Your search keyword '"multiepitope"' showing total 43 results

1. Evaluation of the Safety and Immunogenicity of a Multiple Epitope Polypeptide from Canine Distemper Virus (CDV) in Mice.

Author

Rendon-Marin, Santiago, Rincón-Tabares, Daniel-Santiago, Tabares-Guevara, Jorge H., Arbeláez, Natalia, Forero-Duarte, Jorge E., Díaz, Francisco J., Robledo, Sara M., Hernandez, Juan C., and Ruiz-Saenz, Julian

Subjects

CANINE distemper virus, DOGS, COMMUNICABLE diseases, DOMESTIC animals, T cells

Abstract

Background: Morbillivirus canis is the etiological agent of a highly contagious disease that affects diverse domestic and wild animals. Vaccination is considered the most suitable strategy for controlling CDV dissemination, transmission, and distemper disease. However, the emergence of new CDV strains has led to the need to update the current vaccine strategies employed to prevent CDV infection in domestic and wild animals. Currently, there is a lack of effective alternatives for wild animals. Diverse computational tools, especially peptide-based therapies, enable the development of new universal vaccines. Objective: The aim of this study was to evaluate the safety and humoral and cellular immune response of a new generation of vaccines based on CDV peptides as single-peptide mixtures or multiepitope CDV polypeptides in mice. Methods: Twenty-four BALB/c mice were subjected to a three-dose regimen for 28 days. Seroconversion was evaluated via ELISA, and cellular immune responses were evaluated via flow cytometry through activation-induced markers (AIMs). Results: Compared with the placebo, the peptide mixture and multiepitope CDV polypeptide were safe, and seroconversion was statistically significant in the multiepitope CDV polypeptide and commercial vaccine (CV) groups. The numbers of antigen-specific CD4+CD134+ and IFN-γ+ T cells, CD8+ T cells and TNF-α- and IL-6-producing cells were greater in the mice immunized with the multiepitope CDV polypeptide than in the control mice. Conclusion: This combined approach represents a potential step forward in developing new immunization candidates or enhancing current commercial vaccines to control CDV disease in domestic dogs and wild animals. [ABSTRACT FROM AUTHOR]

Published

2024

2. Designing a Conserved Immunogenic Peptide Construct from the Nucleocapsid Protein of Puumala orthohantavirus.

Author

Sehgal, Ayushi, Sharma, Diksha, Kaushal, Neha, Gupta, Yogita, Martynova, Ekaterina, Kabwe, Emmanuel, Chandy, Sara, Rizvanov, Albert, Khaiboullina, Svetlana, and Baranwal, Manoj

Subjects

*HEMORRHAGIC fever with renal syndrome, *PEPTIDES, *MOLECULAR docking, *B cells, *DATABASES

Abstract

Puumala orthohantavirus (PUUV) is an emerging zoonotic virus endemic to Europe and Russia that causes nephropathia epidemica, a mild form of hemorrhagic fever with renal syndrome (HFRS). There are limited options for treatment and diagnosis of orthohantavirus infection, making the search for potential immunogenic candidates crucial. In the present work, various bioinformatics tools were employed to design conserved immunogenic peptides containing multiple epitopes of PUUV nucleocapsid protein. Eleven conserved peptides (90% conservancy) of the PUUV nucleocapsid protein were identified. Three conserved peptides containing multiple T and B cell epitopes were selected using a consensus epitope prediction algorithm. Molecular docking using the HPEP dock server demonstrated strong binding interactions between the epitopes and HLA molecules (ten alleles for each class I and II HLA). Moreover, an analysis of population coverage using the IEDB database revealed that the identified peptides have over 90% average population coverage across six continents. Molecular docking and simulation analysis reveal a stable interaction with peptide constructs of chosen immunogenic peptides and Toll-like receptor-4. These computational analyses demonstrate selected peptides' immunogenic potential, which needs to be validated in different experimental systems. [ABSTRACT FROM AUTHOR]

Published

2024

3. Evaluation of the Safety and Immunogenicity of a Multiple Epitope Polypeptide from Canine Distemper Virus (CDV) in Mice

Author

Santiago Rendon-Marin, Daniel-Santiago Rincón-Tabares, Jorge H. Tabares-Guevara, Natalia Arbeláez, Jorge E. Forero-Duarte, Francisco J. Díaz, Sara M. Robledo, Juan C. Hernandez, and Julian Ruiz-Saenz

Subjects

multiepitope, vaccination, domestic dogs, canine distemper virus, immune response, safety, Medicine

Abstract

Background: Morbillivirus canis is the etiological agent of a highly contagious disease that affects diverse domestic and wild animals. Vaccination is considered the most suitable strategy for controlling CDV dissemination, transmission, and distemper disease. However, the emergence of new CDV strains has led to the need to update the current vaccine strategies employed to prevent CDV infection in domestic and wild animals. Currently, there is a lack of effective alternatives for wild animals. Diverse computational tools, especially peptide-based therapies, enable the development of new universal vaccines. Objective: The aim of this study was to evaluate the safety and humoral and cellular immune response of a new generation of vaccines based on CDV peptides as single-peptide mixtures or multiepitope CDV polypeptides in mice. Methods: Twenty-four BALB/c mice were subjected to a three-dose regimen for 28 days. Seroconversion was evaluated via ELISA, and cellular immune responses were evaluated via flow cytometry through activation-induced markers (AIMs). Results: Compared with the placebo, the peptide mixture and multiepitope CDV polypeptide were safe, and seroconversion was statistically significant in the multiepitope CDV polypeptide and commercial vaccine (CV) groups. The numbers of antigen-specific CD4+CD134+ and IFN-γ+ T cells, CD8+ T cells and TNF-α- and IL-6-producing cells were greater in the mice immunized with the multiepitope CDV polypeptide than in the control mice. Conclusion: This combined approach represents a potential step forward in developing new immunization candidates or enhancing current commercial vaccines to control CDV disease in domestic dogs and wild animals.

Published

2024

4. Designing a Conserved Immunogenic Peptide Construct from the Nucleocapsid Protein of Puumala orthohantavirus

Author

Ayushi Sehgal, Diksha Sharma, Neha Kaushal, Yogita Gupta, Ekaterina Martynova, Emmanuel Kabwe, Sara Chandy, Albert Rizvanov, Svetlana Khaiboullina, and Manoj Baranwal

Subjects

orthohantavirus, hemorrhagic fever with renal syndrome (HFRS), Nucleocapsid protein, Multiepitope, HLA-peptide interactions, Microbiology, QR1-502

Abstract

Puumala orthohantavirus (PUUV) is an emerging zoonotic virus endemic to Europe and Russia that causes nephropathia epidemica, a mild form of hemorrhagic fever with renal syndrome (HFRS). There are limited options for treatment and diagnosis of orthohantavirus infection, making the search for potential immunogenic candidates crucial. In the present work, various bioinformatics tools were employed to design conserved immunogenic peptides containing multiple epitopes of PUUV nucleocapsid protein. Eleven conserved peptides (90% conservancy) of the PUUV nucleocapsid protein were identified. Three conserved peptides containing multiple T and B cell epitopes were selected using a consensus epitope prediction algorithm. Molecular docking using the HPEP dock server demonstrated strong binding interactions between the epitopes and HLA molecules (ten alleles for each class I and II HLA). Moreover, an analysis of population coverage using the IEDB database revealed that the identified peptides have over 90% average population coverage across six continents. Molecular docking and simulation analysis reveal a stable interaction with peptide constructs of chosen immunogenic peptides and Toll-like receptor-4. These computational analyses demonstrate selected peptides’ immunogenic potential, which needs to be validated in different experimental systems.

Published

2024

5. In silico designing of multiepitope-based-peptide (MBP) vaccine against MAPK protein express for Alzheimer's disease in Zebrafish

Author

Yasir Arfat, Imran Zafar, Sheikh Arslan Sehgal, Mazhar Ayaz, Muhammad Sajid, Jamal Muhammad Khan, Muhammad Ahsan, Mohd Ashraf Rather, Azmat Ali Khan, Jamilah M. Alshehri, Shopnil Akash, Eugenie Nepovimova, Kamil Kuca, and Rohit Sharma

Subjects

Pharmacophore, Virtual screening, Molecular docking, Multiepitope, Vaccine design, MAPK1, Science (General), Q1-390, Social sciences (General), H1-99

Abstract

Understanding the role of the mitogen-activated protein kinases (MAPKs) signalling pathway is essential in advancing treatments for neurodegenerative disorders like Alzheimer's. In this study, we investigate in-silico techniques involving computer-based methods to extract the MAPK1 sequence. Our applied methods enable us to analyze the protein's structure, evaluate its properties, establish its evolutionary relationships, and assess its prevalence in populations. We also predict epitopes, assess their ability to trigger immune responses, and check for allergenicity using advanced computational tools to understand their immunological properties comprehensively. We apply virtual screening, docking, and structure modelling to identify promising drug candidates, analyze their interactions, and enhance drug design processes. We identified a total of 30 cell-targeting molecules against the MAPK1 protein, where we selected top 10 CTL epitopes (PAGGGPNPG, GGGPNPGSG, SAPAGGGPN, AVSAPAGGG, AGGGPNPGS, ATAAVSAPA, TAAVSAPAG, ENIIGINDI, INDIIRTPT, and NDIIRTPTI) for further evaluation to determine their potential efficacy, safety, and suitability for vaccine design based on strong binding potential. The potential to cover a large portion of the world's population with these vaccines is substantial—88.5 % for one type and 99.99 % for another. In exploring the molecular docking analyses, we examined a library of compounds from the ZINC database. Among them, we identified twelve compounds with the lowest binding energy. Critical residues in the MAPK1 protein, such as VAL48, LYS63, CYS175, ASP176, LYS160, ALA61, LEU165, TYR45, SER162, ARG33, PRO365, PHE363, ILE40, ASN163, and GLU42, are pivotal for interactions with these compounds. Our result suggests that these compounds could influence the protein's behaviour. Moreover, our docking analyses revealed that the predicted peptides have a strong affinity for the MAPK1 protein. These peptides form stable complexes, indicating their potential as potent inhibitors. This study contributes to the identification of new drug compounds and the screening of their desired properties. These compounds could potentially help reduce the excessive activity of MAPK1, which is linked to Alzheimer's disease.

