Your search keyword '"peptide vaccines"' showing total 15 results

1. A SARS-CoV-2 recombinant spike protein vaccine (S-268019-b) for COVID-19 prevention during the Omicron-dominant period: A phase 3, randomised, placebo-controlled clinical trial.

Author

Dinh Thiem, Vu, Van Anh, Pham Thi, Van Men, Chu, Hung, Do Thai, Pollard, Andrew J., Kamitani, Akari, Tada, Yukio, Fukuyama, Hidenori, Iwasaki, Yuka, Ariyasu, Mari, and Sonoyama, Takuhiro

Subjects

*SARS-CoV-2, *PEPTIDE vaccines, *COVID-19 pandemic, *REVERSE transcriptase polymerase chain reaction, *COVID-19, *TRANSCRANIAL direct current stimulation

Abstract

• First study of ancestral recombinant vaccine, S-268019-b for prevention in Vietnam. • The vaccine efficacy for prevention not verified in Omicron-dominant period. • S-268019-b immunogenicity and tolerability confirmed. • Similar efficacy and safety of S-268019-b with other ancestral strain vaccines. Clinical trials of new vaccines based on existing variants of Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) are often impacted by the emergence of new virus variants. We evaluated the efficacy, immunogenicity, and safety of S-268019-b, a recombinant spike protein subunit vaccine based on the ancestral strain, for preventing symptomatic coronavirus disease 2019 (COVID-19) during the Omicron (BA.2)-dominant period in Vietnam. In this multicentre, phase 3, randomised (2:1), observer-blind, placebo-controlled crossover study, participants received 2 intramuscular doses (28 days apart) of either 10 µg of S-268019-b (Recombinant S-protein vaccine) or placebo. The primary endpoint was incidence of laboratory-confirmed symptomatic COVID-19 before crossover, with onset within 14 days following the second dose, in participants who were seronegative and reverse transcription polymerase chain reaction (RT-PCR)-negative at baseline. The secondary endpoints included immunogenicity and safety. In total, 8,594 participants were randomised (S-268019-b [n = 5,727]; placebo [n = 2,867]). Vaccine efficacy versus placebo was 39·1 % (95 % confidence interval [CI]:26·6–49·5; one-sided P = 0·0723). The incidence rate (95 % CI) of symptomatic COVID-19 was 776·41/1,000 person-years (682·04–880·19) in the S-268019-b group and 1272·87/1,000 person-years (1101·32–1463·57) in the placebo group. The geometric mean titres (95 % CI) of the SARS-CoV-2 neutralising antibody increased on Day 57 versus baseline with S-268019-b (34·66 [27·04–44·41] versus 2·50 (non-estimable) but not with placebo. There were no safety concerns regarding S-268019-b. S-268019-b did not demonstrate the targeted efficacy threshold against symptomatic COVID-19; however, findings were comparable with other prophylactic vaccines based on ancestor strain during the Omicron-dominant period. S-268019-b demonstrated immunogenicity and was well-tolerated. ClinicalTrials.gov identifier: NCT05212948. [ABSTRACT FROM AUTHOR]

Published

2024

2. Reverse engineering protection: A comprehensive survey of reverse vaccinology-based vaccines targeting viral pathogens.

Author

Ponne, Saravanaraman, Kumar, Rajender, Vanmathi, S.M., Brilhante, Raimunda Sâmia Nogueira, and Kumar, Chinnadurai Raj

Subjects

*VIRAL vaccines, *REVERSE engineering, *VACCINE effectiveness, *PEPTIDE vaccines, *VACCINE development

