticeable difference in the immune response based on sex or previous COVID-19 infection. However, older individuals had a significantly improved response to both vaccines (P=0.01). Furthermore, the type of vaccine influenced the response. Those who received the AstraZeneca vaccine had a higher response rate (59.09%) compared to those who received the Sinopharm vaccine (41.17%) (P=0.02; Table IV).

Following vaccination, 67% of individuals who developed a strong response to the vaccine never contracted the virus, while 24% of the subjects were infected with COVID-19 after 6 months. Among those who developed a weak or no response to the vaccine, 69% did not contract the virus. As regards the type of vaccine, the populations vaccinated with the Sinopharm and AstraZeneca vaccines exhibited similar results in the statistical analysis. These results indicate that there is no significant difference to conclude that post-vaccination infection is directly related to the type of vaccine or the vaccine response (Table V).

Thus, although the AstraZeneca vaccine may induce a higher antibody response, this does not necessarily translate into a significant difference in terms of overall protection against post-vaccinal infection, particularly when assessing severe forms of the disease.

Discussion

The recent and devastating COVID-19 pandemic was caused by SARS-CoV-2 that emerged in Wuhan, China in 2019 and spread globally at a rapid rate, creating a major health emergency with widespread infections and deaths (21,22). International studies have been conducted to evaluate the effectiveness of vaccines (23). They compare vaccinated and unvaccinated individuals, including a placebo group, to assess the effectiveness of the vaccines in different populations. It is also important to examine the impact of the vaccine on transmission by studying how effectively it prevents infections in individuals who have not been vaccinated and how it reduces the contagiousness of vaccinated individuals who do become infected (24,25). Studies have also investigated the duration of protection provided by various COVID-19 vaccines, including the BNT162b2 mRNA (Pfizer-BioNTech) vaccine, demonstrating its high effectiveness for at least 6 months after the second dose (8,26). The Sinopharm (BBIBP-CorV) and AstraZeneca (Vaxzevria) vaccines lead to antibody production at 10-14 days after the first dose, with a peak at 1-2 weeks after the second dose. For Sinopharm, antibodies can be monitored for up to 6 months following vaccination, although their level gradually declines. As regards AstraZeneca, antibodies often remain detectable beyond 6 months, with persistence reaching 9 to 12 months (26,27).

Measuring both antibody-based (humoral) and cell-based (cellular) immune responses is crucial for evaluating the effectiveness of a vaccine. Humoral responses focus on measuring the levels of neutralizing antibodies, which block virus infectivity by preventing it from entering cells. Assessing virus-specific T-cells also provides information about vaccine effectiveness, as previously mentioned by Martin et al (28). Seroconversion studies track post-vaccination antibody development by detecting their presence in blood of vaccinated individuals (29).

The present study evaluated the effectiveness of two vaccines, Sinopharm and AstraZeneca, in protecting against SARS-CoV-2. Antibody levels in subjects who had received two doses of either vaccine were measured 14 days after the second dose. Factors such as age and sex affecting the immune response to these vaccines were examined. In addition, the impact of previous COVID-19 infection on the vaccine-induced immune response was examined. Finally, vaccine efficacy was assessed by examining the incidence of infection after vaccination. To achieve these objectives, 197 participants were enrolled in the present study; of these, 44 subjects received the AstraZeneca vaccine and 153 subjects the Sinopharm vaccine. The levels of antibodies targeting the spike protein were determined using a newly developed serological assay from Roche Diagnostics (30).

Among those vaccinated with the Sinopharm vaccine (153 subjects), 138 subjects (>90%) had antibodies against the virus. This is similar to the rate reported in the Sinopharm vaccination program (>95%). For AstraZeneca, ~98% (42 out of 44 subjects) had antibodies against the virus. This is in line with the rate reported in the Oxford University Hospitals study (>97%) (31).