Published

2023

6. Self-assembled multiepitope nanovaccine based on NoV P particles induces effective and lasting protection against H3N2 influenza virus.

Author

Nie, Jiaojiao, Wang, Qingyu, Jin, Shenghui, Yao, Xin, Xu, Lipeng, Chang, Yaotian, Ding, Fan, Li, Zeyu, Sun, Lulu, Shi, Yuhua, and Shan, Yaming

Subjects

INFLUENZA A virus, H3N2 subtype, INFLUENZA viruses, CYTOTOXIC T cells, ANTIBODY-dependent cell cytotoxicity, EXTRACELLULAR matrix proteins, SEASONAL influenza, AVIAN influenza

Abstract

Current seasonal influenza vaccines confer only limited coverage of virus strains due to the frequent genetic and antigenic variability of influenza virus (IV). Epitope vaccines that accurately target conserved domains provide a promising approach to increase the breadth of protection; however, poor immunogenicity greatly hinders their application. The protruding (P) domain of the norovirus (NoV), which can self-assemble into a 24-mer particle called the NoV P particle, offers an ideal antigen presentation platform. In this study, a multiepitope nanovaccine displaying influenza epitopes (HMN-PP) was constructed based on the NoV P particle nanoplatform. Large amounts of HMN-PP were easily expressed in Escherichia coli in soluble form. Animal experiments showed that the adjuvanted HMN-PP nanovaccine induced epitope-specific antibodies and haemagglutinin (HA)-specific neutralizing antibodies, and the antibodies could persist for at least three months after the last immunization. Furthermore, HMN-PP induced matrix protein 2 extracellular domain (M2e)-specific antibody-dependent cell-mediated cytotoxicity, CD4+ and CD8+ T-cell responses, and a nucleoprotein (NP)-specific cytotoxic T lymphocyte (CTL) response. These results indicated that the combination of a multiepitope vaccine and self-assembled NoV P particles may be an ideal and effective vaccine strategy for highly variable viruses such as IV and SARS-CoV-2. [ABSTRACT FROM AUTHOR]

Published

2023

7. Proof of Concept of a Novel Multiepitope Recombinant Protein for the Serodiagnosis of Patients with Chagas Disease.

Author

Machado, Juliana Martins, Pereira, Isabela Amorim Gonçalves, Maia, Ana Clara Gontijo, Francisco, Mariana Ferraz Chaves, Nogueira, Lais Moreira, Gandra, Isadora Braga, Ribeiro, Anna Julia, Silva, Kamila Alves, Resende, Carlos Ananias Aparecido, da Silva, Jonatas Oliveira, dos Santos, Michelli, Gonçalves, Ana Alice Maia, Tavares, Grasiele de Sousa Vieira, Chávez-Fumagalli, Miguel Angel, Campos-da-Paz, Mariana, Giunchetti, Rodolfo Cordeiro, Rocha, Manoel Otávio da Costa, Chaves, Ana Thereza, Coelho, Eduardo Antônio Ferraz, and Galdino, Alexsandro Sobreira

Subjects

CHAGAS' disease, RECOMBINANT proteins, SERODIAGNOSIS, AMINO acid sequence, PROOF of concept, POLYPEPTIDES

Abstract

Chagas disease remains a neglected disease that is considered to be a public health problem. The early diagnosis of cases is important to improve the prognosis of infected patients and prevent transmission. Serological tests are the method of choice for diagnosis. However, two serological tests are currently recommended to confirm positive cases. In this sense, more sensitive and specific serological tests need to be developed to overcome these current diagnosis problems. This study aimed to develop a new recombinant multiepitope protein for the diagnosis of Chagas disease, hereafter named rTC. The rTC was constructed based on amino acid sequences from different combinations of Trypanosoma cruzi antigens in the same polypeptide and tested using an enzyme-linked immunosorbent assay (ELISA) to detect different types of Chagas disease. rTC was able to discriminate between indeterminate (IND) and cardiac (CARD) cases and cross-reactive diseases, as well as healthy samples, with 98.28% sensitivity and 96.67% specificity, respectively. These data suggest that rTC has the potential to be tested in future studies against a larger serological panel for the diagnosis of Chagas disease. [ABSTRACT FROM AUTHOR]

Published

2023

8. Efficacy of a Novel Multiepitope Vaccine Candidate against Foot-and-Mouth Disease Virus Serotype O and A.

Author

Chathuranga, W. A. Gayan, Hewawaduge, Chamith, Nethmini, N. A. Nadeeka, Kim, Tae-Hwan, Kim, Ju Hun, Ahn, Young-Hoon, Yoon, In-Joong, Yoo, Sung-Sik, Park, Jong-Hyeon, and Lee, Jong-Soo

Subjects

FOOT & mouth disease, VIRUS diseases, RECOMBINANT proteins, ANIMAL diseases, VACCINES

Abstract

Foot-and-mouth disease (FMD) is a highly contagious and economically devastating disease in cloven-hoofed animals. To prevent the spread of FMD virus (FMDV), traditional inactivated vaccines are used to immunize susceptible animals in disease-endemic countries. However, the inactivated FMD vaccine has several limitations, including safety concerns. To overcome these limitations, subunit proteins have been studied as alternative vaccine candidates. In this study, we designed two multiepitope recombinant proteins (OVM and AVM) containing antigenic sites (residue of VP1 132–162 and residue of VP1 192–212) of three topotypes of FMDV serotype O or three topotypes of FMDV serotype A. Each recombinant protein was efficiently expressed in Escherichia coli with high solubility, and the immunogenicity and protective efficacy of the proteins as FMD vaccine candidates were evaluated. The results showed that OVM and AVM emulsified with ISA201 adjuvant induced effective antigen-specific humoral and cell-mediated immune responses and successfully protected mice from O/Jincheon/SKR/2014, O/VET/2013, and A/Malaysia/97 viruses. In addition, intramuscular immunization of pigs with the OVM and AVM emulsified with ISA201 elicited effective levels of neutralizing antibodies to the viruses with homologous epitopes. Importantly, OVM-AVM emulsified with CAvant®SOE-X adjuvant conferred 100% protection against the O/Jincheon/SKR/2014 virus with homologous residues and 75% protection against A/SKR/GP/2018 with heterologous residues. The results presented in this study suggest that the combination of OVM and AVM protein with an effective adjuvant could yield an effective and safe vaccine candidate for the prevention and control of foot-and-mouth disease. In addition, our results provide a vaccine platform that can safely, cost-efficiently, and rapidly generate protective vaccine candidates against diverse FMDVs. [ABSTRACT FROM AUTHOR]

Published

2022

9. In silico and immunoinformatics based multiepitope subunit vaccine design for protection against visceral leishmaniasis.

Author

Bhowmik D, Bhuyan A, Gunalan S, Kothandan G, and Kumar D

Subjects

Humans, Epitopes immunology, Epitopes chemistry, Computer Simulation, Amino Acid Sequence, Leishmaniasis Vaccines immunology, Leishmaniasis Vaccines chemistry, Antigens, Protozoan immunology, Antigens, Protozoan chemistry, Protozoan Proteins immunology, Protozoan Proteins chemistry, Epitopes, T-Lymphocyte immunology, Epitopes, T-Lymphocyte chemistry, Immunoinformatics, Leishmaniasis, Visceral prevention & control, Leishmaniasis, Visceral immunology, Leishmaniasis, Visceral parasitology, Vaccines, Subunit immunology, Vaccines, Subunit chemistry, Molecular Docking Simulation, Computational Biology methods, Molecular Dynamics Simulation, Leishmania donovani immunology

Abstract

Visceral leishmaniasis (VL) is a vector-borne neglected tropical protozoan disease with high fatality and no certified vaccine. Conventional vaccine preparation is challenging and tedious. Here in this work, we created a global multiepitope subunit vaccination against VL utilizing innovative immunoinformatics technique based on the extensively conserved epitopic regions of the PrimPol protein of Leishmania donovani consisting of four subunits which were analyzed and studied, out of which DNA primase large subunit and DNA polymerase α subunit B were evaluated as antigens by Vaxijen 2.0. The multiepitope vaccine design includes a single adjuvant β-defensins, eight CTL epitopes, eight HTL epitopes, seven linear BCL epitopes and one discontinuous BCL epitope to induce innate, cellular and humoral immune responses against VL. The Expasy ProtParam tool characterized the physiochemical parameters of the vaccine. At the same time, SOLpro evaluated our vaccine constructs to be soluble upon expression. We also modeled the stable tertiary structure of our vaccine construct through Robetta modeling for molecular docking studies with toll-like receptor proteins through HADDOCK 2.4. Simulations based on molecular dynamics revealed an intact vaccine and TLR8 complex, supporting our vaccine design's immunogenicity. Also, the immune simulation of our vaccine by the C-ImmSim server demonstrated the potency of the multiepitope vaccine construct to induce proper immune response for host defense. Codon optimization and in silico cloning of our vaccine further assured high expression. The outcomes of our study on multiepitope vaccine design significantly produced a potential candidate against VL and can potentially eradicate the disease in the future after clinical investigations.Communicated by Ramaswamy H. Sarma.

