Your search keyword '"peptide vaccines"' showing total 71 results

1. VEGF165b mutant can be used as a protein carrier to form a chimeric tumor vaccine with Mucin1 peptide to elicit an anti-tumor response.

Author

Liang, Chen, Geng, Lujing, Dong, Yifan, and Zhang, Huiyong

Subjects

*PEPTIDE vaccines, *CARRIER proteins, *CANCER vaccines, *CHIMERIC proteins, *REGULATORY T cells

Abstract

Peptide-based anticancer vaccines have shown some efficacy in generating cancer-specific immune responses in various cancer studies, but clinical success is limited, one of the reasons is due to its prone degradation and weak immunogenicity. So some tumor epitope peptide vaccines often require coupling or forming fusion proteins with corresponding protein carriers to enhance their stability and immunogenicity. Given the scarcity of validated carriers for clinical trials, there is an urgent requirement for the development of novel protein carrier. Our previous work has demonstrated that VEGF165b mutant could be used as an effective immunization adjunct to enhance anti-tumor immune response. By analyzing and evaluating the gene structure of VEGF, we speculated that mVEGF165b has the potential to be utilized as a tumor peptide vaccine carrier. An mVEGF165b-MUC1 chimeric tumor vaccine was produced by fusing the MUC1 peptide （(MUC1, a T-cell epitope dominant peptide from Mucin1） to the C-terminus of mVEGF165b, expressing the fusing protein in pichia yeast, followed by purification with a HiTrap heparin affinity chromatography column. We found that immunizing mice with mVEGF165b-MUC1 fusion protein induced high-titer antibodies against VEGF in a preventive context, which in turn reduced the proportion of Tregs and further stimulated mice to produce T-cell responses specific to mucin1. The high-titer VEGF antibody stimulated by mVEGF165b also promoted tumor blood vessel maturation and facilitated T-cell infiltration. In conclusion，immunized with mVEGF165b-MUC1 protein are beneficial for eliciting immune responses targeting Mucin1, mVEGF165b have the potential to be utilized as a peptide tumor vaccine carrier. • mVEGF165b can be used as a protein carrier for the MUC1 peptide. • High anti-VEGF antibody titers induced by mVEGF165b-MUC1 decreased immunosuppression by reducing the proportion of Tregs. • The decreased immunosuppression augmented the immune response induced by the peptide vaccine from Mucin-1. [ABSTRACT FROM AUTHOR]

Published

2024

2. Identification of a novel DEC-205 binding peptide to develop dendritic cell-targeting nanovaccine for cancer immunotherapy.

Author

Zheng, Jie, Wang, Mingshuang, Pang, Liwei, Wang, Shuai, Kong, Yanan, Zhu, Xueqin, Zhou, Xiuman, Wang, Xiaoxi, Chen, Chunxia, Ning, Haoming, Zhao, Wenshan, Zhai, Wenjie, Qi, Yuanming, Wu, Yahong, and Gao, Yanfeng

Subjects

*VACCINE effectiveness, *ANTIGEN presentation, *DENDRITIC cells, *CANCER vaccines, *PEPTIDE vaccines

Abstract

Cancer vaccine is regarded as an effective immunotherapy approach mediated by dendritic cells (DCs) which are crucial for antigen presentation and the initiation of adaptive immune responses. However, lack of DC-targeting properties significantly hampers the efficacy of cancer vaccines. Here, by using the phage display technique, peptides targeting the endocytic receptor DEC-205 primarily found on cDC1s were initially screened. An optimized hydrolysis-resistant peptide, hr-8, was identified and conjugated to PLGA-loaded antigen (Ag) and CpG adjuvant nanoparticles, resulting in a DC-targeting nanovaccine. The nanovaccine hr-8-PLGA@Ag/CpG facilitates dendritic cell maturation and improves antigen cross-presentation. The nanovaccine can enhance the antitumor immune response mediated by CD8+ T cells by encapsulating the nanovaccine with either exogenous OVA protein antigen or endogenous gp100/E7 antigenic peptide. As a result, strong antitumor effects are observed in both anti-PD-1 responsive B16-OVA and anti-PD-1 non-responsive B16 and TC1 immunocompetent tumor models. In summary, this study presents the initial documentation of a nanovaccine that targets dendritic cells via the novel DEC-205 binding peptide. This approach offers a new method for developing cancer vaccines that can potentially improve the effectiveness of cancer immunotherapy. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

3. Use of a meningococcal group B vaccine (4CMenB) in populations at high risk of gonorrhoea in the UK.

Author

Ladhani, Shamez N, White, Peter J, Campbell, Helen, Mandal, Sema, Borrow, Ray, Andrews, Nick, Bhopal, Sunil, Saunders, John, Mohammed, Hamish, Drisdale-Gordon, Lana, Callan, Emma, Sinka, Katy, Folkard, Kate, Fifer, Helen, and Ramsay, Mary E

Subjects

*PEPTIDE vaccines, *SEXUALLY transmitted diseases, *GONORRHEA, *NEISSERIA gonorrhoeae, *MENINGOCOCCAL infections, *MEDICAL care

Abstract

The meningococcal group B vaccine, 4CMenB, is a broad-spectrum, recombinant protein vaccine that is licensed for protection against meningococcal group B disease in children and adults. Over the past decade, several observational studies supported by laboratory studies have reported protection by 4CMenB against gonorrhoea, a sexually transmitted infection caused by Neisseria gonorrhoeae. Gonorrhoea is a major global public health problem, with rising numbers of diagnoses and increasing resistance to multiple antibiotics. In England, more than 82 000 cases of gonorrhoea were diagnosed in 2022, with nearly half of the cases diagnosed among gay, bisexual, and other men who have sex with men. There are currently no licensed vaccines against gonorrhoea but 4CMenB is estimated to provide 33–47% protection against gonorrhoea. On Nov 10, 2023, the UK Joint Scientific Committee on Vaccination and Immunisation agreed that a targeted programme should be initiated using 4CMenB to prevent gonorrhoea among individuals at higher risk of infection attending sexual health services in the UK. This decision was made after reviewing evidence from retrospective and prospective observational studies, laboratory and clinical data, national surveillance reports, and health economic analyses. In this Review, we summarise the epidemiology of invasive meningococcal disease and gonorrhoea in England, the evidence supporting the use of 4CMenB for protection against gonorrhoea, and the data needed to inform long-term programme planning and extension to the wider population. [ABSTRACT FROM AUTHOR]

Published

2024

4. Next-generation Dengue Vaccines: Leveraging Peptide-Based Immunogens and Advanced Nanoparticles as Delivery Platforms.

Author

Rahman, Nur Adilah Abdul, Fuaad, Abdullah Al-Hadi Ahmad, Azami, Nor Azila Muhammad, Amin, Mohd Cairul Iqbal Mohd, and Azmi, Fazren

Subjects

*B cell receptors, *PEPTIDE vaccines, *CELL-penetrating peptides, *AUTOIMMUNE diseases, *VACCINE effectiveness, *DENGUE viruses, *DENGUE

Abstract

Dengue, caused by the dengue virus (DENV), is a prevalent arthropod-borne disease in humans and poses a significant burden on public health. Severe cases of dengue can be life-threatening. Although a licensed dengue vaccine is available, its efficacy varies across different virus serotypes and may exacerbate the disease in some seronegative recipients. Developing a safe and effective vaccine against all DENV serotypes remains challenging and requires continued research. Conventional approaches in dengue vaccine development, using live or attenuated microorganisms or parts of them often contain unnecessary epitopes, risking allergenic or autoimmune reactions. To address these challenges, innovative strategies such as peptide vaccines have been explored. Peptide vaccines offer a safer alternative by inducing specific immune responses with minimal immunogenic fragments. Chemical modification strategies of peptides have revolutionized their design, allowing for the incorporation of multi-epitope presentation, self-adjuvanting features, and self-assembling properties. These modifications enhance the antigenicity of the peptides, leading to improved vaccine efficacy. This review outlines advancements in peptide-based dengue vaccine development, leveraging nanoparticles as antigen-displaying platforms. Additionally, key immunological considerations for enhancing efficacy and safety against DENV infection have been addressed, providing insight into the next-generation of dengue vaccine development leveraging on peptide-nanoparticle technology. The delivery of peptide vaccines in nanoparticle form facilitates the presentation of antigenic epitopes, fostering a multivalent interaction with host cells like B cells. This arrangement promotes a more efficient clustering of B cell receptors compared to interactions with a single peptide antigen. [Display omitted] • Integration of functional components such as T-helper epitopes, immune-stimulating lipids, and cell-penetrating peptides with antigens to enhance the potency of subunit peptide vaccines. • Progress in nanotechnology-based dengue vaccine, emphasizing the benefits of virus mimicry for immune enhancement. • Development of a next-generation multi-epitope-based peptide dengue vaccine candidate utilizing nanoparticles as a delivery platform. [ABSTRACT FROM AUTHOR]

Published

2024

5. 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

6. Neoantigens and cancer-testis antigens as promising vaccine candidates for triple-negative breast cancer: Delivery strategies and clinical trials.

Author

Malla, RamaRao, Srilatha, Mundla, Muppala, Veda, Farran, Batoul, Chauhan, Virander Singh, and Nagaraju, Ganji Purnachandra

Subjects

*TRIPLE-negative breast cancer, *TESTICULAR cancer, *CLINICAL trials, *SOMATIC mutation, *CANCER vaccines

Abstract

Immunotherapy is gaining prominence as a promising strategy for treating triple-negative breast cancer (TNBC). Neoantigens (neoAgs) and cancer-testis antigens (CTAs) are tumor-specific targets originating from somatic mutations and epigenetic changes in cancer cells. These antigens hold great promise for personalized cancer vaccines, as supported by preclinical and early clinical evidence in TNBC. This review delves into the potential of neoAgs and CTAs as vaccine candidates, emphasizing diverse strategies and delivery approaches. It also highlights the current status of vaccination modalities undergoing clinical trials in TNBC therapy. A comprehensive understanding of neoAgs, CTAs, vaccination strategies, and innovative delivery methods is crucial for optimizing neoAg-based immunotherapies in clinical practice. [Display omitted] • Neoantigens and cancer-testis antigens are promising vaccine candidates for triple-negative breast cancer. • NeoAgs and cancer testis antigens expression in triple-negative breast cancer can be enhanced. • Various vaccine delivery strategies for breast cancer have been developed and tested in clinical trials. • Targeted therapies can improve triple-negative breast cancer management. [ABSTRACT FROM AUTHOR]

Published

2024

7. The predominant Quillaja Saponaria fraction, QS-18, is safe and effective when formulated in a liposomal murine cancer peptide vaccine.