The age and sex of an individual can significantly affect the administration and effectiveness of vaccines. Age-related factors include the development of the immune system, differences in exposure to disease-causing agents, and varying susceptibility to certain illnesses (29). The immune responses of infants, young children and the elderly can be influenced by age-based changes in B-cell and T-cell functionality. Indeed, sex exerts a considerable influence on shaping immune responses, given the interplay of hormonal and genetic factors that can result in variations between males and females. Females typically display more robust immune responses, characterized by higher antibody production and enhanced activation of immune cells (32-34). These differences in immune function between the sexes may contribute to variances in susceptibility to infections and responses to vaccination (35). The present study demonstrated that age plays a significant role in the effectiveness of vaccines. Among participants <60 years of age, 51% had a strong response compared to only 32% of older participants (P=0.01). The response rate also decreased gradually as the age of the subjects increased. As regards sex, there was a slight difference in the response rates between females and males. Females had a slightly higher response to the vaccines (49%) compared to males (41%). Younger subjects (<40 years of age) generally had higher immune responses to the AstraZeneca and Sinopharm vaccines. As regards the AstraZeneca vaccine, this response decreased with age (88% for those <40 years of age, 59.1% for those aged 40-60 years, and 38.5% for those >60 years of age). For the Sinopharm vaccine, the response rate was 43.14% for those <40 years of age, 49.15% for those aged 40-60 years, and 30.6% for those >60 years of age. This pattern is consistent with the findings of other studies that demonstrate that age and sex can affect vaccine responses, specifically for both the AstraZeneca and Sinopharm vaccines; these studies have demonstrated a significant decline in vaccine effectiveness with increasing age, while the effect of sex on response rates varies moderately (31,36).

Out of 118 individuals who had never previously been infected with COVID-19, 10% (i.e., 11) exhibited no immune response after the injections. By contrast, of the 79 subjects who had been previously infected with COVID-19, only 5 subjects (or <7%) did not develop an immune response. This slight difference suggests that individuals who have been previously infected with COVID-19 are more likely to develop an immune response following vaccination. This indicates that vaccination may be particularly beneficial for individuals with a history of COVID-19 infection. As in the previous study by El-Ghitany et al (37), the findings of the present study suggest that individuals who have been infected with COVID-19 prior to being vaccinated are more likely (97.8%) to test positive for anti-spike protein antibodies than those who have not been previously infected (77.3%) (data not shown). Vaccine efficacy was also examined by examining those who contracted infections even after following the two-dose vaccination schedule. Among the 197 participants, 165 (84%) did not become infected for the first 6 months after receiving the vaccine. Even after 1 year, 133 individuals (67%) were still protected against infection. This indicates that the vaccine is highly effective at preventing infections for a long period of time. During the same period as that in the present study, Boshra et al (38) conducted a similar study and found similar outcomes. They observed that after 6 months of vaccination, ~82.2% of the individuals remained unaffected by the virus. Notably, their study recorded a 73% protection rate among those who received the Sinopharm vaccine and a 91.7% protection rate among those who received the AstraZeneca vaccine. The results of the present are in accordance with previous findings, indicating the effectiveness of the Sinopharm and AstraZeneca vaccines. At 6 months following vaccination, a slightly lower, yet still substantial, protection rate of 82% (126 out of 153 subjects) was observed for the Sinopharm and 89% (39 out of 44 subjects) for the AstraZeneca vaccines. This further demonstrates the ability of both vaccines to prevent infections beyond the initial 6-month period. The present study found that the AstraZeneca vaccine consistently produced better results than the Sinopharm vaccine. This difference is likely due to the mechanisms through which the vaccines produce their effect. The AstraZeneca vaccine uses a weakened chimpanzee virus to carry genetic material into the body, which triggers the production of potent antibodies (38). The Sinopharm vaccine, on the other hand, uses a completely inactivated virus that cannot replicate in the body, which stimulates multiple immune responses (39). Moreover, differences in protection rates between the AstraZeneca and Sinopharm vaccines may reflect differences in the way these vaccines induce inflammation and, consequently, the strength and duration of the immune response. Although both vaccines are effective in producing anti-spike protein antibodies, the AstraZeneca vaccine, with its ability to produce potent antibodies, may be linked to a more rapid and stronger initial inflammatory response, leading to longer-lasting immunity than the Sinopharm vaccine, which, while effective, may exhibit a slower increase and steeper decline over time (40).

However, one of the limitations of the present cross-sectional study is the exclusion of individuals with pre-existing medical conditions, such as those undergoing cancer treatments, or those suffering from severe allergies or immunosuppression. Additionally, the levels of anti-spike protein antibodies prior to the second vaccination were not determined, which could have provided valuable insight into the baseline immunity of participants. This exclusion was necessary to preserve the integrity of the study; however, it limited the generalizability of the findings to the whole population. Future studies are thus required to include a more diverse patient population to assess the association between antibody production, longevity and various health conditions.