Published

2024

10. Comparison of BP26, Omp25 and Omp31 and a Multiepitope-Based Fusion Protein in the Serological Detection of Canine Brucellosis.

Author

Yao, Meixue, Liu, Mengda, Chen, Xia, Li, Jianjun, Li, Yan, Wei, Yu Run, Liu, Yong, Yang, Kang Long, Duan, Xiaoxiao, Shao, Weixing, Sun, Xiangxiang, Fan, Xiaoxu, Sun, Shufang, Tian, Lili, Yin, Dehui, and Sun, Mingjun

Subjects

CHIMERIC proteins, BRUCELLOSIS, ZOONOSES, MEMBRANE proteins, VIBRIO parahaemolyticus

Abstract

Background: Brucellosis is one of the most important zoonotic diseases in the world. Canine brucellosis, caused mainly by Brucella canis, is seriously neglected, and there is a lack of accurate diagnostic tools. Methods: In this study, to compare BP26, Omp25, Omp31 and a multiepitope-based fusion protein in the serological detection of canine brucellosis, using 34 brucellosis-positive dog sera and 62 negative control sera, the Brucella outer membrane proteins Omp31, BP26, Omp25 and a multiepitope-based fusion protein were evaluated by iELISA for their potential use as antigens in the serological diagnosis of canine brucellosis. Results: The results showed that the multiepitope-based fusion protein performed best in distinguishing brucellosis-positive and brucellosis-negative dog sera, with a positive predictive value (PPV) of 100% and a negative predictive value (NPV) of 98.41%. BP26 and Omp31 showed excellent sensitivity in detecting brucellosis-positive dog sera, but their cross reaction to sera infected with Vibrio parahaemolyticus and Listeria monocytogenes may hinder their application as diagnostic reagents. Omp25 lacked sufficient sensitivity and showed limited ability in distinguishing positive and negative dog sera. Conclusion: The multiepitope-based fusion protein can be used as an ideal antigen for serologically diagnosing canine brucellosis currently prevalent worldwide. [ABSTRACT FROM AUTHOR]

Published

2022

11. Design of a Multiepitope Vaccine against Chicken Anemia Virus Disease.

Author

Fatoba, Abiodun Joseph, Adeleke, Victoria T., Maharaj, Leah, Okpeku, Moses, Adeniyi, Adebayo A., and Adeleke, Matthew A.

Subjects

*VIRUS diseases, *MOLECULAR dynamics, *VACCINE effectiveness, *VIRAL proteins, *ANEMIA

Abstract

Chicken anemia virus (CAV) causes severe clinical and sub-clinical infection in poultry globally and thus leads to economic losses. The drawbacks of the commercially available vaccines against CAV disease signal the need for a novel, safe, and effective vaccine design. In this study, a multiepitope vaccine (MEV) consisting of T-cell and B-cell epitopes from CAV viral proteins (VP1 and VP2) was computationally constructed with the help of linkers and adjuvant. The 3D model of the MEV construct was refined and validated by different online bioinformatics tools. Molecular docking showed stable interaction of the MEV construct with TLR3, and this was confirmed by Molecular Dynamics Simulation. Codon optimization and in silico cloning of the vaccine in pET-28a (+) vector also showed its potential expression in the E. coli K12 system. The immune simulation also indicated the ability of this vaccine to induce an effective immune response against this virus. Although the vaccine in this study was computationally constructed and still requires further in vivo study to confirm its effectiveness, this study marks a very important step towards designing a potential vaccine against CAV disease. [ABSTRACT FROM AUTHOR]

Published

2022

12. SM-COLSARSPROT: Highly Immunogenic Supramutational Synthetic Peptides Covering the World's Population.

Author

Patarroyo, Manuel A., Patarroyo, Manuel E., Pabón, Laura, Alba, Martha P., Bermudez, Adriana, Rugeles, María Teresa, Díaz-Arevalo, Diana, Zapata-Builes, Wildeman, Zapata, María Isabel, Reyes, César, Suarez, Carlos F., Agudelo, William, López, Carolina, Aza-Conde, Jorge, Melo, Miguel, Escamilla, Luis, Oviedo, Jairo, Guzmán, Fanny, Silva, Yolanda, and Forero, Martha

Subjects

PEPTIDOMIMETICS, PEPTIDES, ANTIGENS, MAJOR histocompatibility complex, POLYPROLINE, HISTOCOMPATIBILITY antigens, ANTIBODY titer

Abstract

Fifty ~20–amino acid (aa)–long peptides were selected from functionally relevant SARS-CoV-2 S, M, and E proteins for trial B-21 and another 53 common ones, plus some new ones derived from the virus' main genetic variants for complementary trial C-21. Peptide selection was based on tremendous SARS-CoV-2 genetic variability for analysing them concerning vast human immunogenetic polymorphism for developing the first supramutational, Colombian SARS-protection (SM-COLSARSPROT), peptide mixture. Specific physicochemical rules were followed, i.e., aa predilection for polyproline type II left-handed (PPIIL) formation, replacing β-branched, aromatic aa, short-chain backbone H-bond-forming residues, π-π interactions (n→π* and π-CH), aa interaction with π systems, and molecular fragments able to interact with them, disrupting PPIIL propensity formation. All these modified structures had PPIIL formation propensity to enable target peptide interaction with human leukocyte antigen-DRβ1* (HLA-DRβ1*) molecules to mediate antigen presentation and induce an appropriate immune response. Such modified peptides were designed for human use; however, they induced high antibody titres against S, M, and E parental mutant peptides and neutralising antibodies when suitably modified and chemically synthesised for immunising 61 major histocompatibility complex class II (MHCII) DNA genotyped Aotus monkeys (matched with their corresponding HLA-DRβ1* molecules), predicted to cover 77.5% to 83.1% of the world's population. Such chemically synthesised peptide mixture represents an extremely pure, stable, reliable, and cheap vaccine for COVID-19 pandemic control, providing a new approach for a logical, rational, and soundly established methodology for other vaccine development. [ABSTRACT FROM AUTHOR]

Published

2022

13. SM-COLSARSPROT: Highly Immunogenic Supramutational Synthetic Peptides Covering the World’s Population

Author

Manuel A. Patarroyo, Manuel E. Patarroyo, Laura Pabón, Martha P. Alba, Adriana Bermudez, María Teresa Rugeles, Diana Díaz-Arevalo, Wildeman Zapata-Builes, María Isabel Zapata, César Reyes, Carlos F. Suarez, William Agudelo, Carolina López, Jorge Aza-Conde, Miguel Melo, Luis Escamilla, Jairo Oviedo, Fanny Guzmán, Yolanda Silva, Martha Forero, Lizdany Flórez-Álvarez, Wbeimar Aguilar-Jimenez, Armando Moreno-Vranich, Jason Garry, and Catalina Avendaño

Subjects

modified synthetic peptides, SARS-CoV-2, mutational variants, multiepitope, supramutational, worldwide coverage, Immunologic diseases. Allergy, RC581-607

Abstract

Fifty ~20–amino acid (aa)–long peptides were selected from functionally relevant SARS-CoV-2 S, M, and E proteins for trial B-21 and another 53 common ones, plus some new ones derived from the virus’ main genetic variants for complementary trial C-21. Peptide selection was based on tremendous SARS-CoV-2 genetic variability for analysing them concerning vast human immunogenetic polymorphism for developing the first supramutational, Colombian SARS-protection (SM-COLSARSPROT), peptide mixture. Specific physicochemical rules were followed, i.e., aa predilection for polyproline type II left-handed (PPIIL) formation, replacing β-branched, aromatic aa, short-chain backbone H-bond-forming residues, π-π interactions (n→π* and π-CH), aa interaction with π systems, and molecular fragments able to interact with them, disrupting PPIIL propensity formation. All these modified structures had PPIIL formation propensity to enable target peptide interaction with human leukocyte antigen-DRβ1* (HLA-DRβ1*) molecules to mediate antigen presentation and induce an appropriate immune response. Such modified peptides were designed for human use; however, they induced high antibody titres against S, M, and E parental mutant peptides and neutralising antibodies when suitably modified and chemically synthesised for immunising 61 major histocompatibility complex class II (MHCII) DNA genotyped Aotus monkeys (matched with their corresponding HLA-DRβ1* molecules), predicted to cover 77.5% to 83.1% of the world’s population. Such chemically synthesised peptide mixture represents an extremely pure, stable, reliable, and cheap vaccine for COVID-19 pandemic control, providing a new approach for a logical, rational, and soundly established methodology for other vaccine development.