Abstract

Vaccines have significantly reduced the impact of numerous deadly viral infections. However, there is an increasing need to expedite vaccine development in light of the recurrent pandemics and epidemics. Also, identifying vaccines against certain viruses is challenging due to various factors, notably the inability to culture certain viruses in cell cultures and the wide-ranging diversity of MHC profiles in humans. Fortunately, reverse vaccinology (RV) efficiently overcomes these limitations and has simplified the identification of epitopes from antigenic proteins across the entire proteome, streamlining the vaccine development process. Furthermore, it enables the creation of multiepitope vaccines that can effectively account for the variations in MHC profiles within the human population. The RV approach offers numerous advantages in developing precise and effective vaccines against viral pathogens, including extensive proteome coverage, accurate epitope identification, cross-protection capabilities, and MHC compatibility. With the introduction of RV, there is a growing emphasis among researchers on creating multiepitope-based vaccines aiming to stimulate the host's immune responses against multiple serotypes, as opposed to single-component monovalent alternatives. Regardless of how promising the RV-based vaccine candidates may appear, they must undergo experimental validation to probe their protection efficacy for real-world applications. The time, effort, and resources allocated to the laborious epitope identification process can now be redirected toward validating vaccine candidates identified through the RV approach. However, to overcome failures in the RV-based approach, efforts must be made to incorporate immunological principles and consider targeting the epitope regions involved in disease pathogenesis, immune responses, and neutralizing antibody maturation. Integrating multi-omics and incorporating artificial intelligence and machine learning-based tools and techniques in RV would increase the chances of developing an effective vaccine. This review thoroughly explains the RV approach, ideal RV-based vaccine construct components, RV-based vaccines designed to combat viral pathogens, its challenges, and future perspectives. [ABSTRACT FROM AUTHOR]

Published

2024

3. Flu-COVID combo recombinant protein vaccines elicited protective immune responses against both influenza and SARS-CoV-2 viruses infection.

Author

Huang, Ying, Shi, Hua, Forgacs, David, and Ross, Ted M.

Subjects

*PEPTIDE vaccines, *VIRUS diseases, *INFLUENZA viruses, *SARS-CoV-2, *COVID-19

Abstract

SARS-CoV-2 and Influenza viruses are both highly transmissible airborne viruses and causing high morbidity and mortality. Co-infection of these two viruses results in severe disease that have been observed when influenza and SARS-CoV-2 viruses cocirculated in the past three years, and vaccination is still the effective way to prevent these two diseases. However, influenza and COVID-19 vaccines are designed and manufactured in different platforms, all the individuals will need to get two shots in order to prevent those two severe respiratory diseases. Therefore, it is urgent to develop a Flu-COVID combo vaccine to provide an efficient way for receiving immunization against those two diseases. In this study, we developed a flu-COVID combo vaccine that includes both influenza virus haemagglutinin (HA) proteins and SARS-CoV-2 Spike (S) protein which formulated with AddaVax. K18-hACE-2 transgenic mice were intramuscularly vaccinated with either combo vaccine or mono Flu (HA) or COVID (S) recombinant protein vaccine in a prime-boost-boost regimen, and then were challenged with lethal doses of influenza virus or SARS-CoV-2 to evaluate vaccine efficacy. The results showed that Flu-COVID combo vaccine protected mice from both Influenza and SARS-CoV-2 challenge by preventing body weight loss and clinical signs progression. The protective immune responses elicited by Flu-COVID combo vaccine were equivalent to those elicited by mono flu or COVID recombinant protein vaccines. In conclusion, our study highlights the effectiveness of the FLU-COVID combo recombinant protein vaccine in preventing both influenza and COVID-19 infections. [ABSTRACT FROM AUTHOR]

Published

2024

4. Immunogenicity and protective efficacy of a trimeric full-length S protein subunit vaccine for porcine epidemic diarrhea virus.

Author

Guo, Weilu, Wang, Chuanhong, Song, Xu, Xu, Hong, Zhao, Shuqing, Gu, Jun, Zou, Zhikun, Li, Jing, Qian, Jiali, Zhang, Xue, Guo, Rongli, Li, Jizong, Li, Li, Hu, Zhaoyang, Ren, Lili, Fan, Baochao, and Li, Bin

Subjects

*PEPTIDE vaccines, *PORCINE epidemic diarrhea virus, *IMMUNE response, *KILLER cells, *PORCINE reproductive & respiratory syndrome, *MONONUCLEAR leukocytes, *PIGLETS, *T cells, *B cells