Author

Zhou, Shiqi, Song, Yiting, Nilam, Anoop, Luo, Yuan, Huang, Wei-Chiao, Long, Mark D., and Lovell, Jonathan F.

Subjects

*PEPTIDE vaccines, *LIPOSOMES, *T cells, *CANCER vaccines, *T cell receptors, *PEPTIDES, *VACCINE development, *SAPONINS

Abstract

Extracts of the Chilean soapbark tree , Quillaja Saponaria (QS) are the source of potent immune-stimulatory saponin compounds. This study compared the adjuvanticity and toxicity of QS-18 and QS-21, assessing the potential to substitute QS-18 in place of QS-21 for vaccine development. QS-18, the most abundant QS saponin fraction, has been largely overlooked due to safety concerns. We found that QS-18 spontaneously inserted into liposomes, thereby neutralizing hemolytic activity, and following administration did not induce local reactogenicity in a footpad swelling test in mice. With high-dose intramuscular administration, transient weight loss was minor, and QS-18 did not induce significantly more weight loss compared to a liposome vaccine adjuvant system lacking it. Two days after administration, no elevation of inflammatory cytokines was detected in murine serum. In a formulation including cobalt-porphyrin-phospholipid (CoPoP) for short peptide sequestration, QS-18 did not impact the formation of peptide nanoparticles. With immunization, QS-18 peptide particles induced higher levels of cancer neoepitope-specific and tumor-associated antigen-specific CD8+ T cells compared to QS-21 particles, without indication of greater toxicity based on mouse body weight. T cell receptor sequencing of antigen-specific CD8+ T cells showed that QS-18 induced significantly more T cell transcripts. In two murine cancer models, vaccination with QS-18 peptide particles induced a similar therapeutic effect as QS-21 particles, without indication of increased toxicity. Antigen-specific CD8+ T cells in the tumor microenvironment were found to express the exhaustion marker PD-1, pointing to the rationale for exploring combination therapy. Taken together, these data demonstrate that QS-18, when formulated in liposomes, can be a safe and effective adjuvant to induce tumor-inhibiting cellular responses in murine models with potential to facilitate or diminish costs of production for vaccine adjuvant systems. Further studies are warranted to assess liposomal QS-18 immunogic, reactogenic and toxicological profiles in mice and other animal species. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

8. 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

9. 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

10. 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

11. Protein subunit vaccines: Promising frontiers against COVID-19.

Author

Chavda, Vivek P., Ghali, Eswara Naga Hanuma Kumar, Balar, Pankti C., Chauhan, Subhash C., Tiwari, Nikita, Shukla, Somanshi, Athalye, Mansi, Patravale, Vandana, Apostolopoulos, Vasso, and Yallapu, Murali M.

Subjects

*PEPTIDE vaccines, *COVID-19, *VACCINE effectiveness, *VIRAL proteins, *VACCINE development

Abstract

The emergence of COVID-19 has posed an unprecedented global health crisis, challenging the healthcare systems worldwide. Amidst the rapid development of several vaccine formulations, protein subunit vaccines have emerged as a promising approach. This article provides an in-depth evaluation of the role of protein subunit vaccines in the management of COVID-19. Leveraging viral protein fragments, particularly the spike protein from SARS-CoV-2, these vaccines elicit a targeted immune response without the risk of inducing disease. Notably, the robust safety profile of protein subunit vaccines makes them a compelling candidate in the management of COVID-19. Various innovative approaches, including reverse vaccinology, virus like particles, and recombinant modifications are incorporated to develop protein subunit vaccines. In addition, the utilization of advanced manufacturing techniques facilitates large-scale production, ensuring widespread distribution. Despite these advancements, challenges persist, such as the requirement for cold-chain storage and the necessity for booster doses. This article evaluates the formulation and applications of protein subunit vaccines, providing a comprehensive overview of their clinical development and approvals in the context of COVID-19. By addressing the current status and challenges, this review aims to contribute to the ongoing discourse on optimizing protein subunit vaccines for effective pandemic control. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

12. Society for Maternal-Fetal Medicine Statement: Clinical considerations for the prevention of respiratory syncytial virus disease in infants.

Author

Joseph, Naima T., Kuller, Jeffrey A., Louis, Judette M., and Hughes, Brenna L.

Subjects

RESPIRATORY syncytial virus infections, OBSTETRICS, HUMAN metapneumovirus infection, CLINICAL medicine, PEPTIDE vaccines, RESPIRATORY syncytial virus

Abstract

Respiratory syncytial virus is a leading cause of lower respiratory tract illness globally in children aged <5 years. Each year, approximately 58,000 hospitalizations in the United States are attributed to respiratory syncytial virus. Infants aged ≤6 months experience the most severe morbidity and mortality. Until recently, prevention with the monoclonal antibody, palivizumab, was only offered to infants with high-risk conditions, and treatment primarily consisted of supportive care. Currently, 2 products are approved for the prevention of respiratory syncytial virus in infants. These include the Pfizer bivalent recombinant respiratory syncytial virus prefusion F protein subunit vaccine, administered seasonally to the pregnant person between 32 0/7 and 36 6/7 weeks of gestation, and the monoclonal antibody, nirsevimab, administered to infants aged up to 8 months entering their first respiratory syncytial virus season. With few exceptions, administering both the vaccine to the pregnant person and the monoclonal antibody to the infant is not recommended. All infants should be protected against respiratory syncytial virus using one of these strategies. Key considerations for pregnant individuals include examining available safety and efficacy data, weighing accessibility and availability, and patient preferences for maternal vaccination vs infant monoclonal antibody treatment. It will be critical for maternal–fetal medicine physicians to provide effective and balanced counseling to aid patients in deciding on a personalized approach to the prevention of respiratory syncytial virus in their infants. [ABSTRACT FROM AUTHOR]

Published

2024

13. 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

14. Personalized Tumor Neoantigen Peptide Vaccine Combined with Radiotherapy in the Treatment of Advanced Tumors - Phase II Randomized Group Study.

Author

Zhang, Y., Li, R., Hu, Y.F., Dai, W., Wang, J., Xu, Z.Y., Su, X., Huang, J., and Kong, F.M.

Subjects

*PEPTIDE vaccines, *CANCER vaccines, *TUMOR growth, *RADIATION doses, *RADIOTHERAPY

Abstract

Neoantigen-based vaccine has shown amazing efficacy in some solid tumors such as melanoma, GBM, NSCLC and CRC. However, neoantigen vaccination has limited activity in stage IV patients, due to ineffective T-cell function and the large tumor burden. The hypothesis of our study is that in stage IV patients, neoantigen peptide vaccines combined with precision radiation therapy (CLERT), delivering optimized radiotherapy doses to tumor-critical regions in multifocal patients, can synergistically inhibit tumor growth. Our main research purpose was to evaluate and explore the anti -tumor activity of personalized tumor neoantigen peptide vaccine combined with radiotherapy in the treatment of patients with advanced malignant tumors. Patients must meet all of the following inclusion criteria to be enrolled in this study: 1) Patients with advanced or recurrent tumors diagnosed by pathology and imaging, who have failed first-line treatments or have progressed; 2) Patients with expected survival ≥3 months and with ECOG (Eastern Cooperative Oncology Group) score was 0-2 points; 3) Patients had more than 1 predicted high-quality tumor neoantigen. This study is an open-label, multicenter phase II randomized study. Includes 2 cohorts: placebo + conventional treatment (including radiotherapy) group; Personalized tumor peptide vaccine + conventional treatment (including radiotherapy) group. Patients were stratified by first, second, and third-line treatment stages based on individual condition assessment, and then randomly entered two cohorts in a 1:1 ratio. In addition, after patients in cohort 1 have disease progression or ineffectiveness after the first-stage treatment, they can "cross-over" to cohort 2 for the second-stage personalized neoantigen peptide vaccine group + conventional treatment (including radiotherapy) through a one-way crossover experiment, and will evaluate response rates in both phases before and after crossover. The clinical trial is initially designed to recruit 154 patients. It has obtained academic and ethical approval and obtained clinical trial registration number ChiCTR2300078055. Preliminary screening of 20 patients has been completed, and two people have been officially enrolled. It is currently recruiting. This clinical design of precision radiotherapy combined with tumor neoantigen vaccine will allow us to answer questions about vaccination efficacy and the impact of various radiation doses and expect to provide new opportunities for patients with advanced and refractory solid tumors. [ABSTRACT FROM AUTHOR]

Published

2024

15. 813MO Phase I trial of a personalized multi-peptide vaccine combined with the TLR1/2 ligand XS15 under Bruton-Tyrosine-Kinase inhibitor (BTKi) treatment in chronic lymphocytic leukemia (CLL) patients.

Author

Hackenbruch, C., Heitmann, J.S., Jung, S., Maringer, Y., Wacker, M., Nelde, A., Marconato, M., Zieschang, L., Kammer, C., Özbek, M.T., Richter, M., Denk, M., Salih, H.R., and Walz, J.S.