In addition, an extension of the present study to other vaccines is planned to assess their efficacy, allowing for a comparison of the principles and techniques of antiviral vaccine production with the corresponding response of the immune system. This comparative analysis could provide valuable insight into optimizing vaccine design and improving overall immunization strategies.

In conclusion, the present study sheds light on how the Sinopharm and AstraZeneca vaccines generate immunity against SARS-CoV-2. The majority of vaccinated individuals developed antibodies, suggesting that the vaccines effectively stimulate an immune defense. While age and sex slightly affect the immune response, younger individuals generally tend to have a stronger response. The present study thus demonstrates that individuals who have contracted COVID-19 prior to being vaccinated have a stronger immune response. This suggests that vaccination is crucial for everyone, even those already infected, as it helps to protect the population as a whole. However, further studies are warranted to determine the duration of this enhanced immune response and its efficacy against new variants of the virus.

Acknowledgements

The authors would like to thank the Ministry of Higher Education, Scientific Research and Innovation of Morocco, the Faculty of Science and Technology of Mohammedia, the University Hassan II of Casablanca, and the Analyses Laboratory Anoual in Casablanca for providing research facilities, laboratory space, access to technical equipment and expertise that significantly contributed to the success of this study.

Availability of data and materials

The datasets used and/or analyzed during the current study are available from the corresponding author on reasonable request.

Authors' contributions

MN was involved in the conception and design of the study, collected patient data, participated in the analysis and interpretation of results, and contributed to the preparation of the initial draft of the manuscript. RB contributed to the conception and design of the study and was involved in the analysis and interpretation of the results. MSSAEK participated in the analysis and interpretation of the results. FZEA was responsible for the collection of patient data, and helped prepare the initial draft of the manuscript. KAT was involved in the analysis and interpretation of the results, as well as in reviewing and editing the main text of the manuscript. MME supervised the study, ensuring its direction and integrity, and contributed to the conception and design of the study and the final editorial changes of the manuscript. MN and MME confirm the authenticity of the raw data. All authors have reviewed and approved the final version of the manuscript. All authors have participated sufficiently in the work and agreed to be accountable for all aspects of the work.

Ethics approval and consent to participate

Patient consent for publication

Not applicable.

Competition interests

The authors declare that they have no competing interests.

References 1

Aktas

A comprehensive review on rational and effective treatment strategies against an invisible enemy; SARS Cov-2 infection

Exp Biomed Res32933112020

McGoogan

Characteristics of and important lessons from the coronavirus disease 2019 (COVID-19) outbreak in China: Summary of a report of 72 314 cases from the Chinese center for disease control and prevention

JAMA323123912422020

32091533

10.1001/jama.2020.2648

Aktas

Hematological predictors of novel coronavirus infection

Rev Assoc Med Bras (1992)67 (Suppl 1)S1S22021

34259763

10.1590/1806-9282.67.Suppl1.20200678

Khalid

Ali Jaffar

Khan

Abbas Lail

Ali

Aktas

Waris

Javaid

Ijaz

Muhammad

Hematological and biochemical parameters as diagnostic and prognostic markers in SARS-COV-2 infected patients of Pakistan: A retrospective comparative analysis

Hematology265295422021

34334100

10.1080/16078454.2021.1950898

Chen

Tian

Han

Wang

Xiang

Zhang

El Arnaout

Cheng

Overview of lethal human coronaviruses

Signal Transduct Target Ther5892020

32533062

10.1038/s41392-020-0190-2

Riedel

Edward Jenner and the history of smallpox and vaccination

Proc (Bayl Univ Med Cent)1821252005

16200144

10.1080/08998280.2005.11928028

Plotkin

History of vaccination

Proc Natl Acad Sci USA11112283122872014

25136134

10.1073/pnas.1400472111

Polack

Thomas

Kitchin

Absalon

Gurtman

Lockhart

Perez

Pérez Marc

Moreira

Zerbini

Safety and efficacy of the BNT162b2 mRNA Covid-19 vaccine

N Engl J Med383260326152020

33301246

10.1056/NEJMoa2034577

Vanaparthy

Mohan

Vasireddy

Atluri

Review of COVID-19 viral vector-based vaccines and COVID-19 variants

Infez Med293283382021

35146337

10.53854/liim-2903-3

Dadras

Mehraeen

Karimi

Tantuoyir

Afzalian

Nazarian

Mojdeganlou

Mirzapour

Shamsabadi

Dashti

Safety and adverse events related to inactivated COVID-19 vaccines and novavax; a systematic review