Abstract

• Trimeric S, S1, COEs, and two adjuvants were selected to evaluate immune effects. • S/M103 elicited neutralizing antibodies, T cells, B cells, and NK cells in mice. • S/M103 induced high levels of neutralizing antibodies, IFN-γ, and IL-4 in piglets. • S/M103 provided protection against viral challenge in piglets. Porcine epidemic diarrhea virus (PEDV) has caused serious economic losses to the pig husbandry worldwide, and the effects of existing commercialized vaccines are suboptimal. Therefore, research to develop an efficacious vaccine for prevention and control of PEDV is essential. In this study, we designed and produced trimerized proteins of full-length PEDV spike (S) protein, S1 subunit, and a tandem of multiple epitopes of S protein using an efficient mammalian expression vector system in HEK 293F cells. The immunogenicity of two commercial adjuvants, M401 and M103, was also evaluated in mice. Enzyme-linked immunosorbent assays demonstrated that all immunized mice generated highly systemic PEDV S-specific IgG and IgA antibodies. Mice in S/M103-immunized group generated the highest neutralizing antibody titer with 1:96. Compared with control group, the subunit vaccines elicited multifunctional CD3+CD4+ and CD3+CD8+ T cells, B220+CD19+ B cells, and CD3-CD49b+ natural killer cells in the spleen. PEDV S/M103 vaccine, which had the best immune effect, was selected for further evaluation in piglets. Immunization with S/M103 vaccine induced high levels of S-specific IgG, IgA, and neutralizing antibodies, and increased the proliferation of peripheral blood mononuclear cells and the expression levels of interferon-γ and interleukin-4 in peripheral blood of piglets. Virus challenge test results showed significantly lower diarrheal index scores and fecal viral loads, and less pathological damage to the intestines in S/M103-immunized piglets than in controls, indicating that S/M103 provides good protection against the virulent virus challenge. Our findings suggest that trimeric PEDV S/M103 has potential as a clinical vaccine candidate. [ABSTRACT FROM AUTHOR]

Published

2024

5. A multifaceted approach for identification, validation, and immunogenicity of naturally processed and in silico-predicted highly conserved SARS-CoV-2 peptides.

Author

Ratishvili, Tamar, Quach, Huy Quang, Haralambieva, Iana H., Suryawanshi, Yogesh R., Ovsyannikova, Inna G., Kennedy, Richard B., and Poland, Gregory A.

Subjects

*LIQUID chromatography-mass spectrometry, *IMMUNE response, *T cells, *PEPTIDES, *SARS-CoV-2, *VIRAL proteins, *IMMUNOGLOBULINS, *T cell receptors, *ALLELES

Abstract

SARS-CoV-2 remains a major global public health concern. Antibody waning and immune escape variant emergence necessitate the development of next generation vaccines that induce cross-reactive durable immune responses. T cell responses to SARS-CoV-2 demonstrate higher conservation, antigenic breadth, and longevity than antibody responses. Therefore, we sought to identify pathogen-derived T cell epitopes for a potential peptide-based vaccine. We pursued an approach leveraging: 1) liquid chromatography and tandem mass spectrometry (LC-MS/MS)-based identification of peptides from ancestral SARS-CoV-2-infected cell lines, 2) epitope prediction algorithms, and 3) overlapping peptide libraries. From this strategy, we identified 380 unique SARS-CoV-2-derived peptide sequences, including 53 antigenic HLA class I and class II peptides from multiple structural and non-structural/accessory viral proteins. These peptide sequences were highly conserved across variants of concern/interest (VoC/VoIs), and are estimated to achieve coverage of >96% of the world population. Our findings validate this discovery pipeline for peptide identification and immunogenicity testing, and are a crucial step toward the development of a next-generation multi-epitope SARS-CoV-2 peptide vaccine, and a novel vaccine platform methodology. [ABSTRACT FROM AUTHOR]

Published

2024

6. Six-month safety follow-up of an adjuvanted SARS-CoV-2 trimeric S-protein subunit vaccine (SCB-2019) in adults: A phase 2/3, double-blind, randomized study.

Author

Hosain, Romana, Aquino, Peter, Baccarini, Carmen, Smolenov, Igor, Li, Ping, Qin, Haijing, Verhoeven, Carole, Hu, Branda, Huang, Yung, and Rubio, Pilar

Subjects

*PEPTIDE vaccines, *VACCINES, *BELL'S palsy, *VITRONECTIN, *ADULT respiratory distress syndrome, *CLINICAL trial registries, *SARS-CoV-2