Subjects

*CHRONIC lymphocytic leukemia, *PEPTIDE vaccines

Published

2024

16. 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

17. 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

18. Peptide vaccine design against glioblastoma by applying immunoinformatics approach.

Author

Mohammadi, Mahsa, Razmara, Jafar, Hadizadeh, Morteza, Parvizpour, Sepideh, and Shahir Shamsir, Mohd

Subjects

*PEPTIDE vaccines, *BRAIN tumors, *VACCINE manufacturing, *OVERALL survival, *DRUG therapy, *CYTOTOXIC T cells

Abstract

• Immunoinformatics approach was used to design a multi-epitope peptide vaccine against glioblastoma. • ITGA5 was considered as the target gene by targeting the PI3K-Akt pathway as a significant association with patient survival. • The vaccine peptide was constructed by fusing the CD8+ cytotoxic T lymphocytes (CTLs) epitopes, helper epitopes and adjuvant. • Different evaluations and simulations were conducted to validate the potential of the vaccine candidate against glioblastoma. Brain tumors are considered to be one of the most fatal forms of cancer owing to their highly aggressive attributes, diverse characteristics, and notably low rate of survival. Among these tumors, glioblastoma stands out as the prevalent and perilous variant Despite the present advancements in surgical procedures, pharmacological treatment, and radiation therapy, the overall prognosis remains notably unfavorable, as merely 4.3 % of individuals manage to attain a five-year survival rate; For this reason, it has emerged as a challenge for cancer researchers. Therefore, among several immunotherapy methods, using peptide-based vaccines for cancer treatment is considered promising due to their ability to generate a focused immune response with minimal damage. This study endeavors to devise a multi-epitope vaccine utilizing an immunoinformatics methodology to address the challenge posed by glioblastoma disease. Through this approach, it is anticipated that the duration and expenses associated with vaccine manufacturing can be diminished, while simultaneously enhancing the characteristics of the vaccine. The target gene in this research is ITGA5, which was achieved through TCGA analysis by targeting the PI3K-Akt pathway as a significant association with patient survival. Subsequently, the suitable epitopes of T and B cells were selected through various immunoinformatics tools by analyzing their sequence. Then, nine epitopes were merged with GM-CSF as an adjuvant to enhance immunogenicity. The outcomes encompass molecular docking, molecular dynamics (MD) simulation, simulation of the immune response, prognosis and confirmation of the secondary and tertiary structure, Chemical and physical characteristics, toxicity, as well as antigenicity and allergenicity of the potential vaccine candidate against glioblastoma. [ABSTRACT FROM AUTHOR]

Published

2024

19. Unlocking Immunity: Innovative prostate cancer vaccine strategies.

Author

Gu, Qiannan., Qi, Anning., Wang, Ne., Zhou, Zhenxian., and Zhou, Xiaohui.

Subjects

*PEPTIDE vaccines, *CANCER vaccines, *DNA vaccines, *ORAL vaccines, *IMMUNE checkpoint inhibitors

Abstract

• New Immunotherapy Breakthrough. • Diverse Vaccine Approaches. • Potential of Personalized Care. • Innovations in Vaccine Tech. Prostate Cancer (PCa) is a leading cause of cancer-related mortality in men, especially in Western societies. The objective of this research is to address the unmet need for effective treatments in advanced or recurrent PCa, where current strategies fall short of offering a cure. The focus is on leveraging immunotherapy and cancer vaccines to target the tumor's unique immunological microenvironment. Despite immunotherapy's success in other cancers, its effectiveness in PCa has been limited by the tumor's immunosuppressive characteristics. However, cancer vaccines that engage Tumor-Specific Antigens (TSA) and Tumor-Associated Antigens (TAA) have emerged as a promising approach. Preclinical and clinical investigations of Dendritic Cell (DC) vaccines, DNA vaccines, mRNA vaccines, peptide vaccines, and viral vectors have shown their potential to elicit anti-tumor immune responses. The exploration of combination therapies with immune checkpoint inhibitors and the advent of novel adjuvants and oral microparticle vaccines present innovative strategies to improve efficacy and compliance. The development of cancer vaccines for PCa holds significant potential. Future directions include optimizing vaccine design, refining combination therapy strategies, and creating patient-friendly administration methods. The integration of interdisciplinary knowledge and innovative clinical trial designs is essential for advancing personalized and precision immunotherapy for PCa. [ABSTRACT FROM AUTHOR]

Published

2024

20. Old concepts, new tricks: How peptide vaccines are reshaping cancer immunotherapy?

Author

Liu, Qingyang, Wu, Peihua, Lei, Jun, Bai, Peng, Zhong, Peiluan, Yang, Min, and Wei, Pengcheng

Subjects

*PEPTIDE vaccines, *HLA histocompatibility antigens, *CANCER vaccines, *T cells, *VACCINE development, *IMMUNE response

Abstract

Over the past few decades, research on cancer immunotherapy has firmly established immune cells as key players in effective cancer treatment. Peptide vaccines directly targeting immune cells have demonstrated immense potential due to their specificity and applicability. However, developing peptide vaccines to generate tumor-reactive T cells remains challenging, primarily due to suboptimal immunogenicity and overcoming the immunosuppressive tumor microenvironment (TME). In this review, we discuss various elements of effective peptide vaccines, including antigen selection, peptide epitope optimization, vaccine adjuvants, and the combination of multiple immunotherapies, in addition to recent advances in tumor neoantigens as well as epitopes bound by non-classical human leukocyte antigen (HLA) molecules, to increase the understanding of cancer peptide vaccines and provide multiple references for the design of subsequent T cell-based peptide vaccines. [ABSTRACT FROM AUTHOR]

Published

2024

21. 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

22. 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

23. Immunogenicity of Abdala COVID-19 vaccine in Vietnamese people after primary and booster vaccinations: A prospective observational study in Vietnam.

Author

Thanh, Tran Tan, Tu, Nguyen Thi Kha, Nguyet, Lam Anh, Thuy, Cao Thu, Thuan, Nguyen Lam Thai, Ny, Nguyen Thi Han, Nhu, Le Nguyen Truc, Thanh, Le Kim, Hong, Nguyen Thi Thu, Anh, Nguyen To, Truong, Nguyen Thanh, Chau, Nguyen Van Vinh, Yen, Lam Minh, Van E, Phan, Thuong, Nguyen Phong, Van Truc, Nguyen, Trung, Pham Huu, Yap, Wee Chee, Pandey, Rahul, and Yee, Sidney

Subjects

*MEDICAL personnel, *PEPTIDE vaccines, *VIETNAMESE people, *BOOSTER vaccines, *SARS-CoV-2

Abstract

• Abdala COVID-19 vaccine is immunogenic in Vietnamese people. • Antibodies obtained after primary series were comparable with that of ChAdOx1-S. • Antibodies induced by a booster dose cross-neutralize Omicron and SARS-CoV-1. We studied the immunogenicity after primary and booster vaccinations of the Abdala COVID-19 vaccine, a receptor-binding domain protein subunit vaccine, in Vietnamese people by determining the level of neutralization and cross-neutralization activities against the ancestral SARS-CoV-2 and its variants and SARS-CoV-1. We performed a prospective observational study, enrolling adults aged 19-59 years in Dong Thap province, southern Vietnam, and collected blood samples from baseline until 4 weeks after the booster dose. We measured anti-nucleocapsid, anti-spike, and neutralizing antibodies against SARS-CoV-2 and assessed the cross-neutralization against 14 SARS-CoV-2 variants and SARS-CoV-1. Complementary antibody data came from Vietnamese health care workers fully vaccinated with ChAdOx1-S. After primary vaccination, anti-spike antibody and neutralizing antibodies were detectable in 98.4% and 87% of 251 study participants, respectively, with neutralizing antibody titers similar to that induced by ChAdOx1-S vaccine. Antibody responses after a homologous (Abdala COVID-19) or heterologous (messenger RNA BNT162b2) booster could neutralize 14 SARS-CoV-2 variants (including Omicron) and SARS-CoV-1. Abdala COVID-19 vaccine is immunogenic in Vietnamese people. Enhanced antibody response after a booster dose could cross-neutralize 14 SARS-CoV-2 variants and SARS-CoV-1. Our results have added to the growing body of knowledge about the contribution of protein subunit vaccine platforms to pandemic control. [ABSTRACT FROM AUTHOR]

Published

2024

24. 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

25. Immunoprotective efficacy of 3 Klebsiella pneumoniae type I fimbriae proteins in a murine model.

Author

Tong, Xiaofang, Cao, Zhongming, Cheng, Siying, Zhang, Baoling, Li, Xiaoping, Kastelic, John P., Xu, Chuang, Han, Bo, and Gao, Jian

Subjects

*PEPTIDE vaccines, *KLEBSIELLA pneumoniae, *KLEBSIELLA infections, *VACCINE trials, *RECOMBINANT proteins

Abstract

Klebsiella pneumoniae is a primary cause of clinical mastitis in dairy cows, with prevention being crucial, as treatments often fail due to antimicrobial resistance. Recent studies identified type I fimbrial antigens of K. pneumoniae as promising vaccine candidates, but there are limited research data. In this study, 3 fimbriae genes (fimA , fimC and fimG) were cloned and recombinantly expressed in Escherichia coli and their protective efficacy against K. pneumoniae evaluated in a mouse model. All 3 recombinant fimbriae proteins elicited strong humoral immune responses in mice, significantly increasing IgG, IgG1 and IgG2a. Notably, using a model of mice challenged with an intraperitoneal injection of bacteria, FimG significantly reduced bacterial loads in the spleen and lung, whereas FimA and FimC had limited protection for these organs. Either active or passive immunization with FimG produced substantial protective effects in mice challenged with K. pneumoniae LD 100 ; in contrast, the mortality rate in the FimA-immunized group was similar to that of the control group, whereas FimC had weak protection. We concluded that the FimG recombinant protein vaccine had a favorable protective effect, with potential for immunization against K. pneumoniae mastitis. • Three Klebsiella pneumoniae recombinant type I fimbrial protein subunits were purified for vaccine trials. • Immunization of mice with fimbrial protein subunits elicited a strong humoral antibody response. • Immunization with FimG protected against Klebsiella pneumoniae infection. [ABSTRACT FROM AUTHOR]