Published

2022

14. Proof of Concept of a Novel Multiepitope Recombinant Protein for the Serodiagnosis of Patients with Chagas Disease

Author

Juliana Martins Machado, Isabela Amorim Gonçalves Pereira, Ana Clara Gontijo Maia, Mariana Ferraz Chaves Francisco, Lais Moreira Nogueira, Isadora Braga Gandra, Anna Julia Ribeiro, Kamila Alves Silva, Carlos Ananias Aparecido Resende, Jonatas Oliveira da Silva, Michelli dos Santos, Ana Alice Maia Gonçalves, Grasiele de Sousa Vieira Tavares, Miguel Angel Chávez-Fumagalli, Mariana Campos-da-Paz, Rodolfo Cordeiro Giunchetti, Manoel Otávio da Costa Rocha, Ana Thereza Chaves, Eduardo Antônio Ferraz Coelho, and Alexsandro Sobreira Galdino

Subjects

multiepitope, recombinant protein, immunodiagnosis, Chagas disease, Medicine

Abstract

Chagas disease remains a neglected disease that is considered to be a public health problem. The early diagnosis of cases is important to improve the prognosis of infected patients and prevent transmission. Serological tests are the method of choice for diagnosis. However, two serological tests are currently recommended to confirm positive cases. In this sense, more sensitive and specific serological tests need to be developed to overcome these current diagnosis problems. This study aimed to develop a new recombinant multiepitope protein for the diagnosis of Chagas disease, hereafter named rTC. The rTC was constructed based on amino acid sequences from different combinations of Trypanosoma cruzi antigens in the same polypeptide and tested using an enzyme-linked immunosorbent assay (ELISA) to detect different types of Chagas disease. rTC was able to discriminate between indeterminate (IND) and cardiac (CARD) cases and cross-reactive diseases, as well as healthy samples, with 98.28% sensitivity and 96.67% specificity, respectively. These data suggest that rTC has the potential to be tested in future studies against a larger serological panel for the diagnosis of Chagas disease.

Published

2023

15. A broad-spectrum multiepitope vaccine against seasonal influenza A and B viruses in mice.

Author

Yuan L, Zhang S, Bi R, Liu X, Han Z, Li M, Liao X, Xie T, Bai S, Xie Q, Luo C, Jiang Y, Yuan J, Luo H, Yan H, Sun C, and Shu Y

Subjects

Animals, Mice, Female, Influenza A virus immunology, Antibodies, Viral immunology, Epitopes, T-Lymphocyte immunology, Disease Models, Animal, Mice, Inbred C57BL, Vaccines, DNA immunology, Vaccines, DNA administration & dosage, Seasons, Influenza A Virus, H3N2 Subtype immunology, Humans, Influenza Vaccines immunology, Influenza Vaccines administration & dosage, Influenza B virus immunology, Orthomyxoviridae Infections prevention & control, Orthomyxoviridae Infections immunology, Epitopes, B-Lymphocyte immunology

Abstract

Background: Influenza viruses pose a persistent threat to global public health, necessitating the development of innovative and broadly effective vaccines., Methods: This study focuses on a multiepitope vaccine (MEV) designed to provide broad-spectrum protection against different influenza viruses. The MEV, containing 19 B-cell linear epitopes, 7 CD4 + T cells, and 11 CD8 + T cells epitopes identified through enzyme-linked immunospot assay (ELISPOT) in influenza viruses infected mice, was administered through a regimen of two doses of DNA vaccine followed by one dose of a protein vaccine in C57BL/6 female mice., Findings: Upon lethal challenge with both seasonal circulating strains (H1N1, H3N2, BV, and BY) and historical strains (H1N1-PR8 and H3N2-X31), MEV demonstrated substantial protection against different influenza seasonal strains, with partial efficacy against historical strains. Notably, the increased germinal centre B cells and antibody-secreting cells, along with robust T cell immune responses, highlighted the comprehensive immune defence elicited by MEV. Elevated hemagglutinin inhibition antibody was also observed against seasonal circulating and historical strains. Additionally, mice vaccinated with MEV exhibited significantly lower counts of inflammatory cells in the lungs compared to negative control groups., Interpretation: Our results demonstrated the efficacy of a broad-spectrum MEV against influenza viruses in mice. Conducting long-term studies to evaluate the durability of MEV-induced immune responses and explore its potential application in diverse populations will offer valuable insights for the continued advancement of this promising vaccine., Funding: Funding bodies are described in the Acknowledgments section., Competing Interests: Declaration of interests The authors declare that they have no competing financial interests., (Copyright © 2024 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published

2024

16. Immunoinformatics Design of Multiepitope Vaccine Against Enterococcus faecium Infection.

Author

Fatoba, Abiodun J., Adeleke, Victoria T., Maharaj, Leah, Okpeku, Moses, Adeniyi, Adebayo A., and Adeleke, Matthew A.

Subjects

*ENTEROCOCCUS faecium, *ENTEROCOCCAL infections, *ENTEROCOCCUS, *VACCINE effectiveness, *VACCINE approval, *VACCINES

Abstract

Enterococcus faecium has emerged as the fourth most commonly isolated nosocomial pathogen due to its resistance to commonly used antibiotics and, as such, poses a serious threat to human health. Alternative control through vaccination has received much attention, but there is no clinically approved vaccine against this pathogen. This, therefore, necessitates the need for a novel vaccine design. This present study was conducted to design a multiepitope-based vaccine (MEV) against E. faecium infection based on the secreted antigen A (SagA) and peptidyl-prolyl cis–trans isomerase (PPic) of this pathogen which are promising vaccine candidates. A final total of 7 CD8+ T-cell and 11 CD4+ T-cell epitopes, which are highly antigenic, IFN-γ inducer, and overlapping, were shortlisted from both protein antigens. The selected epitopes showed good population coverage and interacted with both HLA-A*02:06 and HLA-DRB1*01:01 alleles. The constructed MEV which consists of T-cell epitopes of both SagA and PPic antigen was fused by linkers and adjuvant. The 3D structure of the MEV construct was predicted, refined, and validated using different bioinformatics tools. The MEV construct showed a strong binding interaction and stability with Toll-like receptor 2 (TLR2). Finally, the vaccine construct was codon-optimised for expression in E. coli K12 system and cloned into a pET-28a (+) vector. This study provides background for designing a suitable, safe, and effective vaccine against antibiotic-resistant E. faecium infection. [ABSTRACT FROM AUTHOR]

Published

2021

17. Efficacy of a Novel Multiepitope Vaccine Candidate against Foot-and-Mouth Disease Virus Serotype O and A

Author

W. A. Gayan Chathuranga, Chamith Hewawaduge, N. A. Nadeeka Nethmini, Tae-Hwan Kim, Ju Hun Kim, Young-Hoon Ahn, In-Joong Yoon, Sung-Sik Yoo, Jong-Hyeon Park, and Jong-Soo Lee

Subjects

foot-and-mouth disease virus, subunit vaccine, B cell epitope, multiepitope, ISA201, Medicine

Abstract

Foot-and-mouth disease (FMD) is a highly contagious and economically devastating disease in cloven-hoofed animals. To prevent the spread of FMD virus (FMDV), traditional inactivated vaccines are used to immunize susceptible animals in disease-endemic countries. However, the inactivated FMD vaccine has several limitations, including safety concerns. To overcome these limitations, subunit proteins have been studied as alternative vaccine candidates. In this study, we designed two multiepitope recombinant proteins (OVM and AVM) containing antigenic sites (residue of VP1 132–162 and residue of VP1 192–212) of three topotypes of FMDV serotype O or three topotypes of FMDV serotype A. Each recombinant protein was efficiently expressed in Escherichia coli with high solubility, and the immunogenicity and protective efficacy of the proteins as FMD vaccine candidates were evaluated. The results showed that OVM and AVM emulsified with ISA201 adjuvant induced effective antigen-specific humoral and cell-mediated immune responses and successfully protected mice from O/Jincheon/SKR/2014, O/VET/2013, and A/Malaysia/97 viruses. In addition, intramuscular immunization of pigs with the OVM and AVM emulsified with ISA201 elicited effective levels of neutralizing antibodies to the viruses with homologous epitopes. Importantly, OVM-AVM emulsified with CAvant®SOE-X adjuvant conferred 100% protection against the O/Jincheon/SKR/2014 virus with homologous residues and 75% protection against A/SKR/GP/2018 with heterologous residues. The results presented in this study suggest that the combination of OVM and AVM protein with an effective adjuvant could yield an effective and safe vaccine candidate for the prevention and control of foot-and-mouth disease. In addition, our results provide a vaccine platform that can safely, cost-efficiently, and rapidly generate protective vaccine candidates against diverse FMDVs.