Abstract

• SCB-2019 contains recombinant SARS-CoV-2 S protein adjuvanted with CpG-1018/alum. • Frequencies of unsolicited AEs, MAAEs, SAEs, and AESIs were similar in both arms. • No signs of vaccine-associated enhanced disease were observed. • No safety concerns during the 6-month follow-up after the vaccination. • SCB-2019 has an acceptable safety profile. We evaluated the safety of SCB-2019, a protein subunit vaccine candidate containing a recombinant SARS-CoV-2 spike (S) trimer fusion protein, combined with CpG-1018/alum adjuvants. This ongoing phase 2/3, double-blind, placebo-controlled, randomized trial is being conducted in Belgium, Brazil, Colombia, the Philippines, and South Africa in participants ≥ 12 years of age. Participants were randomly assigned to receive 2 doses of SCB-2019 or placebo administered intramuscularly 21 days apart. Here, we present the safety results of SCB-2019 over the 6-month period following 2-dose primary vaccination series in all adult participants (≥18 years of age). A total of 30,137 adult participants received at least one dose of study vaccine (n = 15,070) or placebo (n = 15,067) between 24 March 2021 and 01 December 2021. Unsolicited adverse events, medically-attended adverse events, adverse events of special interest, and serious adverse events were reported in similar frequencies in both study arms over the 6-month follow-up period. Vaccine-related SAEs were reported by 4 of 15,070 SCB-2019 recipients (hypersensitivity reactions in two participants, Bell's palsy, and spontaneous abortion) and 2 of 15,067 placebo recipients (COVID-19, pneumonia, and acute respiratory distress syndrome in one participant and spontaneous abortion in the other one). No signs of vaccine-associated enhanced disease were observed. SCB-2019 administered as a 2-dose series has an acceptable safety profile. No safety concerns were identified during the 6-month follow-up after the primary vaccination. Clinical Trials Registration: NCT04672395; EudraCT: 2020–004272-17. [ABSTRACT FROM AUTHOR]

Published

2023

7. Immunogenicity of an adjuvanted SARS-CoV-2 trimeric S-protein subunit vaccine (SCB-2019) in SARS-CoV-2-naïve and exposed individuals in a phase 2/3, double-blind, randomized study.

Author

Buntinx, Erik, Brochado, Leonardo, Borja-Tabora, Charissa, Yu, Charles Y., Alberto, Edison R, Montellano, May Emmeline B., Carlos, Josefina C., Toloza, Leonardo Bautista, Hites, Maya, Siber, George, Clemens, Ralf, Ambrosino, Donna, Qin, Haijing, Chen, Hui Ling, Han, Htay Htay, Hu, Branda, Li, Ping, Baccarini, Carmen, and Smolenov, Igor

Subjects

*IMMUNE response, *PEPTIDE vaccines, *VITRONECTIN, *CELLULAR immunity, *SARS-CoV-2, *SARS-CoV-2 Omicron variant

Abstract

• SCB-2019 is a protein subunit vaccine candidate against COVID-19. • SCB-2019 contains the SARS-CoV-2 spike protein adjuvanted with CpG-1018/alum. • A single dose of SCB-2019 was immunogenic in SARS-CoV-2-exposed individuals. • Two doses are required to induce immune response in SARS-CoV-2-naïve individuals. • SCB-2019 induced cross-reactive neutralizing antibodies to SARS-CoV-2 variants. We evaluated immunogenicity of SCB-2019, a subunit vaccine candidate containing a pre-fusion trimeric form of the SARS-CoV-2 spike (S)-protein adjuvanted with CpG-1018/alum. The phase 2/3, double-blind, randomized SPECTRA trial was conducted in five countries in participants aged ≥ 18 years, either SARS-CoV-2-naïve or previously exposed. Participants were randomly assigned to receive two doses of SCB-2019 or placebo administered intramuscularly 21 days apart. In the phase 2 part of the study, on days 1, 22, and 36, neutralizing antibodies were measured by pseudovirus and wild-type virus neutralization assays to SARS-CoV-2 prototype and variants, and ACE2-receptor-binding antibodies and SCB-2019–binding antibodies were measured by ELISA. Cell-mediated immunity was measured by intracellular cytokine staining via flow cytometry. 1601 individuals were enrolled between 24 March and 13 September 2021 and received at least one vaccine dose. Immunogenicity analysis was conducted in a phase 2 subset of 691 participants, including 428 SARS-CoV-2-naïve (381 vaccine and 47 placebo recipients) and 263 SARS-CoV-2-exposed (235 vaccine and 28 placebo recipients). In SARS-CoV-2-naïve participants, GMTs of neutralizing antibodies against prototype virus increased 2 weeks post-second dose (day 36) compared to baseline (224 vs 12.7 IU/mL). Seroconversion rate was 82.5 %. In SARS-CoV-2-exposed participants, one SCB-2019 dose increased GMT of neutralizing antibodies by 48.3-fold (1276.1 IU/mL on day 22) compared to baseline. Seroconversion rate was 92.4 %. Increase was marginal post-second dose. SCB-2019 also showed cross-neutralization capability against nine variants, including Omicron, in SARS-CoV-2-exposed participants at day 36. SCB-2019 stimulated Th1-biased cell-mediated immunity to the S-protein in both naïve and exposed participants. The vaccine was well tolerated, no safety concerns were raised from the study. A single dose of SCB-2019 was immunogenic in SARS-CoV-2-exposed individuals, whereas two doses were required to induce immune response in SARS-CoV-2-naïve individuals. SCB-2019 elicited a cross-neutralizing response against emergent SARS-CoV-2 variants at antibody levels associated with clinical protection, underlining its potential as a booster. Clinicaltrials.gov: NCT04672395; EudraCT: 2020-004272-17. [ABSTRACT FROM AUTHOR]