Published

2024

26. Vaccinomics strategy to design an epitope peptide vaccine against Helicobacter pylori.

Author

Tamjid, Navid, Eskandari, Sedigheh, Karimi, Zeinab, Nezafat, Navid, and Negahdaripour, Manica

Subjects

*PEPTIDES, *HELICOBACTER pylori, *ORAL vaccines, *T cells, *CYTOTOXIC T cells, *PEPTIDE vaccines, *B cells

Abstract

Helicobacter pylori is a Gram-negative bacterium estimated to infect about half of the world's population. The world health organization (WHO) has classified this bacterium in the first line of carcinogen agents; however, the only current strategy to deal with this bacterium is using antibiotics. The increase of antibiotic resistance is alarming. Vaccines could be an advantageous approach to overcome this pathogen. In this study, a multi-epitope oral vaccine was designed against H. pylori using computational approaches. GGT, BabA, HP_1453 proteins were used as antigens for finding epitopes. the two CD8+ cytolytic T lymphocyte (CTL) and seven CD4+ helper T lymphocyte (HTL) and B cell immunodominant epitopes were selected using several servers. Then, they were connected to the adjuvant (U-Omp19), COMP, and M-cell motif by GSGSG, KK and EAAAK linkers. Evaluation of the vaccine construct showed it a non-allergen, immunogen, non-toxic, and stable protein. Docking and MD results indicated its proper interaction with TLR4. Based on the obtained results, the designed vaccine, has acceptable mucosal immunogenicity besides stability in the acidic environment. It can be a proper candidate against H. pylori. However, experimental studies should be performed to confirm its stability, efficacy, and safety. [Display omitted] • Helicobacter pylori is the cunning bacterium, which can lead to gastric cancer if untreated. • The GGT, BabA, HP_1453 antigens were used to select immunodominant epitopes. • U-Omp19 adjuvant, COMP, and M-cell motif and the epitopes were joined using GSGSG, KK, and EAAAK linkers. • Computational structural and immunological studies showed the vaccine is non-allergen, immunogen, non-toxic, and stable. [ABSTRACT FROM AUTHOR]

Published

2022

27. Clinical and Translational Advances in Glioma Immunotherapy.

Author

Bunse, Lukas, Bunse, Theresa, Krämer, Christopher, Chih, Yu-Chan, and Platten, Michael

Abstract

Gliomas are highly treatment refractory against immune checkpoint blockade, an immunotherapeutic modality that revolutionized therapy for many tumors. At the same time, technological innovation has dramatically accelerated the development of immunotherapeutic approaches such as personalized tumor-specific vaccine production, dendritic cell vaccine manufacture, patient-individual target selection and chimeric antigen receptor, and T cell receptor T cell manufacture. Here we review recent clinical and translational advances in glioma immunotherapy with a focus on targets and their cognate immune receptor derivates as well as concepts to improve intratumoral T cell effector functions. [ABSTRACT FROM AUTHOR]

Published

2022

28. A multistage protein subunit vaccine as BCG-booster confers protection against Mycobacterium tuberculosis infection in murine models.

Author

Chen, Zhenyan, Zhang, Ying, Wu, Juan, Xu, Jinchuan, Hu, Zhidong, and Fan, Xiao-Yong

Subjects

*PEPTIDE vaccines, *LATENT tuberculosis, *BOOSTER vaccines, *BCG vaccines, *LATENT infection, *T cells

Abstract

• A recombinant protein subunit vaccine A986 expressing three latency antigens and one early secreted antigen Ag85A was constructed. • A986 adjuvanted with MPL/QS21 induced robust cellular and humoral immune responses in mice. • A986 adjuvanted with MPL/QS21 induced immune protection against Mtb infection in naïve and BCG-primed mice. The eradication of tuberculosis remains a global challenge. Despite being the only licensed vaccine, Bacillus Calmette-Guérin (BCG) confers limited protective efficacy in adults and individuals with latent tuberculosis infections (LTBI). There is an urgent need to develop novel vaccines that can enhance the protective effect of BCG. Protein subunit vaccines have garnered significant research interest due to their safety and plasticity. Based on previous studies, we selected three antigens associated with LTBI (Rv2028c, Rv2029c, Rv3126c) and fused them with an immunodominant antigen Ag85A, resulting in the construction of a multistage protein subunit vaccine named A986. We evaluated the protective effect of recombinant protein A986 adjuvanted with MPL/QS21 as a booster vaccine for BCG against Mycobacterium tuberculosis (Mtb) infection in mice. The A986 + MPL/QS21 induced the secretion of antigen-specific Th1 (IL-2+, IFN-γ+ and TNF-α+) and Th17 (IL-17A+) cytokines in CD4+ and CD8+ T cells within the lung and spleen of mice, while also increased the frequency of central memory and effector memory T cells. Additionally, it also induced the enhanced production of IgG antibodies. Compared to BCG alone, A986 + MPL/QS21 boosting significantly augmented the proliferation of antigen-specific multifunctional T cells and effectively reduced bacterial load in infected mice. Taken together, A986 + MPL/QS21 formulation induced robust antigen-specific immune responses and provided enhanced protection against Mtb infection as a booster of BCG vaccine. [ABSTRACT FROM AUTHOR]

Published

2024

29. 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

30. Vaccination of cattle with a virus vector vaccine against a major membrane protein of Mycobacterium avium subsp. paratuberculosis elicits CD8 cytotoxic T cells that kill intracellular bacteria.

Author

Mahmoud, Asmaa H., Abdellrazeq, Gaber S., Franceschi, Valentina, Schneider, David A., Bannantine, John P., Fry, Lindsay M., Hulubei, Victoria, De Matteis, Giovanna, Park, Kun Taek, Minesso, Sergio, Davis, William C., and Donofrio, Gaetano

Subjects

*CYTOTOXIC T cells, *MYCOBACTERIUM avium paratuberculosis, *PEPTIDE vaccines, *ANTIGEN presenting cells, *VIRAL vaccines, *PARATUBERCULOSIS

Abstract

Analysis of the recall response ex vivo in cattle vaccinated with a Mycobacterium a vium subsp. paratuberculosis (Map) rel deletion mutant revealed the immune response was directed toward a 35 kD major membrane protein (MMP) of Map. Antigen presenting cells (APC) primed with MMP elicited expansion of CD8 cytotoxic memory T cells (CTL) with ability to kill intracellular bacteria. Development of CTL was MHC-restricted. The gene MAP2121c, encoding MMP, was modified for expression of MMP (tPA-MMP-2mut) in a mammalian cell line to explore the potential of developing MMP as a vaccine. Ex vivo stimulation of PBMC, from Map free cattle, with APC primed with tPA-MMP-2mut expressed p35 elicited a primary CD8 CTL response comparable to the recall response elicited with PBMC from cattle vaccinated with either the Maprel deletion mutant or MMP. In the present study, the modified gene for MMP, now referred to as p35NN, was placed into a bovine herpes virus-4 (BoHV4) vector to determine the potential use of BoHV-4AΔTK-p35NN as a peptide-based vaccine. Subcutaneous vaccination of healthy cattle with BoHV-4AΔTK-p35NN elicited a CTL recall response, as detected ex vivo. The results show use of a virus vector is an effective way for delivery of MMP as a vaccine. The immunogenic activity of MMP was not lost when modified for expression in mammalian cells. The next step is to conduct a field trial to determine if presence of an immune response to MMP prevents Map from establishing an infection. • Mycobacterium avium subsp paratuberculosis killed by virus vectored peptide vaccine. • Vaccine elicits cytotoxic T cells that kill Mycobacterium. avium subsp. paratuberculosis. • Virus vectored peptide vaccine for Mycobacterium a. subsp. paratuberculosis. [ABSTRACT FROM AUTHOR]

Published

2024

31. Preparation and immunological activity evaluation of an intranasal protein subunit vaccine against ancestral and mutant SARS-CoV-2 with curdlan sulfate/O-linked quaternized chitosan nanoparticles as carrier and adjuvant.

Author

Chen, Yipan, Wang, Yan, Li, Zuyi, Jiang, Honglei, Pan, Wei, Liu, Minghui, Jiang, Wenjie, Zhang, Xinke, and Wang, Fengshan

Subjects

*PEPTIDE vaccines, *BOOSTER vaccines, *ANTIGEN presenting cells, *CELLULAR immunity, *POLYSACCHARIDES

Abstract

Chitosan and its derivatives are ideal nasal vaccine adjuvant to deliver antigens to immune cells. Previously, we successfully used a chitosan derivative, O -(2-Hydroxyl) propyl-3-trimethyl ammonium chitosan chloride (O -HTCC), and a β-glucan derivative, curdlan sulfate (CS), to prepare a nanoparticle adjuvant CS/ O -HTCC which could deliver ovalbumin to antigen presenting cells (APCs) through nasal inhalation. In this article, we used SARS-CoV-2 spike receptor binding domain (S-RBD) as the antigen and CS/ O -HTCC nanoparticles as the adjuvant to develop a nasal mucosal protein subunit vaccine, CS/S-RBD/ O -HTCC. The humoral immunity, cell-mediated immunity and mucosal immunity induced by vaccines were evaluated. The results showed that CS/S-RBD/ O -HTCC could induce desirable immunization with single or bivalent antigen through nasal inoculation, giving one booster vaccination with mutated S-RBD (beta) could bring about a broad cross reaction with ancestral and different mutated S-RBD, and vaccination of the BALB/c mice with CS/S-RBD/ O -HTCC containing S-RBD mix antigens (ancestral and omicron) could induce the production of binding and neutralizing antibodies against both of the two antigens. Our results indicate that CS/ O -HTCC is a promising nasal mucosal adjuvant to prepare protein subunit vaccine for both primary and booster immunization, and the adjuvant is suitable for loading more than one antigen for preparing multivalent vaccines. [ABSTRACT FROM AUTHOR]