Published

2022

18. Reverse vaccinology approach towards the in-silico multiepitope vaccine development against SARS-CoV-2 [version 1; peer review: 2 approved]

Author

Vipul Kumar, Sudhakar Kancharla, Prachetha Kolli, and Manoj Jena

Subjects

Research Article, Articles, SARS-CoV-2, COVID-19, Immunoinformatics, multiepitope, docking, simulations.

Abstract

Background: The novel severe acute respiratory syndrome related corona virus-2 (SARS-CoV-2) belongs to the “Coronaviridae” family and order “Nidovirales”, which has caused the pandemic coronavirus disease 2019 (COVID-19). SARS-CoV-2 has been spread in more than a 100 countries, and more than a million have lost their lives. Vaccination and immunization could be an effective strategy to combat fatal COVID-19. Methods: For identification of effective vaccine candidate against COVID-19, various immunoinformatics online tools and softwares were used to predict epitopes. Cytotoxic T cell epitopes, helper T cell epitopes, and B cell epitopes from three structural polyproteins (Spike, Membrane, and Nucleocapsid (SMN) based on the binding affinity towards MHC, antigenicity, non-allergenicity, and non-toxicity) were identified for vaccine development. The multiepitope based vaccine was constructed linking two additional adjuvants human beta-defensin-3 and human beta-defensin-2 at N and C terminal, respectively. Results: The constructed vaccine sequence was found to be a good antigen and non-allergen for the human body. The constructed vaccine was docked with the TLR-3 receptor. The docked complex was further taken for molecular dynamics simulations and RMSD was calculated, which showed stable binding of the complex. The codon adaptation index (CAI) of 0.92 and GC content of 55.5% for E. coli (K12 strain) suggested efficient expression of the predicted vaccine. Conclusion: The current study can be helpful in the reduction of time and cost for further experimental validations and could give a valuable contribution against this pandemic.

Published

2021

19. Construction of a polyepitope vaccine against Newcastle disease by immunoinformatics design of immunogenic proteins.

Author

Roudbari, Zahra, Gorj, Abdolvahab Ebrahimpour, and Brazandeh, Arsalan

Abstract

Objective Application of molecular biology techniques to the production of new vaccines against different strains of the Newcastle disease virus (NDV) has been the subject of recent research reports. Development of improved techniques for genome sequencing has led to the recognition of protective mechanisms and the identification of possible candidate antigens. The present research aimed to design a recombinant chimeric immunogen against binding agents in Newcastle virus in birds. Materials and methods Therefore, we conducted this investigation to make a recombinant vaccine in silico in order to control and eliminate this disease using anti-leptospirosis epitopes, F, and HN antigens. To bind these epitopes, KK, as AAY linkers, were selected to bind the structure. This structure contained 309 amino acids. The important biological factors of this recombinant vaccine, such as physicochemical properties, different structures, stability, intrinsic protein disorder, solubility, and allergenicity of this vaccine structure were evaluated using immune system analysis. Results Various analyses confirmed the stability of this structure, and the epitopes predicted in the chimeric vaccine showed a high potential for inducing the immune response of B cell and T cell. Thus, immune system analysis revealed that the modeled multi-epitope vaccine could properly stimulate T and B cell immune responses and could potentially be utilized for prophylactic or control applications. Conclusion The results of this study could be employed to control and eliminate leptospirosis in the future after confirming its effectiveness by experimental immunological assays. [ABSTRACT FROM AUTHOR]

Published

2021

20. Design of a Multiepitope Vaccine against Chicken Anemia Virus Disease

Author

Abiodun Joseph Fatoba, Victoria T. Adeleke, Leah Maharaj, Moses Okpeku, Adebayo A. Adeniyi, and Matthew A. Adeleke

Subjects

chicken anemia virus, disease, immunoinformatics, immune response, multiepitope, viral proteins, Microbiology, QR1-502

Abstract

Chicken anemia virus (CAV) causes severe clinical and sub-clinical infection in poultry globally and thus leads to economic losses. The drawbacks of the commercially available vaccines against CAV disease signal the need for a novel, safe, and effective vaccine design. In this study, a multiepitope vaccine (MEV) consisting of T-cell and B-cell epitopes from CAV viral proteins (VP1 and VP2) was computationally constructed with the help of linkers and adjuvant. The 3D model of the MEV construct was refined and validated by different online bioinformatics tools. Molecular docking showed stable interaction of the MEV construct with TLR3, and this was confirmed by Molecular Dynamics Simulation. Codon optimization and in silico cloning of the vaccine in pET-28a (+) vector also showed its potential expression in the E. coli K12 system. The immune simulation also indicated the ability of this vaccine to induce an effective immune response against this virus. Although the vaccine in this study was computationally constructed and still requires further in vivo study to confirm its effectiveness, this study marks a very important step towards designing a potential vaccine against CAV disease.

Published

2022

21. 3CL hydrolase‐based multiepitope peptide vaccine against SARS‐CoV‐2 using immunoinformatics.

Author

Jakhar, Renu, Kaushik, Samander, and Gakhar, Surendra K.

Subjects

SARS-CoV-2, VACCINES, INFECTION control, POPULATION, EPITOPES

Abstract

The present study provides the first multiepitope vaccine construct using the 3CL hydrolase protein of SARS‐CoV‐2. The coronavirus 3CL hydrolase (Mpro) enzyme is essential for proteolytic maturation of the virus. This study was based on immunoinformatics and structural vaccinology strategies. The design of the multiepitope vaccine was built using helper T‐cell and cytotoxic T‐cell epitopes from the 3CL hydrolase protein along with an adjuvant to enhance immune response; these are joined to each other by short peptide linkers. The vaccine also carries potential B‐cell linear epitope regions, B‐cell discontinuous epitopes, and interferon‐γ‐inducing epitopes. Epitopes of the constructed multiepitope vaccine were found to be antigenic, nonallergic, nontoxic, and covering large human populations worldwide. The vaccine construct was modeled, validated, and refined by different programs to achieve a high‐quality three‐dimensional structure. The resulting high‐quality model was applied for conformational B‐cell epitope selection and docking analyses with toll‐like receptor‐3 for understanding the capability of the vaccine to elicit an immune response. In silico cloning and codon adaptation were also performed with the pET‐19b plasmid vector. The designed multiepitope peptide vaccine may prompt the development of a vaccine to control SARS‐CoV‐2 infection. [ABSTRACT FROM AUTHOR]

Published

2020

22. In silico design of a broad-spectrum multiepitope vaccine against influenza virus.

Author

Yuan, Lifang, Li, Xu, Li, Minchao, Bi, Rongjun, Li, Yingrui, Song, Jiaping, Li, Wei, Yan, Mingchen, Luo, Huanle, Sun, Caijun, and Shu, Yuelong

Subjects

*INFLUENZA vaccines, *IMMUNOGLOBULINS, *INFLUENZA B virus, *SEASONAL influenza, *ESCHERICHIA coli, *INFLUENZA viruses, *CYTOTOXIC T cells

Abstract

Influenza remains a global health concern due to its potential to cause pandemics as a result of rapidly mutating influenza virus strains. Existing vaccines often struggle to keep up with these rapidly mutating flu viruses. Therefore, the development of a broad-spectrum peptide vaccine that can stimulate an optimal antibody response has emerged as an innovative approach to addressing the influenza threat. In this study, an immunoinformatic approach was employed to rapidly predict immunodominant epitopes from different antigens, aiming to develop an effective multiepitope influenza vaccine (MEV). The immunodominant B-cell linear epitopes of seasonal influenza strains hemagglutinin (HA) and neuraminidase (NA) were predicted using an antibody-peptide microarray, involving a human cohort including vaccinees and infected patients. On the other hand, bioinformatics tools were used to predict immunodominant cytotoxic T-cell (CTL) and helper T-cell (HTL) epitopes. Subsequently, these epitopes were evaluated by various immunoinformatic tools. Epitopes with high antigenicity, high immunogenicity, non-allergenicity, non-toxicity, as well as exemplary conservation were then connected in series with appropriate linkers and adjuvants to construct a broad-spectrum MEV. Moreover, the structural analysis revealed that the MEV candidates exhibited good stability, and the docking results demonstrated their strong affinity to Toll-like receptors 4 (TLR4). In addition, molecular dynamics simulation confirmed the stable interaction between TLR4 and MEVs. Three injections with MEVs showed a high level of B-cell and T-cell immune responses according to the immunological simulations in silico. Furthermore, in-silico cloning was performed, and the results indicated that the MEVs could be produced in considerable quantities in Escherichia coli (E. coli). Based on these findings, it is reasonable to create a broad-spectrum MEV against different subtypes of influenza A and B viruses in silico. [ABSTRACT FROM AUTHOR]

Published

2024

23. Design and production of a chimeric antigen against Zika virus.

Author

Miranda-López, Arleth, González-Ortega, Omar, Comas-García, Mauricio, and Rosales-Mendoza, Sergio