Published

2023

8. Addition of nucleotide adjuvants enhances the immunogenicity of a recombinant subunit vaccine against the Zika virus in BALB/c mice.

Author

Valdes, Iris, Suzarte, Edith, Lazo, Laura, Cobas, Karem, Cabrales, Ania, Pérez, Yusleidi, Garateix, Rocío, Silva, José A., Aguilar, Julio C., Guzman, Carlos A., and Guillén, Gerardo

Subjects

*PEPTIDE vaccines, *ZIKA virus infections, *CELLULAR immunity, *ZIKA virus, *IMMUNE response

Abstract

Zika virus (ZIKV) infection remains a global public health problem. After the "Public Health Emergencies of International Concern" declared in February 2016, the incidence of new infections by this pathogen has been decreasing in many areas. However, there is still a likely risk that ZIKV will spread to more countries. To date, there is no vaccine or antiviral drug available to prevent or treat Zika virus infection. In the Zika vaccine development, those based on protein subunits are attractive as a non-replicable platform due to their potentially enhanced safety profile to be used in all populations. However, these vaccines frequently require multiple doses and adjuvants to achieve protective immunity. In this study we show the immunological evaluation of new formulations of the recombinant protein ZEC, which combines regions of domain III of the envelope and the capsid from ZIKV. Two nucleotide-based adjuvants were used to enhance the immunity elicited by the vaccine candidate ZEC. ODN 39M or c -di-AMP was incorporated as immunomodulator into the formulations combined with aluminum hydroxide. Following immunizations in immunocompetent BALB/c mice, the formulations stimulated high IgG antibodies. Although the IgG subtypes suggested a predominantly Th1-biased immune response by the formulation including the ODN 39M, cellular immune responses measured by IFNγ secretion from spleen cells after in vitro stimulations were induced by both immunomodulators. These results demonstrate the capacity of both immunomodulators to enhance the immunogenicity of the recombinant subunit ZEC as a vaccine candidate against ZIKV. [ABSTRACT FROM AUTHOR]

Published

2024

9. Reverse vaccinology approach for identification of epitopes from E1 protein as peptide vaccine against HCV: A proof of concept.

Author

Meshram, Rohan, Kolte, Baban, and Gacche, Rajesh

Subjects

*HEPATITIS C vaccines, *PEPTIDE vaccines, *MOLECULAR dynamics, *VACCINE effectiveness, *PEPTIDES