Published

2024

32. Development of nanoparticle vaccines utilizing designed Fc-binding homo-oligomers and RBD-Fc of SARS-CoV-2.

Author

Liang, Yucai, Xiao, Weiling, Peng, Yuan, Zhang, Shengshuo, Dong, Jinhua, Zhao, Jun, Wang, Yuhui, Zhang, Mengtao, Liu, Zhijun, and Yu, Bowen

Subjects

*PEPTIDE vaccines, *VACCINE development, *SARS-CoV-2, *NANOPARTICLES, *COVID-19 vaccines, *OLIGOMERS

Abstract

The Fc-fused receptor binding domain (RBD-Fc) vaccine for SARS-CoV-2 has garnered significant attention for its capacity to provide effective and specific immune protection. However, its immunogenicity is limited, highlighting the need for improvement in clinical application. Nanoparticle delivery has been shown to be an effective method for enhancing antigen immunogenicity. In this study, we developed bivalent nanoparticle recombinant protein vaccines by assembling the RBD-Fc of SARS-CoV-2 and Fc-binding homo-oligomers o42.1 and i52.3 into octahedral and icosahedral nanoparticles. The formation of RBD-Fc nanoparticles was confirmed through structural characterization and cell binding experiments. Compared to RBD-Fc dimers, the nanoparticle vaccines induced more potent neutralizing antibodies (nAb) and stronger cellular immune responses. Therefore, using bivalent nanoparticle vaccines based on RBD-Fc presents a promising vaccination strategy against SARS-CoV-2 and offers a universal approach for enhancing the immunogenicity of Fc fusion protein vaccines. • RBD-Fc based nanoparticle vaccines are assembled using designed Fc-binding homo-oligomers. • RBD-Fc nanoparticle vaccines enhance the humoral and cellular immune response induced by RBD-Fc. • This study provides a feasible method for enhancing the immunogenicity of Fc fusion antigens. [ABSTRACT FROM AUTHOR]

Published

2024

33. A minigene DNA vaccine encoding peptide epitopes derived from Galectin-1 has protective antitumoral effects in a model of neuroblastoma.

Author

Liebscher, Laura, Weißenborn, Christine, Langwisch, Stefanie, Gohlke, Björn-Oliver, Preissner, Robert, Rabinovich, Gabriel A., Christiansen, Nina, Christiansen, Holger, Zenclussen, Ana Claudia, and Fest, Stefan

Subjects

*DNA vaccines, *NEUROBLASTOMA, *EPITOPES, *TUMOR growth, *LECTINS, *CANCER invasiveness, *T cell receptors, *PROTEINS, *RESEARCH, *IMMUNIZATION, *VACCINES, *ANIMAL experimentation, *ANTHROPOMETRY, *RESEARCH methodology, *CELL physiology, *IMMUNOLOGY technique, *EVALUATION research, *PEPTIDE vaccines, *LYMPHOCYTES, *COMPARATIVE studies, *IMMUNITY, *CANCER vaccines, *T cells, *CELL lines, *ANTIGENS, *MICE, *PHARMACODYNAMICS

Abstract

We recently identified Galectin-1 (Gal-1), a β-galactoside-binding lectin, as a novel immune regulator in neuroblastoma (NB). Here, we characterized the tolerogenic function of Gal-1 within the CD8+ T cell compartment and further evaluated its relevance as an antigen for effective DNA vaccination against NB in a mouse model. NB cells with Gal-1 knockdown (NXS-2L) exhibited significantly reduced tumor growth compared to NXS-2 NB cells. Administration of anti-CD8 antibodies prevented this antitumor effect, with primary tumor growth comparable to that from Gal-1 (G1)-sufficient NB cells. Peptide epitope screening with online databases and in silico docking experiments predicted the sequences "FDQADLTI" (#1), "GDFKIKCV" (#2), and "AHGDANTI" (#3) to have superior H2-KK binding affinities and "KFPNRLNM" (#4), "DGDFKIKCV" (#5), and "LGKDSNNL" (#6) to have superior H2-DD binding affinities. Minigenes encoding G1-KK (#1-#2-#3), G1-DD (#4-#5-#6) and the triplet with the highest affinity, G1-H (#1-#2-#4), were generated and cloned into a ubiquitin-containing plasmid (pU). Mice receiving pU-G1-KK or pU-G-1H presented a reduction in the s.c. tumor volume and weight of up to 80% compared to control mice; this reduction was associated with increased cytotoxicity of isolated splenocytes from vaccinated animals. Vaccination with pUG1-DD showed a lower capability to suppress primary tumor progression. In conclusion, Gal-1 expression by NB negatively regulates CD8+ T cells. Vaccination with DNA plasmids encoding Gal-1 epitopes overcomes immune escape, enhances CD8+ T cell-dependent immunity and displays effective antitumor activity against NB. [ABSTRACT FROM AUTHOR]

Published

2021

34. Differential protective impact of peptide vaccine formulae targeting the lung- and liver-stage of challenge Schistosoma mansoni infection in mice.

Author

Tallima, Hatem, Tadros, Menerva M., and El Ridi, Rashika

Subjects

*LUNGS, *PEPTIDE vaccines, *SCHISTOSOMA mansoni, *PEPTIDASE, *IMMUNOLOGIC memory, *PEROXIREDOXINS, WORM eggs

Abstract

• Vaccine comprised gut cysteine peptidases and peroxiredoxin-1-derived peptides. • Vaccine/alum elicited significant reduction in challenge Schistosoma mansoni burden. • Vaccination was associated with tissues worm egg burden similar to control mice. • Increase in lung cytokines and reactive oxygen species content led to larval death. • Increase in lung lipids induced surviving worms to resist liver immune effectors. The study aimed to elicit protective immune responses against murine schistosomiasis mansoni at the parasite lung- and liver stage. Two peptides showing amino acid sequence similarity to gut cysteine peptidases, which induce strong memory immune effectors in the liver, were combined with a peptide based on S. mansoni thioredoxin peroxidase (TPX), a prominent lung-stage schistosomula excretory-secretory product, and alum as adjuvant. Only one of the 2 cysteine peptidases-based peptides in a multiple antigenic peptide construct (MAP-3 and MAP-4) appeared to adjuvant protective immune responses induced by the TPX peptide in a MAP form. Production of TPX MAP-specific IgG1 serum antibodies, and increase in lung interleukin-1 (IL-1), uric acid, and reactive oxygen species (ROS) content were associated with significant (P < 0.05) 50 % reduction in recovery of lung-stage larvae. Increase in lung triglycerides and cholesterol levels appeared to provide the surviving worms with nutrients necessary for a stout double lipid bilayer barrier at the parasite-host interface. Surviving worms-released products elicited memory responses to the MAP-3 immunogen, including production of specific IgG1 antibodies and increase in liver IL-33 and ROS. Reduction in challenge worm burden recorded 45 days post infection did not exceed 48 % associated with no differences in parasite egg counts in the host liver and small intestine compared to unimmunized adjuvant control mice. Alum adjuvant assisted the second peptide, MAP-4, in production of IgG1, IgG2a, IgG2b and IgA specific antibodies and increase in liver ROS, but with no protective potential, raising doubt about the necessity of adjuvant addition. Accordingly, different vaccine formulas containing TPX MAP and 1, 2 or 3 cysteine peptidases-derived peptides with or without alum were used to immunize parallel groups of mice. Compared to unimmunized control mice, significant (P < 0.05 to < 0.005) 22 to 54 % reduction in worm burden was recorded in the different groups associated with insignificant changes in parasite egg output. The results together indicated that a schistosomiasis vaccine able to entirely prevent disease and halt its transmission still remains elusive. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

35. Immune targeting of filarial glutaredoxin through a multi-epitope peptide-based vaccine: A reverse vaccinology approach.

Author

Das, Nabarun Chandra, Gorai, Sampa, Gupta, Parth Sarthi Sen, Panda, Saroj Kumar, Rana, Malay Kumar, and Mukherjee, Suprabhat

Subjects

*GLUTAREDOXIN, *PEPTIDE vaccines, *AMINO acid sequence, *VACCINE immunogenicity, *VACCINES, *IMMUNOGLOBULIN M

Abstract

• Multi-epitope-based peptide vaccine was designed to target W. bancrofti glutaredoxin. • Molecular docking, dynamic simulation, and an examination of conformational changes suggested vaccine complex plays a role in eliciting protective innate immune responses. • Immune-simulation study demonstrated IgG and IgM as crucial contributors in triggering vaccine-induced adaptive responses. • Multi epitope-vaccine was cloned into the pET28a(+) vector for recombinant production, facilitating subsequent experimental validation. Despite the efforts of global programme to eliminate lymphatic filariasis (GPELF), the threat of lymphatic filariasis (LF) still looms over humanity in terms of long-term disabilities, and morbidities across the globe. In light of this situation, investigators have chosen to focus on the development of immunotherapeutics targeting the physiologically important filarial-specific proteins. Glutaredoxin (16.43 kDa) plays a pivotal role in filarial redox biology, serving as a vital contributor. In the context of the intra-host survival of filarial parasites, this antioxidant helps in mitigating the oxidative stress imposed by the host immune system. Given its significant contribution, the development of a vaccine targeting glutaredoxin holds promise as a new avenue for achieving a filaria-free world. Herein, multi-epitope-based vaccine was designed using advanced immunoinformatics approach. Initially, 4B-cell epitopes and 6 T-cell epitopes (4 MHC I and 2 MHC II) were identified from the 146 amino acid long sequence of glutaredoxin of the human filarid, Wuchereria bancrofti. Subsequent clustering of these epitopes with linker peptides finalized the vaccine structure. To boost TLR-mediated innate immunity, TLR-specific adjuvants were incorporated into the designed vaccine. After that, experimental analyses confirm the designed vaccine, Vac4 as anefficient ligand of human TLR5 to elicit protective innate immunity against filarial glutaredoxin. Immune simulation further demonstrated abundant levels of IgG and IgM as crucial contributors in triggering vaccine-induced adaptive responses in the recipients. Hence, to facilitate the validation of immunogenicity of the designed vaccine, Vac4 was cloned in silico in pET28a(+) expression vector for recombinant production. Taken together, our findings suggest that vaccine-mediated targeting of filarial glutaredoxin could be a future option for intervening LF on a global scale. [ABSTRACT FROM AUTHOR]

Published

2024

36. A novel multi-epitope peptide vaccine candidate against prostate cancer: An in silico approach.

Author

Rezaei Arablouydareh, S., Movahedpour, A., and Taheri-Anganeh, M.