Arch Acad Emerg Med10e542022

36033990

10.22037/aaem.v10i1.1585

Gorman

Patel

Guebre-Xabier

Zhu

Atyeo

Pullen

Loos

Goez-Gazi

Carrion

R Jr

Tian

Fab and Fc contribute to maximal protection against SARS-CoV-2 following NVX-CoV2373 subunit vaccine with Matrix-M vaccination

Cell Rep Med21004052021

34485950

10.1016/j.xcrm.2021.100405

Zhang

Mao

Gao

Bian

Wang

Liu

Song

Boosting with heterologous vaccines effectively improves protective immune responses of the inactivated SARS-CoV-2 vaccine

Emerg Microbes Infect10159816082021

34278956

10.1080/22221751.2021.1957401

Song

Zhao

Xue

Zhao

Little to no expression of angiotensin-converting enzyme-2 on most human peripheral blood immune cells but highly expressed on tissue macrophages

Cytometry A1031361452023

33280254

10.1002/cyto.a.24285

Khalis

Boucham

Luo

Marfak

Saad

Mariama Aboubacar

Ait El Haj

Jallal

Aazi

Charaka

Nejjari

COVID-19 vaccination acceptance among health science students in morocco: A cross-sectional study

Vaccines (Basel)914512021

34960197

10.3390/vaccines9121451

Maci

The (Re) creation of self-identity in times of crises: The case of AstraZeneca press-releases

Elephant Castle961102024

Anvari

Ghamar Talepoor

Eshkevar Vakili

Karimi

Ataollahi

Najafi

Kabelitz

Ahmadi

Kalantar

Comparison of the antibody responses following vaccination with AstraZeneca and Sinopharm

Iran J Immunol193213292022

36190385

10.22034/iji.2022.94298.2300

Nappi

Iervolino

Avtaar Singh

COVID-19 pathogenesis: From molecular pathway to vaccine administration

Biomedicines99032021

34440107

10.3390/biomedicines9080903

Gard

Fliss

Bosma

Ter Veen

Niesters

HGM

Validation and verification of the GeneFinder^™ COVID-19 Plus RealAmp kit on the ELITe InGenius^® instrument

J Virol Methods3001143782022

34838535

10.1016/j.jviromet.2021.114378

Livak

Schmittgen

Analysis of relative gene expression data using real-time quantitative PCR and the 2(-Delta Delta C(T)) method

Methods254024082001

11846609

10.1006/meth.2001.1262

Gilda

Sheila

Hany

Giselle

Amalia

Beatriz

Lismary

Ricardo

Yahima

Edelgis

Elevated antibody titers in Abdala vaccinees evaluated by Elecsys^® anti-SARS-CoV-2 S highly correlate with UMELISA SARS-CoV-2 ANTI RBD, ACE-2 binding inhibition and viral neutralization assays

J Biomed Biotechnol51542022

Cheng

Xue

Huang

Fang

Zeng

Lin

Liang

Investigation of antibody levels during three doses of Sinopharm/BBIBP vaccine inoculation

Front Immunol139137322022

35812449

10.3389/fimmu.2022.913732

Baden

El Sahly

Essink

Kotloff

Frey

Novak

Diemert

Spector

Rouphael

Creech

COVE study group: Efficacy and safety of the mRNA-1273 SARS-CoV-2 vaccine

N Engl J Med3844034162021

33378609

10.1056/NEJMoa2035389

Yan

Chang

Wang

Laboratory testing of SARS-CoV, MERS-CoV, and SARS-CoV-2 (2019-nCoV): Current status, challenges, and countermeasures

Rev Med Virol30e21062020

32302058

10.1002/rmv.2106

Holt

Mahmoud

Ahmed

Acuna

Al Madani

Eltantawy

Zaher

Goodier

Al Kaabi

Al Obaidli

An analysis of antibody responses and clinical sequalae of the Sinopharm HB02 COVID19 vaccine in dialysis patients in the United Arab Emirates