Abstract

[Display omitted] • Computational Identification of Epitopes on E1 glycoprotein in HCV. • Molecular Dynamics Simulations. • Advanced Free energy Estimations using MMPBSA. • Synthesis and characterization of candidate epitope peptides. • Assay for activation of CD4 + and CD8 + T cells using synthesized epitope peptides in healthy individuals, and HCV recovered Human subjects. The development of effective vaccines against Hepatitis C Virus (HCV) remains a global health priority and challenge. In this study, we employed an integrative approach combining computational epitope prediction with experimental validation to identify immunogenic peptides targeting the E1 glycoprotein of HCV. In the present report, computational data from various epitope prediction algorithms such as IEDB and SYFPEITHI, followed by molecular dynamics (MD) simulations and immuno-informatics analysis is presented. Through computational screening, we identified potential epitope candidates, with QVRNSSGLY (P3) and QLFTFSPRH (P7) emerging as promising candidates. MD simulations revealed stable interactions between these epitopes and MHC molecule, further validated by free energy estimations using MMPBSA method. Immuno-informatics analysis supported these findings, showing high binding potential and immunogenicity scores for the selected peptides. Subsequent synthesis and characterization of epitope peptides confirmed their structural integrity and purity required for conducting immune activation assays. Experimental immunological assays carried out in this study involved epitope peptide induced activation of CD8 + and CD4 + T cells from healthy human subjects and HCV- recovered patients. Data from experimental validation revealed significant cytokine release upon exposure to epitope peptides, particularly TNF-a, IL-6, and GM-CSF, indicative of robust immune responses. Notably, peptides P3 and P7 exhibited the most pronounced cytokine induction profiles, underscoring their potential as vaccine candidates. Further investigations addressing the mechanism of action of these epitope peptides under preclinical and clinical settings may help in developing effective vaccine against HCV. [ABSTRACT FROM AUTHOR]

Published

2024

10. Stability and antigenicity of Chlamydia muridarum major outer membrane protein antigen at body temperature.

Author

Russell, Freya A., Trim, Logan, Bryan, Emily, Fisher, Mark A., Leahy, Darren, Harris, Jonathan M., Hutmacher, Dietmar, Dargaville, Tim R., and Beagley, Kenneth W.

Subjects

*PEPTIDE vaccines, *BOOSTER vaccines, *MEMBRANE proteins, *GENITALIA, *BODY temperature

Abstract

• Degradation of a major outer membrane protein at 37 °C for four to six weeks. • In vitro assessment to determine whether aged protein retains antigenicity. • In vivo assessment to determine whether aged protein retains immunogenicity. • Histological analysis of mice reproductive tracts to determine aged protein protective ability. Chlamydia is an obligate intracellular bacterial pathogen responsible for disease and infertility across multiple species. Currently vaccines are being studied to help reduce the prevalence of this disease. The main advantage of protein subunit vaccines is their high degree of safety although this is traded off with the requirement for multiple booster doses to achieve complete protection. Although in certain populations the booster dose can be difficult and costly to administer, development of delayed vaccine delivery techniques, such as a vaccine capsule, could be the solution to this problem. One of the main drawbacks in this technology is that the antigen must remain stable at body temperature (37 °C) until release is achieved. Here we elucidate the stability of a recombinant chlamydial major outer membrane protein (MOMP) antigen and assess its antigenic and immunogenic properties after subjecting the antigen to 37 °C for four to six weeks. Through in vitro and in vivo assessment we found that the aged chlamydial MOMP was able to produce equivalent humoral and cell-mediated immune responses when compared with the unaged vaccine. It was also found that vaccines formulated with the aged antigen conferred equivalent protection against a live infection challenge as the unaged antigen. Thus ageing chlamydial MOMP antigens at 37 °C for four to six weeks did not cause any significant structural or antigenic/immunogenic degradation and recombinant C. muridarum MOMP is suitable for use in a delayed vaccine delivery system. [ABSTRACT FROM AUTHOR]

Published

2024

11. Efficacy and safety of Abdala COVID-19 subunit vaccine in children and adolescents: An open-label, single-arm, phase 2 trial (MEÑIQUE).

Author

Hernández-Bernal, Francisco, Noa-Romero, Enrique, Quintana-Guerra, Joel, Chávez-Chong, Cristina O., Martín-Bauta, Yenima, Alvaré-Alvaré, Laura, Salvato-Dueñas, Alena, Felipe-Mallea, Danusia, Porta-Díaz, Mairalys, Cruz-Sui, Otto, Urrutia-Pérez, Karen, Urrutia-Pérez, Klaudia, Rodríguez-Reinoso, José L., Alonso-Valdés, Marel, Cinza-Estévez, Zurina, Rodríguez-Triana, Aylin, Cruz-Gómez, Yolanda, Limonta-Fernández, Miladys, Rodríguez-Acosta, Mireida, and Ayala-Ávila, Marta