Subjects

*PEPTIDE vaccines, *PROSTATE cancer

Published

2024

37. In silico discovery of diagnostic/vaccine candidate antigenic epitopes and a multi-epitope peptide vaccine (NaeVac) design for the brain-eating amoeba Naegleria fowleri causing human meningitis.

Author

Köseoğlu, Ahmet Efe, Özgül, Filiz, Işıksal, Elif Naz, Şeflekçi, Yusuf, Tülümen, Deniz, Özgültekin, Buminhan, Deniz Köseoğlu, Gülsüm, Özyiğit, Sena, Ihlamur, Murat, and Ekenoğlu Merdan, Yağmur

Subjects

*PEPTIDE vaccines, *NAEGLERIA fowleri, *EPITOPES, *AMOEBA, *LIFE cycles (Biology), *GIARDIA lamblia, *ARENAVIRUSES

Abstract

[Display omitted] • After the in silico evaluation of N. fowleri candidate proteins, three prominent diagnostic/vaccine candidate epitopes with the highest antigenicities were discovered. • A potentially highly immunogenic/antigenic multi-epitope peptide vaccine (NaeVac) was designed. • Our findings contain important up-to-date data for diagnostic and vaccine development in case N. fowleri becomes an emerging pathogen. Naegleria fowleri , the brain-eating amoeba, is a free-living amoeboflagellate with three different life cycles (trophozoite, flagellated, and cyst) that lives in a variety of habitats around the world including warm freshwater and soil. It causes a disease called naegleriasis leading meningitis and primary amoebic meningoencephalitis (PAM) in humans. N. fowleri is transmitted through contaminated water sources such as insufficiently chlorinated swimming pool water or contaminated tap water, and swimmers are at risk. N. fowleri is found all over the world, and most infections were reported in both developed and developing countries with high mortality rates and serious clinical findings. Until now, there is no FDA approved vaccine and early diagnosis is urgent against this pathogen. In this study, by analyzing the N. fowleri vaccine candidate proteins (Mp2CL5, Nfa1, Nf314, proNP-A and proNP-B), it was aimed to discover diagnostic/vaccine candidate epitopes and to design a multi-epitope peptide vaccine against this pathogen. After the in silico evaluation, three prominent diagnostic/vaccine candidate epitopes (EAKDSK, LLPHIRILVY, and FYAKLLPHIRILVYS) with the highest antigenicities were discovered and a potentially highly immunogenic/antigenic multi-epitope peptide vaccine (NaeVac) was designed against the brain-eating amoeba N. fowleri causing human meningitis. [ABSTRACT FROM AUTHOR]

Published

2024

38. Ag85B-ENO146-82 therapeutic vaccines enhance anti-tumor immunity by inducing CD8+ T cells and remodeling tumor microenvironment.

Author

Liu, Fengjun, Huang, Huan, Yang, Xiaoli, Jiang, Shasha, Xu, Aotian, Yu, Zhongjie, Li, Jun, Yu, Meng, Wang, Yunyang, and Wang, Bin

Subjects

*T cells, *TUMOR microenvironment, *PEPTIDE vaccines, *CD8 antigen, *IMMUNITY, *CANCER vaccines

Abstract

• The growth of tumor was inhibited by Ag85B-ENO1 46-82. • Ag85B-ENO1 46-82 was beneficial for anti-tumor immune responses in the TME. • The CD8 + T cell immune responses were indispensable for the therapeutic effect of Ag85B-ENO1 46-82. Lung cancer is the leading cause of cancer-related morbidity and mortality in China. However, the effect of traditional cancer treatment is limited. Herein, we designed a therapeutic cancer vaccine based on the tumor-associated antigen mENO1, which can prevent lung cancer growth in vivo, and explored the underlying mechanism of Ag85B-ENO1 46-82 therapy. Lewis lung carcinoma (LLC) tumor-bearing immunocompetent C57BL/6 mice that received Ag85B-ENO1 46-82 treatment showed antitumor effect. Further, we detected CD8+ T, CD4+ T in LLC-bearing C57BL/6 mice to understand the impact of Ag85B-ENO1 46-82 therapy on antitumor capacity. The Ag85B-ENO1 46-82 therapy induced intensive infiltration of CD4+ and CD8+ T cells in tumors, increased tumor-specific IFN-γ and TNF-α secretion by CD8+ T cells and promoted macrophage polarization toward M1 phenotype. Flow cytometric analysis revealed that CD8+ T effector memory (TEM) cells and central memory (TCM) cells were upregulated. qPCR and ELISA analysis showed that the expression of IFN-γ and TNF-α were upregulated, whereas of IL1β, IL6 and IL10 were downregulated. This study demonstrated that Ag85B-ENO1 46-82 vaccine augmented antitumor efficacy, which was CD8+ T cells dependent. Our findings paved the way for therapeutic tumor-associated antigen peptide vaccines to enhance anti-tumor immunotherapy for treatment of cancer. [ABSTRACT FROM AUTHOR]

Published

2024

39. Fourth dose of microneedle array patch of SARS-CoV-2 S1 protein subunit vaccine elicits robust long-lasting humoral responses in mice.

Author

Kim, Eun, Shin, Juyeop, Ferrari, Alessandro, Huang, Shaohua, An, Eunjin, Han, Donghoon, Khan, Muhammad S., Kenniston, Thomas W., Cassaniti, Irene, Baldanti, Fausto, Jeong, Dohyeon, and Gambotto, Andrea

Subjects

*PEPTIDE vaccines, *HUMORAL immunity, *SARS-CoV-2 Delta variant, *SARS-CoV-2 Omicron variant, *BOOSTER vaccines

Abstract

• Assessment of SARS-CoV2 vaccination efficacy of four prime-boost doses. • A vaccine delivery platform that is cost-effective, user-friendly and safe. • Broad SARS-CoV-2 neutralizing antibodies response by heterologous booster vaccination. • Sustained immune response persisting until the end of the mice's lifespan. The COVID-19 pandemic has underscored the pressing need for safe and effective booster vaccines, particularly in considering the emergence of new SARS-CoV-2 variants and addressing vaccine distribution inequalities. Dissolving microneedle array patches (MAP) offer a promising delivery method, enhancing immunogenicity and improving accessibility through the skin's immune potential. In this study, we evaluated a microneedle array patch-based S1 subunit protein COVID-19 vaccine candidate, which comprised a bivalent formulation targeting the Wuhan and Beta variant alongside a monovalent Delta variant spike proteins in a murine model. Notably, the second boost of homologous bivalent MAP-S1(WU + Beta) induced a 15.7-fold increase in IgG endpoint titer, while the third boost of heterologous MAP-S1RS09Delta yielded a more modest 1.6-fold increase. Importantly, this study demonstrated that the administration of four doses of the MAP vaccine induced robust and long-lasting immune responses, persisting for at least 80 weeks. These immune responses encompassed various IgG isotypes and remained statistically significant for one year. Furthermore, neutralizing antibodies against multiple SARS-CoV-2 variants were generated, with comparable responses observed against the Omicron variant. Overall, these findings emphasize the potential of MAP-based vaccines as a promising strategy to combat the evolving landscape of COVID-19 and to deliver a safe and effective booster vaccine worldwide. [ABSTRACT FROM AUTHOR]

Published

2024

40. Peptide nanovaccine in melanoma immunotherapy.

Author

Dehghankhold, Mahvash, Sadat Abolmaali, Samira, Nezafat, Navid, and Mohammad Tamaddon, Ali

Subjects

*TUMOR antigens, *PEPTIDES, *PEPTIDE vaccines, *MELANOMA, *CANCER vaccines, *NANOCARRIERS

Abstract

[Display omitted] • Melanoma is a fatal neoplasm resistant to traditional treatment. • Recently peptide vaccine has obtained remarkable attention in treatment of melanoma. • Nanoparticles can incite a strong immunity to peptide-based melanoma vaccines. Melanoma is an especially fatal neoplasm resistant to traditional treatment. The advancement of novel therapeutical approaches has gained attention in recent years by shedding light on the molecular mechanisms of melanoma tumorigenesis and their powerful interplay with the immune system. The presence of many mutations in melanoma cells results in the production of a varied array of antigens. These antigens can be recognized by the immune system, thereby enabling it to distinguish between tumors and healthy cells. In the context of peptide cancer vaccines, generally, they are designed based on tumor antigens that stimulate immunity through antigen-presenting cells (APCs). As naked peptides often have low potential in eliciting a desirable immune reaction, immunization with such compounds usually necessitates adjuvants and nanocarriers. Actually, nanoparticles (NPs) can provide a robust immune response to peptide-based melanoma vaccines. They improve the directing of peptide vaccines to APCs and induce the secretion of cytokines to get maximum immune response. This review provides an overview of the current knowledge of the utilization of nanotechnology in peptide vaccines emphasizing melanoma, as well as highlights the significance of physicochemical properties in determining the fate of these nanovaccines in vivo, including their drainage to lymph nodes, cellular uptake, and influence on immune responses. [ABSTRACT FROM AUTHOR]

Published

2024

41. Oropouche virus: A neglected global arboviral threat.

Author

Zhang, Yuli, Liu, Xiao, Wu, Zhen, Feng, Shuo, Lu, Ke, Zhu, Wenbing, Sun, Hengyi, and Niu, Guoyu

Subjects

*PEPTIDE vaccines, *ANIMAL migration, *THERAPEUTICS, *CERATOPOGONIDAE, *VACCINE development, *SCHMALLENBERG virus, *BUNYAVIRUSES