Nephrology (Carlton)272602682022

34569677

10.1111/nep.13980

Halloran

Longini

IM Jr

Struchiner

Design and interpretation of vaccine field studies

Epidemiol Rev2173881999

10520474

10.1093/oxfordjournals.epirev.a017990

Mubarak

Almutairi

Al-Dhabbah

Aldabas

Bhat

Alqoufail

Abdel-Maksoud

Almanaa

Farrag

Alturaiki

Durability of SARS-CoV-2 specific IgG antibody responses following two doses of match and mixed COVID-19 vaccines regimens in Saudi population

Infect Drug Resist15379138002022

35875613

10.2147/IDR.S369769

Upreti

Samant

A review on immunological responses to SARS-CoV-2 and various COVID-19 vaccine regimens

Pharm Res39211921342022

35773445

10.1007/s11095-022-03323-w

Martin

Louder

Holman

Gordon

Enama

Larkin

Andrews

Vogel

Koup

Roederer

A SARS DNA vaccine induces neutralizing antibody and cellular immune responses in healthy adults in a phase I clinical trial

Vaccine26633863432008

18824060

10.1016/j.vaccine.2008.09.026

Siegrist

Aspinall

B-cell responses to vaccination at the extremes of age

Nat Rev Immunol91851942009

19240757

10.1038/nri2508

Higgins

Fabros

Kulasingam

Quantitative measurement of anti-SARS-CoV-2 antibodies: Analytical and clinical evaluation

J Clin Microbiol59e03149202021

33483360

10.1128/JCM.03149-20

Eyre

Lumley

Wei

Cox

James

Justice

Jesuthasan

O'Donnell

Howarth

Hatch

Quantitative SARS-CoV-2 anti-spike responses to Pfizer-BioNTech and Oxford-AstraZeneca vaccines by previous infection status

Clin Microbiol Infect271516.e71516.e142021

34111577

10.1016/j.cmi.2021.05.041

Lipsitch

Kahn

Interpreting vaccine efficacy trial results for infection and transmission

Vaccine39408240882021

34130883

10.1016/j.vaccine.2021.06.011

Gustafson

Kim

Weyand

Goronzy

Influence of immune aging on vaccine responses

J Allergy Clin Immunol145130913212020

32386655

10.1016/j.jaci.2020.03.017

Bajaj

Gadi

Spihlman

Choi

Moulton

Aging, immunity, and COVID-19: How age influences the host immune response to coronavirus infections

Front Physiol115714162021

33510644

10.3389/fphys.2020.571416

Giefing-Kröll

Berger

Lepperdinger

Grubeck-Loebenstein

How sex and age affect immune responses, susceptibility to infections, and response to vaccination

Aging Cell143093212015

25720438

10.1111/acel.12326

Farid

Herrera-Uribe

Stevenson

The effect of age, gender and comorbidities upon SARS-CoV-2 spike antibody induction after two doses of sinopharm vaccine and the effect of a pfizer/BioNtech booster vaccine

Front Immunol138175972022

35711448

10.3389/fimmu.2022.817597

El-Ghitany

Hashish

Farag

Omran

Farghaly

Azzam

NFAEM

Determinants of the development of SARS-CoV-2 anti-spike immune-response after vaccination among healthcare workers in Egypt

Vaccines (Basel)101742022

35214633

10.3390/vaccines10020174

Boshra

Hussein

RRS

Mohsen

Elberry

Altyar

Tammam

Sarhan

A battle against COVID-19: Vaccine hesitancy and awareness with a comparative study between sinopharm and AstraZeneca

Vaccines (Basel)102922022

35214750

10.3390/vaccines10020292

Wang

Zhang

Huang

Deng

Quan

Wang

Zhao

Zhang

Development of an inactivated vaccine candidate, BBIBP-CorV, with potent protection against SARS-CoV-2

Cell182713721.e92020

32778225

10.1016/j.cell.2020.06.008

Letafati

Eyvazzadeh

Gharehkhani

Khorshidian

Chalabiani

Soufiani

Khakpoor

Shamsodini

Beheshti

Bavili Olyaei

Comparison of AstraZeneca and sinopharm vaccines as boosters in protection against COVID-19 infection

Biologicals821016682023

37004277

10.1016/j.biologicals.2023.101668

Table I

General clinical characteristics of the subjects included in the present study.