Subjects

*PEPTIDE vaccines, *SARS-CoV-2 Delta variant, *COVID-19, *AGE groups, *COVID-19 vaccines

Abstract

Objectives We evaluated the safety, immunogenicity and efficacy of Abdala, a protein subunit vaccine for 2019 coronavirus disease (COVID-19), in children and adolescents. Methods A phase 2, open-label, single-arm clinical trial was carried out. Subjects aged 3 to 18 years were eligible. Abdala vaccine was administered intramuscularly at 0–14-28 days. The main endpoints were safety and the immunobridging analysis with a non-inferiority design, to infer the efficacy of the vaccine in paediatric population based on the comparison of neutralizing antibodies (NAb) to SARS-CoV-2, with adults (19–21 years). The trial is registered with the Cuban Public Registry of Clinical Trials, RPCEC00000390. Results From September 13th to September 17th, 2021, 703 participants were included in the context of a predominantly SARS-CoV-2 Delta variant circulation. The number of individuals who experienced adverse reactions was 264/703 (37·6%). Adverse reactions were mostly mild and occurred at the injection site, which resolved within the first 24–48 h. There were no reports of severe adverse events. For the non-inferiority comparison of 297 children (3–11 years) with 297 adults, the geometric mean (GMT) ratio of SARS-CoV-2 NAb was 0·87 (95% CI 0·69–1·08) and 1·07 (0·82–1·39) in the same comparison for 203 adolescents (12–18 years) and 203 adults. For both age groups, the lower limit of GMT was higher than 0·67. The differences in seroresponse rates of Nab for children were 1% (−2%, 4%) and −3% (−7%, 1%) for adolescents, higher than −10% in both age groups. Conclusions The Abdala vaccine was safe and immunogenic in a paediatric population aged 3–18 years, with inferred efficacy based on non-inferior analysis. The vaccine is very suitable to fit into massive vaccination strategies, considering the advantages of using the same vaccine strength (RBD 50 μg) and schedule of administration for both adults and children, as well as the easy storage and handling conditions at 2–8 °C. • Abdala is a COVID-19 subunit vaccine based on RBD protein with demonstrated clinical efficacy and safety in adults. • Abdala is safe, well tolerated and induces neutralizing antibody titers against SARS-CoV-2 in children and adolescents. • The efficacy of Abdala in paediatric population was inferred from a non-inferiority immunobridging analysis with adults. • Abdala is very suitable to be included into massive vaccination strategies for children, adolescents and adults. [ABSTRACT FROM AUTHOR]

Published

2024

12. A novel strategy to mimic discontinuous protective epitopes using a synthetic scaffold

Author

Hijnen, Marcel, van Zoelen, Dirk J., Chamorro, Cristina, van Gageldonk, Pieter, Mooi, Frits R., Berbers, Guy, and Liskamp, Rob M.J.

Subjects

*EPITOPES, *IMMUNOGLOBULINS, *PREVENTIVE medicine, *VACCINATION

Abstract

Abstract: Although vaccines have been used for a long time and different types of vaccines have been developed, as yet no fully synthetic vaccines have been produced. The production of fully synthetic vaccines has probably not been realized so far due to the structural limitations of linear synthetic peptides to mimic the native shape of protein fragments which is often needed to induce protective antibodies. In this report we used the Bordetella pertussis protein pertactin as a model and show that a novel synthetic scaffold can be used to mimic structurally defined epitopes by confined presentation of several different peptide arms. Guided by modelling a construct was synthesized that induced protective antibodies directed towards a discontinuous epitope. This approach opens up the possibility to the design of new and fully synthetic vaccines that can induce protective antibodies. [Copyright &y& Elsevier]

Published

2007

13. Functional memory CD8+ T cells can be generated in vivo without evident T help

Author

Andrews, Melanie R., Peters, Tania, Khammanivong, Vithagna, Leggatt, Graham R., Frazer, Ian H., and Fernando, Germain J.P.