Subjects

*CHIMERIC antigen receptors, *ZIKA virus, *FLAVIVIRUSES

Abstract

Zika virus (ZIKV) is a flavivirus belonging to the family Flaviviridae. According to the World Health Organization, ZIKV is considered a serious public health problem worldwide because of its association with microcephaly and Guillain-Barré syndrome. There are currently no approved vaccines or specific medical treatments, making both aspects relevant targets for biomedical research. In our study we designed and produced in Escherichia coli a multiepitope vaccine candidate against ZIKV capable of inducing cellular and humoral responses. A chimeric protein was designed based on a series of ZIKV antigenic sequences and a bacterial carrier. Modeling, prediction, and analysis of the recombinant protein structure was performed using Phyre2 and ChimeraX servers. The antigen was produced in Escherichia coli and purified from inclusion bodies. Twenty-six sequences were obtained and analyzed on the Phyre2 and ChimeraX servers. The selected chimera had a hydrophobicity index of - 4.635. The protein was efficiently induced at a lactose concentration of 1.5 g/L, and the SDS-PAGE analysis shows that most of the protein remains in the insoluble fraction. However, the protein was successfully solubilized, refolded and purified. The next step is evaluation in mice to determine the immunogenic response. [ABSTRACT FROM AUTHOR]

Published

2024

24. An evaluation of a recombinant multiepitope based antigen for detection of Toxoplasma gondii specific antibodies

Author

Khalid Hajissa, Robaiza Zakaria, Rapeah Suppian, and Zeehaida Mohamed

Subjects

T. Gondii, Elisa, Multiepitope, USM.TOXO1, Serodiagnosis, Recombinant antigens, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background The inefficiency of the current tachyzoite antigen-based serological assays for the serodiagnosis of Toxoplasma gondii infection mandates the need for acquirement of reliable and standard diagnostic reagents. Recently, epitope-based antigens have emerged as an alternative diagnostic marker for the achievement of highly sensitive and specific capture antigens. In this study, the diagnostic utility of a recombinant multiepitope antigen (USM.TOXO1) for the serodiagnosis of human toxoplasmosis was evaluated. Methods An indirect enzyme-linked immunosorbent assay (ELISA) was developed to evaluate the usefulness of USM.TOXO1 antigen for the detection of IgG antibodies against Toxoplasma gondii in human sera. Whereas the reactivity of the developed antigen against IgM antibody was evaluated by western blot and Dot enzyme immunoassay (dot-EIA) analysis. Results The diagnostic performance of the new antigens in IgG ELISA was achieved at the maximum values of 85.43% and 81.25% for diagnostic sensitivity and specificity respectively. The USM.TOXO1 was also proven to be reactive with anti- T. gondii IgM antibody. Conclusions This finding makes the USM.TOXO1 antigen an attractive candidate for improving the toxoplasmosis serodiagnosis and demonstrates that multiepitope antigens could be a potential and promising diagnostic marker for the development of high sensitive and accurate assays.

Published

2017

25. Immunoinformatics Approach to Design a Novel Epitope-Based Oral Vaccine Against Helicobacter pylori.

Author

Urrutia-Baca, Victor Hugo, Gomez-flores, Ricardo, De La Garza-Ramos, Myriam Angélica, Tamez-guerra, Patricia, Lucio-sauceda, Daniela Guadalupe, and Rodríguez-padilla, María Cristina

Subjects

*ORAL vaccines, *HELICOBACTER pylori, *HELICOBACTER pylori infections, *CHOLERA toxin, *GASTRIC mucosa, *ISOELECTRIC point, *PEPTIC ulcer

Abstract

Helicobacter pylori is an infectious agent that colonizes the gastric mucosa of half of the population worldwide. This bacterium has been recognized as belonging to group 1 carcinogen by the World Health Organization for the role in development of gastritis, peptic ulcers, and cancer. Due to the increase in resistance to antibiotics used in the anti-H. pylori therapy, the development of an effective vaccine is an alternative of great interest, which remains a challenge. Therefore, a rational, strategic, and efficient vaccine design against H. pylori is necessary where the use of the most current bioinformatics tools could help achieve it. In this study, immunoinformatics approach was used to design a novel multiepitope oral vaccine against H. pylori. Our multiepitope vaccine is composed of cholera toxin subunit B (CTB) that is used as a mucosal adjuvant to enhance vaccine immunogenicity for oral immunization. CTB fused to 11 epitopes predicted of pathogenic (UreB170–189, VacA459–478, CagA1103–1122, GGT106–126, NapA30–44, and OipA211–230) and colonization (HpaA33–52, FlaA487–506, FecA437–456, BabA129–149, and SabA540–559) proteins from H. pylori. CKS9 peptide (CKSTHPLSC) targets epithelial microfold cells to enhance vaccine uptake from the gut barrier. All sequences were joined to each other by proper linkers. The vaccine was modeled and validated to achieve a high-quality three-dimensional structure. The vaccine design was evaluated as nonallergenic, antigenic, soluble, and with an appropriate molecular weight and isoelectric point. Our results suggest that our newly designed vaccine could serve as a promising anti-H. pylori vaccine candidate. [ABSTRACT FROM AUTHOR]

Published

2019

26. Expression of Breast Cancer-Related Epitopes Targeting the IGF-1 Receptor in Chimeric Human Parvovirus B19 Virus-Like Particles.

Author

Salazar-González, Jorge Alberto, Ruiz-Cruz, Alail Antonio, Bustos-Jaimes, Ismael, and Moreno-Fierros, Leticia

Abstract

Breast cancer is a worldwide health problem, and the complexity of the disease, as well as the lack of treatment specificity, generates an urgent need for developing prophylactic and therapeutic measures. Searching for novel epitope-based approaches able to induce tumour immunity, we designed virus-like particles (VLPs) derived from Human parvovirus B19 assembled of chimeric VP2 proteins displaying two epitopes from the insulin-like growth factor-1 receptor (IGF-1R). Here, we present the generation of two chimeric VP2s that retain the stability, solubility and conditions of purification and assembly of the native VP2. We generated versatile chimeric multiepitope anti-cancer vaccine candidates, which prevented and delayed tumour growth when used in a prophylactic scheme of 4 weekly immunizations prior to 4T1 cell inoculation in female BALB/c mice. The presence of specific antibodies against the displayed epitopes suggests their participation in the protective effect; in contrast, no significant proliferative T-cell responses were recorded following stimulation by specific epitopes. The results comprise an approach whereby fusing desired epitopes from cancer to the N-terminus of B19 VP2 protein can generate a library of chimeric VP2-desired epitopes for further assembly in a designed and personalized epitope delivery system. [ABSTRACT FROM AUTHOR]

Published

2019

27. In silico designing of multiepitope-based-peptide (MBP) vaccine against MAPK protein express for Alzheimer's disease in Zebrafish.

Author

Arfat Y, Zafar I, Sehgal SA, Ayaz M, Sajid M, Khan JM, Ahsan M, Rather MA, Khan AA, Alshehri JM, Akash S, Nepovimova E, Kuca K, and Sharma R

Abstract

Understanding the role of the mitogen-activated protein kinases (MAPKs) signalling pathway is essential in advancing treatments for neurodegenerative disorders like Alzheimer's. In this study, we investigate in-silico techniques involving computer-based methods to extract the MAPK1 sequence. Our applied methods enable us to analyze the protein's structure, evaluate its properties, establish its evolutionary relationships, and assess its prevalence in populations. We also predict epitopes, assess their ability to trigger immune responses, and check for allergenicity using advanced computational tools to understand their immunological properties comprehensively. We apply virtual screening, docking, and structure modelling to identify promising drug candidates, analyze their interactions, and enhance drug design processes. We identified a total of 30 cell-targeting molecules against the MAPK1 protein, where we selected top 10 CTL epitopes (PAGGGPNPG, GGGPNPGSG, SAPAGGGPN, AVSAPAGGG, AGGGPNPGS, ATAAVSAPA, TAAVSAPAG, ENIIGINDI, INDIIRTPT, and NDIIRTPTI) for further evaluation to determine their potential efficacy, safety, and suitability for vaccine design based on strong binding potential. The potential to cover a large portion of the world's population with these vaccines is substantial-88.5 % for one type and 99.99 % for another. In exploring the molecular docking analyses, we examined a library of compounds from the ZINC database. Among them, we identified twelve compounds with the lowest binding energy. Critical residues in the MAPK1 protein, such as VAL48, LYS63, CYS175, ASP176, LYS160, ALA61, LEU165, TYR45, SER162, ARG33, PRO365, PHE363, ILE40, ASN163, and GLU42, are pivotal for interactions with these compounds. Our result suggests that these compounds could influence the protein's behaviour. Moreover, our docking analyses revealed that the predicted peptides have a strong affinity for the MAPK1 protein. These peptides form stable complexes, indicating their potential as potent inhibitors. This study contributes to the identification of new drug compounds and the screening of their desired properties. These compounds could potentially help reduce the excessive activity of MAPK1, which is linked to Alzheimer's disease., Competing Interests: The authors declare no conflict of interest, financial or otherwise., (© 2023 The Authors.)