Abstract

• According to the latest ICTV 2023 publication, oropouche virus (OROV) is a member of bunyavirales order, peribunyaviridae family, orthobunyavirus geneus, the orthobunyavirus oropoucheense species. • The history of the epidemiological development of fever suggests that, given the global nature of environmental and climate change and the widespread migration of animals and humans, OROV is likely to expand beyond south america in the near future. • The proteins encoded by the different segments enables OROV to replicate efficiently in the host and to resist the host's immune response. • Phylogenetic analyses showed that OROV sequences are geographically distinct and have closer homologies with iquitos virus and perdoes virus. • Recent studies have utilised immunoinformatics approaches to develop epitope-based peptide vaccines against OROV. The Oropouche virus is an important arthropod-borne virus in the Peribunyaviridae family that can cause febrile illnesses, and it is widely distributed in tropical regions such as Central and South America. Since the virus was first identified, a large number of related cases are reported every year. No deaths have been reported to date, however, the virus can cause systemic infections, including the nervous and blood systems, leading to serious complications. The transmission of Oropouche virus occurs through both urban and sylvatic cycles, with the anthropophilic biting midge Culicoides paraensis serving as the primary vector in urban areas. Direct human-to-human transmission of Oropouche virus has not been observed. Oropouche virus consists of three segments, and the proteins encoded by the different segments enables the virus to replicate efficiently in the host and to resist the host's immune response. Phylogenetic analyses showed that Oropouche virus sequences are geographically distinct and have closer homologies with Iquitos virus and Perdoes virus, which belong to the family Peribunyaviridae. Despite the enormous threat it poses to public health, there are currently no licensed vaccines or specific antiviral treatments for the disease it causes. Recent studies have utilised imJatobal virusmunoinformatics approaches to develop epitope-based peptide vaccines, which have laid the groundwork for the clinical use of vaccines. The present review focuses on the structure, epidemiology, immunity and phylogeny of Oropouche virus, as well as the progress of vaccine development, thereby attracting wider attention and research, particularly with regard to potential vaccine programs. [ABSTRACT FROM AUTHOR]

Published

2024

42. Advances and prospects of mRNA vaccines in cancer immunotherapy.

Author

Liu, Yixuan, Yan, Qijia, Zeng, Zhaoyang, Fan, Chunmei, and Xiong, Wei

Subjects

*CANCER vaccines, *PEPTIDE vaccines, *PEPTIDE nucleic acids, *DNA vaccines, *VIRAL vaccines, *GENITAL warts

Abstract

Cancer vaccines, designed to activate the body's own immune system to fight against tumors, are a current trend in cancer treatment and receiving increasing attention. Cancer vaccines mainly include oncolytic virus vaccine, cell vaccine, peptide vaccine and nucleic acid vaccine. Over the course of decades of research, oncolytic virus vaccine T-VEC, cellular vaccine sipuleucel-T, various peptide vaccines, and DNA vaccine against HPV positive cervical cancer have brought encouraging results for cancer therapy, but are losing momentum in development due to their respective shortcomings. In contrast, the advantages of mRNA vaccines such as high safety, ease of production, and unmatched efficacy are on full display. In addition, advances in technology such as pseudouridine modification have cracked down the bottleneck for developing mRNA vaccines including instability, innate immunogenicity, and low efficiency of in vivo delivery. Several cancer mRNA vaccines have achieved promising results in clinical trials, and their usage in conjunction with other immune checkpoint inhibitors (ICIs) has further boosted the efficiency of anti-tumor immune response. We expect a rapid development of mRNA vaccines for cancer immunotherapy in the near future. This review provides a brief overview of the current status of mRNA vaccines, highlights the action mechanism of cancer mRNA vaccines, their recent advances in clinical trials, and prospects for their clinical applications. [ABSTRACT FROM AUTHOR]

Published

2024

43. Biophysical and biochemical characterization of a recombinant Lyme disease vaccine antigen, CspZ-YA.

Author

Chen, Yi-Lin, Lee, Jungsoon, Liu, Zhuyun, Strych, Ulrich, Bottazzi, Maria Elena, Lin, Yi-Pin, and Chen, Wen-Hsiang

Subjects

*LYME disease vaccines, *PEPTIDE vaccines, *ESCHERICHIA coli, *LYME disease, *VACCINE development

Abstract

Lyme disease, caused by Lyme Borrelia spirochetes, is the most common vector-borne illness in the United States. Despite its global significance, with an estimated 14.5 % seroprevalence, there is currently no licensed vaccine. Previously, we demonstrated that CspZ-YA protein conferred protection against Lyme Borrelia infection, making it a promising vaccine candidate. However, such a protein was tagged with hexahistidine, and thus not preferred for vaccine development; furthermore, the formulation to stabilize the protein was understudied. In this work, we developed a two-step purification process for tag-free E. coli -expressed recombinant CspZ-YA. We further utilized various bioassays to analyze the protein and determine the suitable buffer system for long-term storage and formulation as a vaccine immunogen. The results indicated that a buffer with a pH between 6.5 and 8.5 stabilized CspZ-YA by reducing its surface hydrophobicity and colloidal interactions. Additionally, low pH values induced a change in local spatial conformation and resulted in a decrease in α-helix content. Lastly, an optimal salinity of 22–400 mM at pH 7.5 was found to be important for its stability. Collectively, this study provides a fundamental biochemical and biophysical understanding and insights into the ideal stabilizing conditions to produce CspZ-YA recombinant protein for use in vaccine formulation and development. [ABSTRACT FROM AUTHOR]

Published

2024

44. Design, development, and assessment of a novel multi-peptide vaccine targeting PspC, PsaA, and PhtD proteins of Streptococcus pneumoniae.

Author

Bahadori, Zohreh, Shafaghi, Mona, Sabzevari, Jahangir, Madanchi, Hamid, Ranjbar, Mohammad Mehdi, Mousavi, Seyed Fazlollah, and Shabani, Ali Akbar

Subjects

*PEPTIDE vaccines, *STREPTOCOCCUS pneumoniae, *CHIMERIC proteins, *PNEUMOCOCCAL vaccines, *PROTEINS

Abstract

Pneumococcus is the top cause of diseases such as pneumonia/meningitis, and of secondary infections after viral respiratory diseases like COVID-19/flu. Pneumococcal protein-based vaccines consisting of proteins with various functions in virulence might provide a qualified alternative for present vaccines. In this project, PspC, PsaA, and PhtD proteins were considered to anticipate B/T-cell epitopes using immunoinformatics to develop 4 multi-peptide constructs (C, A, and D individual constructs, and a fusion construct CAD). We tested whether vaccination with CAD is able to elicit more efficient protective responses against infection than vaccination with the individual constructs or combination of C + A + D. Based on the in silico results, the constructs were predicted to be antigenic, soluble, non-toxic, and stable, and also be able to provoke humoral/cellular immune reactions. When mice were immunized with the fusion protein, significantly higher levels of IgG and cytokines were induced in serum. The IgG in the fusion group had an effective bioactivity for pneumococcus clearance utilizing the complement pathway. The mice immunized with fusion protein were the most protected from challenge. This report for the first time presents a novel multi-peptide vaccine composed of immunodominant peptides of PspC, PsaA, and PhtD. In general, the experimental results supported the immunoinformatics predictions. [ABSTRACT FROM AUTHOR]

Published

2024

45. Recombinant bacteriophage T4 displaying key epitopes of the foot-and-mouth disease virus as a novel nanoparticle vaccine.

Author

Chen, Cen, Zhang, Nan, Li, Mengling, Guo, Aili, Zheng, Yifei, Humak, Farwa, Qian, Ping, and Tao, Pan

Subjects

*VIRUS diseases, *FOOT & mouth disease, *BACTERIOPHAGE T4, *PEPTIDE vaccines, *NANOPARTICLES, *BACTERIOPHAGES

Abstract

Foot-and-mouth disease virus (FMDV) is a highly contagious pathogen that has caused significant economic losses in the livestock industry. Peptide vaccines engineered with the protective epitopes of FMDV have provided a safer alternative for disease prevention than the traditional inactivated vaccines. However, the immunogenicity of the peptide is usually poor and therefore an adjuvant is required. Here, we showed that recombinant T4 phages displaying the B-cell epitope of the FMDV VP1 protein (VP1 130–158), without additional adjuvants, induced similar levels of antigen-specific IgG1 but higher levels of IgG2a compared to the peptide vaccine. Incorporation of a CD4+ T cell epitope, either 3A 21–35 of FMDV 3A protein or P2 830–844 of tetanus toxoid, further enhanced the immunogenicity of VP1-T4 phage nanoparticles. Interestingly, the extrinsic adjuvant cannot enhance the immunogenicity of the nanoparticles, indicating the intrinsic adjuvant activities of T4 phage. Furthermore, the recombinant T4 phage can be produced on a large scale within a short period of time at a relatively low-cost using Escherichia coli , heralding its potential in the development of a safe and effective FMDV vaccine. [ABSTRACT FROM AUTHOR]

Published

2024

46. Novel toxin-based mRNA vaccine against Clostridium perfringens using in silico approaches.

Author

Asadollahi, Parisa and Kalani, Behrooz Sadeghi

Subjects

*CLOSTRIDIUM perfringens, *CYTOTOXIC T cells, *PEPTIDE vaccines, *T cells, *TOLL-like receptors, *VACCINES