Subjects

*T cells, *LYMPHOCYTES, *PROTEINS, *BIOMOLECULES

Abstract

Abstract: Synthetic cytotoxic T cell (CTL) epitope peptides provide an effective and safe means of vaccination against cancers and viruses, as these peptides can induce specific CD8+ effector T cells in vivo. However, the effector CD8+ T cells induced by the minimal CTL epitope peptides do not last past about 3 weeks after the induction and no functional memory CD8+ T cells are generated. It is held that simultaneous induction of CD4+ T cells by incorporating peptides containing T-helper epitopes in the vaccine at the time of primary vaccination are necessary for the induction of long-lived functional memory CD8+ T cells. We now report that, surprisingly, incorporation of medium length (>20 AA) peptides devoid of detectable T-helper epitopes in a minimal CTL epitope-based vaccine can also induce long-lasting functional tumour antigen specific memory CD8+ T cells that are capable of promoting protection against tumour challenge. This observation may have implications for the formulation of therapeutic anti-cancer and anti-virus peptide vaccines where a strong induction of CD4 T help would be undesirable. [Copyright &y& Elsevier]

Published

2004

14. A synthetic peptide containing the consensus sequence of the G–H loop region of foot-and-mouth disease virus type-O VP1 and a promiscuous T-helper epitope induces peptide-specific antibodies but fails to protect cattle against viral challenge

Author

Rodriguez, Luis L., Barrera, Jose, Kramer, Ed, Lubroth, Juan, Brown, Fred, and Golde, William T.

Subjects

*IMMUNOGENETICS, *IMMUNOGLOBULINS, *PEPTIDES

Abstract

A pilot study was carried out in cattle to determine the immunogenicity of a synthetic consensus peptide comprising the G–H loop region of foot-and-mouth disease virus (FMDV) type-O VP1 and a non-VP1 T-helper (Th) epitope. Cattle vaccinated intramuscularly either once (n=5) or twice (n=4) with 50 μg of the peptide preparation at a 21-day interval developed antibodies to the peptide as determined by ELISA with the exception of one steer that received a single dose. However, neutralizing antibody titers against FMDV type-O were modest and all animals presented with clinical FMD signs upon challenge 21 days after the last vaccination. In contrast, four of the five animals inoculated with an inactivated FMD type-O commercially prepared vaccine developed neutralizing antibodies and were fully protected against clinical disease following virus challenge 21 days post-vaccination (dpv). Nucleotide sequence comparison of the VP1 region between the challenge virus and RT-PCR products recovered from a lesion of the peptide-vaccinated animal with the highest neutralizing antibody titer 5 days post-challenge (dpc) showed no evidence for selection of a neutralization-resistant mutant. We conclude that although the synthetic peptide induced an antibody response in cattle, it failed to confer protection against FMDV challenge. [Copyright &y& Elsevier]

Published

2003

15. In vivo anti-melanoma activities of the Melan-A/MART-1101–115 T CD4+ cell peptide

Author

Balasse, Emilie, Gatouillat, Gregory, Patigny, Dominique, Andry, Marie Christine, and Madoulet, Claudie

Subjects

*CANCER vaccines, *TUMOR antigens, *ANTINEOPLASTIC agents, *MELANOMA treatment, *PEPTIDES, *T cells, *IMMUNE response, *IMMUNOTHERAPY, *AMINO acid sequence, *THERAPEUTICS

Abstract

Abstract: Malignant melanoma causes significant health problems. The identification of tumour-associated antigens has led to novel approaches to increase T cell mediated anti-tumour immune response. Melan-A/MART-1 has been use as target antigen for several T cell based immunotherapeutic treatments. More recently, the critical role of CD4+ T cells in inducing and maintaining anti-tumour immunity has been increasingly recognized. In order to optimize tumour immunotherapy, greater efforts have been concentrated on the identification of tumour antigens presented by MHC class II molecules to CD4+ T cells. In a publication, Tiwari et al. (2004) have identified by a computational approach the 15-mer amino-acid sequence 101–115 (PPAYEKLSAEQSPPP) of the Melan-A/MART-1 as a good target for a vigorous and safe immunotherapy. Therefore, we have investigated the in vivo anti-tumour activity of this peptide in a murine melanoma model. For the prophylactic treatment, 20μg or 50μg peptide was subcutaneously injected in mice once a week during 3 weeks before tumour induction. Treatment with 50μg peptide significantly affected tumour development. Thus, our preliminary data demonstrate potential in vivo prophylactic activity of the 101–115 peptide-based vaccine to control melanoma growth. [Copyright &y& Elsevier]

Published

2009