Published

2023

28. An evaluation of a recombinant multiepitope based antigen for detection of Toxoplasma gondii specific antibodies.

Author

Hajissa, Khalid, Zakaria, Robaiza, Suppian, Rapeah, and Mohamed, Zeehaida

Subjects

*TOXOPLASMA gondii, *SERODIAGNOSIS, *ENZYME-linked immunosorbent assay, *IMMUNOGLOBULIN G, *ANTIGENS, *DIAGNOSIS, *TOXOPLASMOSIS diagnosis, *ANTIGEN-antibody reactions, *COMPARATIVE studies, *IMMUNOGLOBULINS, *RESEARCH methodology, *MEDICAL cooperation, *PROTOZOA, *RECOMBINANT proteins, *RESEARCH, *TOXOPLASMOSIS, *WESTERN immunoblotting, *EVALUATION research

Abstract

Background: The inefficiency of the current tachyzoite antigen-based serological assays for the serodiagnosis of Toxoplasma gondii infection mandates the need for acquirement of reliable and standard diagnostic reagents. Recently, epitope-based antigens have emerged as an alternative diagnostic marker for the achievement of highly sensitive and specific capture antigens. In this study, the diagnostic utility of a recombinant multiepitope antigen (USM.TOXO1) for the serodiagnosis of human toxoplasmosis was evaluated.Methods: An indirect enzyme-linked immunosorbent assay (ELISA) was developed to evaluate the usefulness of USM.TOXO1 antigen for the detection of IgG antibodies against Toxoplasma gondii in human sera. Whereas the reactivity of the developed antigen against IgM antibody was evaluated by western blot and Dot enzyme immunoassay (dot-EIA) analysis.Results: The diagnostic performance of the new antigens in IgG ELISA was achieved at the maximum values of 85.43% and 81.25% for diagnostic sensitivity and specificity respectively. The USM.TOXO1 was also proven to be reactive with anti- T. gondii IgM antibody.Conclusions: This finding makes the USM.TOXO1 antigen an attractive candidate for improving the toxoplasmosis serodiagnosis and demonstrates that multiepitope antigens could be a potential and promising diagnostic marker for the development of high sensitive and accurate assays. [ABSTRACT FROM AUTHOR]

Published

2017

29. Development and assessment of an improved recombinant multiepitope antigen-based immunoassay to diagnose chronic Chagas disease.

Author

Peverengo, Luz María, Garcia, Valeria, Rodeles, Luz María, Mendicino, Diego, Vicco, Miguel, Lagier, Claudia, Gonzalez, Verónica, Gugliotta, Luis, and Marcipar, Iván

Subjects

*DIAGNOSIS of Chagas' disease, *RECOMBINANT proteins, *IMMUNOASSAY, *ENZYME-linked immunosorbent assay, *EPITOPES

Abstract

The use of chimeric molecules fusing several antigenic determinants is a promising strategy for the development of low-cost, standardized and reliable kits to determine specific antibodies. In this study, we designed and assessed a novel recombinant chimera that complements the performance of our previously developed chimera, CP1 [FRA and SAPA antigens (Ags)], to diagnose chronic Chagas disease. The new chimeric protein, named CP3, is composed of MAP, TcD and TSSAII/V/VI antigenic determinants. We compared the performance of both chimeric Ags using a panel of 67 Trypanosoma cruzi -reactive sera and 67 non-reactive ones. The sensitivity of CP3 vs CP1 was 100 and 90.2%, and specificity was 92.5 and 100%, respectively. The mixture of CP1 + CP3 achieved 100% of sensitivity and specificity. More importantly, an additional subset of 17 sera from patients with discordant results of conventional serological methods was analysed; the CP1 + CP3 mixture allowed us to accurately classify 14 of them with respect to IIF, the usual technique used in most of the reference centres. These results show an improved performance of the CP1 + CP3 mixture in comparison with enzyme-linked immunosorbent assay and indirect haemagglutination commercial assays. [ABSTRACT FROM AUTHOR]

Published

2018

30. Immunoinformatics Approach to Design a Novel Epitope-Based Oral Vaccine AgainstHelicobacter pylori

Author

Ricardo Gomez-Flores, Patricia Tamez-Guerra, María Cristina Rodríguez-Padilla, Víctor Hugo Urrutia-Baca, Daniela Guadalupe Lucio-sauceda, and Myriam Angelica De La Garza-Ramos

Subjects

Models, Molecular, Cholera Toxin, medicine.drug_class, Population, Antibiotics, Administration, Oral, medicine.disease_cause, Protein Structure, Secondary, Epitope, Helicobacter Infections, Epitopes, Mice, 03 medical and health sciences, reverse vaccinology, 0302 clinical medicine, Adjuvants, Immunologic, Bacterial Proteins, Antigen, Genetics, medicine, Animals, Humans, Amino Acid Sequence, education, Molecular Biology, Research Articles, 030304 developmental biology, 0303 health sciences, education.field_of_study, Helicobacter pylori, biology, business.industry, Cholera toxin, Reverse vaccinology, Computational Biology, biology.organism_classification, Virology, Computational Mathematics, Computational Theory and Mathematics, in silico, 030220 oncology & carcinogenesis, Modeling and Simulation, Bacterial Vaccines, multiepitope, Gastritis, medicine.symptom, oral vaccine, business

Abstract

Helicobacter pylori is an infectious agent that colonizes the gastric mucosa of half of the population worldwide. This bacterium has been recognized as belonging to group 1 carcinogen by the World Health Organization for the role in development of gastritis, peptic ulcers, and cancer. Due to the increase in resistance to antibiotics used in the anti-H. pylori therapy, the development of an effective vaccine is an alternative of great interest, which remains a challenge. Therefore, a rational, strategic, and efficient vaccine design against H. pylori is necessary where the use of the most current bioinformatics tools could help achieve it. In this study, immunoinformatics approach was used to design a novel multiepitope oral vaccine against H. pylori. Our multiepitope vaccine is composed of cholera toxin subunit B (CTB) that is used as a mucosal adjuvant to enhance vaccine immunogenicity for oral immunization. CTB fused to 11 epitopes predicted of pathogenic (UreB170–189, VacA459–478, CagA1103–1122, GGT106–126, NapA30–44, and OipA211–230) and colonization (HpaA33–52, FlaA487–506, FecA437–456, BabA129–149, and SabA540–559) proteins from H. pylori. CKS9 peptide (CKSTHPLSC) targets epithelial microfold cells to enhance vaccine uptake from the gut barrier. All sequences were joined to each other by proper linkers. The vaccine was modeled and validated to achieve a high-quality three-dimensional structure. The vaccine design was evaluated as nonallergenic, antigenic, soluble, and with an appropriate molecular weight and isoelectric point. Our results suggest that our newly designed vaccine could serve as a promising anti-H. pylori vaccine candidate.

Published

2019

31. Design of a polytopic construct of LACK, TSA and GP63 proteins for the diagnosis of cutaneous leishmaniasis: An in silico strategy.

Author

Arab-Mazar, Zahra, Mohebali, Mehdi, Ranjbar, Mohammad Mehdi, Tabaei, Seyyed Javad Seyyed, Mamaghani, Amirreza Javadi, and Taghipour, Niloofar

Abstract

[Display omitted] • The synthesized multi-epitope was successfully expressed into Escherichia coli. • rGLT increased specificity of antigen detection tests by identifying B-cell epitopes. • Our novel multi-epitope antigens represent a potential target for CL diagnostic. Cutaneous leishmaniasis (CL), which is caused by different species of the genus Leishmania, including L. major , is a significant parasitic disease worldwide. Commercial leishmaniasis diagnostic kits frequently target the entire parasite antigen, although this approach can reduce the specificity of the tests. The present study sought to increase the specificity of antigen detection tests by identifying the B-cell epitopes on the surface of the protozoa and developing an antigenic multiepitope construct to react with the system of B-cell epitopes unique to L. major. More specifically, the linear and conformational B-cell epitopes for three L. major proteins, namely, GP63, LACK, and TSA, were predicted using the ABCprd, IEDB, LBtope, CBTOPE, and DiscoTope servers. The three-dimensional structures of these proteins, as well as of the complete multiepitope, were predicted using the I-TASSER server. The multiepitope structure models were validated by means of Ramachandran plots and the Prosa and Verify3D servers. The multiepitope construct was evaluated using the ProtParam and SOLpro servers. The synthesized multiepitope was then successfully expressed into a pET28a plasmid. The expression was confirmed using SDS-PAGE and dot blot techniques. Moreover, the expressed protein was evaluated by means of Western blotting. A band of approximately 39 kDa was observed by SDS-PAGE. The rGLT-pET-28a showed a high response with the 1:1000 dilution of the anti-His-tag monoclonal antibody by Western blot. The results of this study indicated that the integrated GP63, LACK, and TSA multiepitope antigens of L. major represent a potential target for a novel diagnostic kit for CL. [ABSTRACT FROM AUTHOR]

Published

2022

32. Pan genome based reverse vaccinology approach to explore Enterococcus faecium (VRE) strains for identification of novel multi-epitopes vaccine candidate.