Abstract

Clostridium perfringens is a bacterium that causes gastrointestinal diseases in humans and animals. The several powerful toxins such as alpha toxin (CPA), beta toxin (CPB), enterotoxin (CPE), Epsilon toxin (ETX), and theta toxin, play a major role in its pathogenesis. Traditional vaccine development methods are time-consuming and costly. In silico approaches offer an alternative strategy for designing vaccines by analyzing biological data and predicting immunogenic peptides. In this study, computational tools were utilized to design a RNA vaccine targeting C. perfringens toxins. Toxin protein sequences were retrieved and their linear B-cell, MHCI, and MHCII binding epitopes were predicted. Allergenicity, toxigenicity, and IFN-γ induction were assessed to select non-allergenic, non-toxic, and IFN-γ-inducing epitopes. Molecular docking was performed to identify epitopes that fit within the binding cleft of MHC alleles. A final peptide vaccine construct was designed with selected epitopes separated by a linker sequence. The antigenicity and physicochemical properties of the vaccine were evaluated. Immune response simulation showed enhanced secondary and tertiary immune responses, increased levels of immunoglobulins, cytotoxic T lymphocytes, helper T lymphocytes, macrophage activity, and elevated levels IFN-γ and interleukin-2. Docking analysis was done to assess interactions between the vaccine structure and Toll-like receptors. Codon optimization was performed, and a final RNA vaccine construct was designed. The secondary structure of the RNA vaccine was predicted and validated. Overall, this study demonstrates the potential of in silico approaches for designing an RNA vaccine against C. perfringens toxins, contributing to improved prevention and control of associated diseases. [Display omitted] • The several powerful toxins play major role in Clostridium perfringens pathogenesis. • In this study, computational tools were utilized to design an RNA vaccine targeting Clostridium perfringens toxins. • B-cell and T-cell binding epitopes were predicted. The biological properties of the epitopes were evaluated. • Docking analysis was done to assess interactions between the vaccine structure and Toll-like receptors. • Immune response simulation showed enhanced secondary and tertiary immune responses. [ABSTRACT FROM AUTHOR]

Published

2024

47. Liposome-based peptide vaccines to elicit immune responses against the membrane active domains of the HIV-1 Env glycoprotein.

Author

Rujas, Edurne, Apellániz, Beatriz, Torralba, Johana, Andreu, David, Caaveiro, Jose M.M., Wang, Shixia, Lu, Shan, and Nieva, Jose L.

Subjects

*PEPTIDES, *IMMUNE response, *HYDROPHOBIC surfaces, *HIV, *PEPTIDE vaccines, *VIRAL envelope proteins, *MEMBRANE lipids

Abstract

The fusion peptide (FP) and the Trp-rich membrane proximal external region (MPER) display membrane activity during HIV-1 fusion. These domains are highly conserved in the envelope glycoprotein (Env) and, consequently, antibodies targeting these regions block entry of divergent HIV strains and isolates into target cells. With the aim of recovering concurrent responses against the membrane-active Env domains, we have produced hybrid peptides that connect FP and MPER sequences via flexible aminohexanoic acid tethers, and tested their potential as immunogens. We demonstrate that liposome-based formulations containing FP-MPER hybrid peptides could elicit in rabbits, antibodies with the binding sequence specificity of neutralizing antibodies that engage with the N-terminal MPER sub-region. Determination of the thermodynamic parameters of binding using the Fab 2F5 as an N-terminal MPER antibody model, revealed that the hydrophobic interaction surface for epitope engagement appears to be optimal in the FP-MPER hybrid. In general, our data support: i) the use of liposomes as carriers for membrane active peptides; ii) the capacity of these liposome-based vaccines to focus humoral responses to N-terminal MPER epitopes; and iii) the need to include lipid membranes in immunogens to elicit such specific responses. • Liposomes containing FP-MPER hybrid peptides have been tested as HIV immunogens. • These vaccines are useful to focus humoral responses to N-terminal MPER epitopes. • Lipid membranes are necessary to elicit 2F5-like responses. [ABSTRACT FROM AUTHOR]

Published

2024

48. Immunotherapy for High-Grade Gliomas: A Clinical Update and Practical Considerations for Neurosurgeons.

Author

Young, Jacob S., Dayani, Fara, Morshed, Ramin A., Okada, Hideho, and Aghi, Manish K.

Subjects

*GLIOMAS, *IMMUNOTHERAPY, *NEUROSURGEONS, *BRAIN tumors, *DENDRITIC cells

Abstract

Background The current standard of care for patients with high-grade gliomas includes surgical resection, chemotherapy, and radiation; but even still most patients experience disease progression and succumb to their illness within a few years of diagnosis. Immunotherapy, which stimulates an anti-tumor immune response, has been revolutionary in the treatment of some hematologic and solid malignancies, generating substantial excitement for its potential for patients with glioblastoma. However, to date, the preclinical success of these approaches against high-grade glioma models has not been replicated in human clinical trials. Moreover, the complex response to these biologically active treatments can complicate management decisions, and the neurosurgical oncology community needs to be actively involved in and up to date on the use of these agents in patients with high-grade glioma. In this review, we discuss the challenges immunotherapy faces for high-grade gliomas, the completed and ongoing clinical trials for the major immunotherapies, and the nuances in management for patients being actively treated with one of these agents. Methods We reviewed the literature to summarize the current immunotherapy strategies for high-grade gliomas. Results Preclinical and clinical trials investigating dendritic cell and peptide vaccines, checkpoint inhibitors, and adoptive T cell therapy are highlighted in this review. Conclusions Although immunotherapy has yet to fully fulfill its promise for patients with glioblastoma and improve patient outcomes, there is still excitement that these approaches will eventually lead to durable anti-tumor responses. As neurosurgeons, an understanding of the complex interactions between the standard of care therapies and the other medications used in the treatment arsenal for patients with high-grade brain tumors is crucial to the management of these patients. [ABSTRACT FROM AUTHOR]

Published

2019

49. Immunoinformatics-based potential multi-peptide vaccine designing against Jamestown Canyon Virus (JCV) capable of eliciting cellular and humoral immune responses.

Author

Shahab, Muhammad, Aiman, Sara, Alshammari, Abdulrahman, Alasmari, Abdullah F., Alharbi, Metab, Khan, Abbas, Wei, Dong-Qing, and Zheng, Guojun

Subjects

*MEDICAL informatics, *TROPICAL medicine, *TORTICOLLIS, *MOLECULAR dynamics, *AMINO acid sequence, *PEPTIDE vaccines

Abstract

Jamestown Canyon virus (JCV) is a deadly viral infection transmitted by various mosquito species. This mosquito-borne virus belongs to Bunyaviridae family, posing a high public health threat in the in tropical regions of the United States causing encephalitis in humans. Common symptoms of JCV include fever, headache, stiff neck, photophobia, nausea, vomiting, and seizures. Despite the availability of resources, there is currently no vaccine or drug available to combat JCV. The purpose of this study was to develop an epitope-based vaccine using immunoinformatics approaches. The vaccine aimed to be secure, efficient, bio-compatible, and capable of stimulating both innate and adaptive immune responses. In this study, the protein sequence of JCV was obtained from the NCBI database. Various bioinformatics methods, including toxicity evaluation, antigenicity testing, conservancy analysis, and allergenicity assessment were utilized to identify the most promising epitopes. Suitable linkers and adjuvant sequences were used in the design of vaccine construct. 50s ribosomal protein sequence was used as an adjuvant at the N-terminus of the construct. A total of 5 CTL, 5 HTL, and 5 linear B cell epitopes were selected based on non-allergenicity, immunological potential, and antigenicity scores to design a highly immunogenic multi-peptide vaccine construct. Strong interactions between the proposed vaccine and human immune receptors, i.e., TLR-2 and TLR-4, were revealed in a docking study using ClusPro software, suggesting their possible relevance in the immunological response to the vaccine. Immunological and physicochemical properties assessment ensured that the proposed vaccine demonstrated high immunogenicity, solubility and thermostability. Molecular dynamics simulations confirmed the strong binding affinities, as well as dynamic and structural stability of the proposed vaccine. Immune simulation suggest that the vaccine has the potential to effectively stimulate cellular and humoral immune responses to combat JCV infection. Experimental and clinical assays are required to validate the results of this study. [ABSTRACT FROM AUTHOR]

Published

2023

50. Improving the efficacy of peptide vaccines in cancer immunotherapy.

Author

Zahedipour, Fatemeh, Jamialahmadi, Khadijeh, Zamani, Parvin, and Reza Jaafari, Mahmoud

Subjects

*CANCER vaccines, *VACCINE effectiveness, *VACCINE trials, *IMMUNOLOGIC memory, *ANTIGEN presentation

Abstract

• Peptide vaccines are able to elicit an immune response against cancer cells by presenting specific antigens to the immune system. • Although, the peptide vaccines have several advantages, including their specificity for cancer cells, potential for long-term immune memory, ease of production and scale up, and minimal toxicity the efficacy of peptide vaccines in clinical trials has been modest and faces some challenges. • The limited success of peptide vaccines in cancer immunotherapy can be attributed to several factors, including poor antigen presentation, low immunogenicity, and immune evasion by cancer cells. • There are several strategies to overcome these challenges and improve the efficacy of peptide vaccines such the design of more potent peptides, using adjuvants and TLRs agonists, optimization of vaccine delivery, and combination therapies with other immunotherapies or chemotherapies that are comprehensively discussed in this review. Peptide vaccines have shown great potential in cancer immunotherapy by targeting tumor antigens and activating the patient's immune system to mount a specific response against cancer cells. However, the efficacy of peptide vaccines in inducing a sustained immune response and achieving clinical benefit remains a major challenge. In this review, we discuss the current status of peptide vaccines in cancer immunotherapy and strategies to improve their efficacy. We summarize the recent advancements in the development of peptide vaccines in pre-clinical and clinical settings, including the use of novel adjuvants, neoantigens, nano-delivery systems, and combination therapies. We also highlight the importance of personalized cancer vaccines, which consider the unique genetic and immunological profiles of individual patients. We also discuss the strategies to enhance the immunogenicity of peptide vaccines such as multivalent peptides, conjugated peptides, fusion proteins, and self-assembled peptides. Although, peptide vaccines alone are weak immunogens, combining peptide vaccines with other immunotherapeutic approaches and developing novel approaches such as personalized vaccines can be promising methods to significantly enhance their efficacy and improve the clinical outcomes for cancer patients. [ABSTRACT FROM AUTHOR]

Published

2023