Parameters	AstraZeneca (n=44)	Sinopharm (n=153)	No. of subjects (%)
Age, years
<40	9	44	53(27)
40-60	22	60	82(42)
>60	13	49	62(31)
Sex
Female	22	79	101(51)
Male	22	74	96(49)
Vaccine
Sinopharm	-	-	153(78)
AstraZeneca	-	-	44(22)
Vaccine response
High response	26	63	89(45)
Average response	10	13	23(11)
Low response	7	62	69(36)
No response	1	15	16 (8.1)
History of COVID-19 infection
No	27	91	118 (59,89)
Yes	17	62	79 (40.10)
Post-vaccination infection
No	28	105	133 (67.51)
During the first 6 months	5	27	32 (16.24)
After 6 months	11	21	32 (16.24)

Table II

Association between the clinical features of subjects and the response to the AstraZeneca vaccine.

Parameter	High response (n=26) (%)	Low response (n=10) (%)	Average response (n=7) (%)	No response (n=1) (%)	P-value
Age, years
<40	8 (88.9)	1 (11.1)	0 (0)	0 (0)	0.31
40-60	13 (59.1)	4 (18.18)	5 (22.73)	0 (0)
>60	5 (38.5)	5 (38.5)	2 (15.38)	1 (7.7)
Sex
Female	12(55)	5(23)	4(18)	1(4)	0.999
Male	14(64)	5(23)	3(13)	0 (0)
History of COVID-19 infection
No	14(52)	9(33)	3(11)	1(4)	0.23
Yes	12(70)	1(6)	4(24)	0 (0)

Table III

Association between the clinical features of subjects and the response to the Sinopharm vaccine.

Parameter	High response (n=63) (%)	Average response (n=13) (%)	Low response (n=62) (%)	No response (n=15) (%)	P-value
Age, years
<40	19(43)	4(9)	12(27)	9(21)	0.018^a
40-60	29(49)	3(4)	26(44)	2(3)
>60	15(31)	6(12)	24(49)	4(8)
Sex
Female	38(48)	4(5)	31(39)	6(8)	0.22
Male	25(34)	9(12)	31(42)	9(12)
History of COVID-19 infection
No	33(36)	8(9)	40(44)	10(11)	0.48
Yes	30(48)	5(8)	22(36)	5(8)

^aIndicates a significant difference (P<0.05).

Table IV

Association between the clinical features of subjects and the response to both the AstraZeneca and Sinopharm vaccines.

Parameter	High response (n=89) (%)	Average response (n=20) (%)	Low response (n=72) (%)	No response (n=16) (%)	Total	P-value
Age, years
40-60	42(51)	8(10)	30(37)	2(2)		0.01^a
>60	20(32)	8(13)	29(47)	5(8)
<40	27(51)	4(8)	13(23)	9(18)
Sex
Female	50(49)	8(8)	36(36)	7(7)		0.52
Male	39(41)	12(13)	36(37)	9(9)
History of COVID-19 infection
No	47(40)	11(9)	49(42)	11(9)		0.21
Yes	42(53)	9(11)	23(29)	5(7)
Vaccine
Sinopharm	63(41)	13(9)	62(40)	15(10)	153	0.02^a
AstraZeneca	26(59)	7(16)	10(23)	1(2)	44

^aIndicates a significant difference (P<0.05).

Table V

Association between the clinical features of subjects and post-infection with COVID-19 following vaccination with the AstraZeneca and Sinopharm vaccines.

Parameter	No post-vaccination infection (n=133) (%)	During 6 months (n=32) (%)	After 6 months (n=32) (%)	P-value
Age, years
40-60	54(66)	13(7)	15(18)	0.84
>60	42(68)	12(19)	8(13)
<40	37(70)	7	9
Sex
Female	76(75)	15(15)	10(10)	0.027^a
Male	57(59)	17(18)	22(23)
History of COVID-19 infection
No	118(89)	0 (0)	0 (0)	<0.001^a
Yes	15(11)	32(100)	32(100)
Vaccine
Sinopharm	105(69)	27(17)	21(14)	0.16
AstraZeneca	28(64)	5(11)	11(25)
Response
High response	60(67)	8(9)	21(24)	0.034^a
Low response	50(69)	16(23)	6(8)
Average response	12(60)	4(20)	4(20)
No response	11(69)	4(25)	1(6)

^aIndicates a significant difference (P<0.05).