Author

Alotaibi, Ghallab, Khan, Kanwal, Al Mouslem, Abdulaziz K., Ahmad Khan, Saeed, Naseer Abbas, Muhammad, Abbas, Muhammad, Ali Shah, Shafiq, and Jalal, Khurshid

Subjects

*ENTEROCOCCUS faecium, *ENTEROCOCCUS, *ATP-binding cassette transporters, *MEMBRANE proteins, *CARRIER proteins, *VANCOMYCIN resistance

Abstract

Enterococcus faecium is regarded as fourth most emerging common pathogen causing hospital acquired infections (HAIs), with high mortality rate, especially in children, elderly and immunocompromised patients. Recently, due to the emergence of E. faecium resistant strains especially vancomycin resistance (VRE) and their continuously growing resistivity to antibiotics, design of safe vaccine remains a choice for its control. Alternative control through vaccination has received much attention, but there is no clinically approved vaccine against this pathogen. Therefore, in current study we have applied a triple helix approach i.e., Pan-genome, subtractive genome and reverse vaccinology to identify and design potential vaccine candidates and multiepitope-based vaccine (MEV) construct against E. faecium (via core genome analysis from 216 strains). In this study, only 2 outer membrane proteins were identified through genome subtraction of resistant strains genes against human and essential proteins. Subsequently, phosphate ABC transporter substrate binding protein (Psts) was selected as a promiscuous vaccine candidate to develop a potent vaccine model. A final of four epitopes from CD8 + T-cell, CD4 + T-cell epitopes, and B-cell were shortlisted from outer membrane protein with highly antigenic, IFN-γ inducer, and overlapping characteristics for the construction of twelve vaccine models. The V3 construct was found to be highly immunogenic, non-toxic, non-allergenic, highly antigenic and most stable in terms of molecular docking and simulation studies against six HLAs, TLR2, and TLR4 complex. So far, this protein and multiepitope have never been characterized as vaccine targets against E. faecium. The current study proposed V3 as a significant vaccine candidate that could help the scientific community to treat E. faecium infections. [ABSTRACT FROM AUTHOR]

Published

2022

33. Immune responses induced in HHD mice by multiepitope HIV vaccine based on cryptic epitope modification.

Author

Li, Yinghui, Huang, Yuxiao, Liang, Jiao, Xu, Zhikai, Shen, Yan, Zhang, Ning, Liu, Zhongxiang, and Zhao, Ya

Abstract

CD8+ T cells play an important role in early HIV infection. However, HIV has the capacity to avoid specific CTL responses due to a high rate of mutation under selection pressure. Although the HIV proteins, gag and pol, are relatively conserved, these sequences generate low-affinity MHC-associated epitopes that are poorly immunogenic. Here, we applied an approach that enhanced the immunogenicity of low-affinity HLA-A2.1-binding peptides. The first position with tyrosine (P1Y) substitution enhanced the affinity of HLA-A2.1-associated peptides without altering their antigenic specificity. More importantly, P1Y variants efficiently stimulated in vivo native peptide-specific CTL that also recognized the corresponding naturally processed epitope. The potential to generate CTL against any low-affinity HLA-A2.1-associated peptide provides us with the necessary technique for identification of virus cryptic epitopes for development of peptide-based immunotherapy. Therefore, identification and modification of the cryptic epitopes of gal and pol provides promising candidates for HIV immunotherapy dependent upon efficient presentation by virus cells. Furthermore, this may be a breakthrough that overcomes the obstacle of immune escape caused by high rates of mutation. In this study, bioinformatics analysis was used to predict six low-affinity cryptic HIV gag and pol epitopes presented by HLA-A*0201. A HIV compound multi-CTL epitope gene was constructed comprising the gene encoding the modified cryptic epitope and the HIV p24 antigen, which induced a strong CD8+ T cell immune response regardless of the mutation. This approach represents a novel strategy for the development of safe and effective HIV prophylactic and therapeutic vaccines. [ABSTRACT FROM AUTHOR]

Published

2013

34. Computational characterization of Plasmodium falciparum proteomic data for screening of potential vaccine candidates

Author

Singh, Satarudra P., Khan, Feroz, and Mishra, Bhartendu N.

Subjects

*PLASMODIUM falciparum, *PROTEOMICS, *BIOINFORMATICS, *EPITOPES, *MALARIA, *T cells, *PEPTIDES

Abstract

Abstract: Advancement in the field of proteomics and bioinformatics offers tremendous opportunities for the development of novel epitope-based effective vaccine against human malaria. In this study, we have characterized 25 antigens as a vaccine candidate and screened the potential T-lymphocyte epitopes presented by human leukocyte antigen (HLA)-A, -B, and -DR molecules based on the proteomic data of Plasmodium falciparum. Of the 25 proteins, 22 were predicted as probable antigens and two were predicted as adhesions. In addition, seven proteins were predicted to contain signal peptide for secretary pathway and six proteins were found similar to the human and mouse reference proteins, whereas none of the proteins were predicted as allergen. A total of 14,841 peptides were predicted as epitope, presented by HLA class I and II supertypes that covered a broad human population (∼95%). Our results suggest that HLA-based multistage and multiepitope malaria vaccine would likely be needed to induce broader CD8+ as well as CD4+ T-cell responses. The predicted epitopes may be served as a useful diagnostic reagent for evaluating T-cell responses in the context of natural infection and/or vaccine trials. [Copyright &y& Elsevier]

Published

2010

35. A melanoma multiepitope polypeptide induces specific CD8+ T-cell response

Author

Levy, Adva, Pitcovski, Jacob, Frankenburg, Shoshana, Elias, Orit, Altuvia, Yael, Margalit, Hanna, Peretz, Tamar, Golenser, Jacob, and Lotem, Michal

Subjects

*MELANOMA, *IMMUNOTHERAPY, *T cells, *POLYPEPTIDES

Abstract

Abstract: Strategies using epitope-based vaccination are being considered for melanoma immunotherapy, in an attempt to overcome failure of other modalities. In the present study, we designed and produced a multiepitope polypeptide for melanoma (MEP-mel), which contains three repeats of four antigenic epitopes (gp100: 209–217 (210M); gp100: 280–288 (288V); Mart1: 26–35 (27L); tyrosinase: 368–376 (370D). The peptides were attached to each other by linkers containing sequences recognized by the proteasome, to improve protein cleavage and antigen presentation. The results show that peptide-specific T cells produced IFN-γ when stimulated with MEP-mel-transfected dendritic cells. The presentation of peptides by MEP-mel-transfected dendritic cells was proteasome-dependent and was more long-lasting than the presentation of exogenously delivered native peptides. When dendritic cells were loaded with MEP-mel protein, weak cross presentation was induced. The production of multiepitope molecules based on several peptides linked by sequences sensitive to proteasomal cleavage represents a promising new tool for the improvement of cancer immunotherapy. [Copyright &y& Elsevier]

Published

2007

36. Mucosal immunization with PLGA-microencapsulated DNA primes a SIV-specific CTL response revealed by boosting with cognate recombinant modified vaccinia virus Ankara

Author

Sharpe, Sally, Hanke, Tomás, Tinsley-Bown, Anne, Dennis, Mike, Dowall, Stuart, McMichael, Andrew, and Cranage, Martin

Subjects

*RHESUS monkeys, *HIV, *LYMPHOCYTES, *DNA

Abstract

Systemically administered DNA encoding a recombinant human immunodeficiency virus (HIV) derived immunogen effectively primes a cytotoxic T lymphocyte (CTL) response in macaques. In this further pilot study we have evaluated mucosal delivery of DNA as an alternative priming strategy. Plasmid DNA, pTH.HW, encoding a multi-CTL epitope gene, was incorporated into poly(d,l-lactic-co-glycolic acid) microparticles of less than 10 μm in diameter. Five intrarectal immunizations failed to stimulate a circulating vaccine-specific CTL response in 2 Mamu-A*01+ rhesus macaques. However, 1 week after intradermal immunization with a cognate modified vaccinia virus Ankara vaccine MVA.HW, CTL responses were detected in both animals that persisted until analysis postmortem, 12 weeks after the final boost. In contrast, a weaker and less durable response was seen in an animal vaccinated with the MVA construct alone. Analysis of lymphoid tissues revealed a disseminated CTL response in peripheral and regional lymph nodes but not the spleen of both mucosally primed animals. [Copyright &y& Elsevier]

Published

2003

37. The design of multiepitope vaccines from plasmids of diarrheagenic Escherichia coli against diarrhoea infection: Immunoinformatics approach.

Author

Adeleke, Victoria T., Adeniyi, Adebayo A., Adeleke, Matthew A., Okpeku, Moses, and Lokhat, David

Subjects

*EPITOPES, *ESCHERICHIA coli, *DRUG resistance in bacteria, *DIARRHEA, *PLASMIDS, *VACCINES, *PATHOGENIC bacteria

Abstract

Diarrhoea infection is a major global health public problem and is caused by many organisms including diarrheagenic Escherichia coli pathotypes. The common problem with diarrhoea is the drug resistance of pathogenic bacteria, the most promising alternative means of preventing drug resistance is vaccination. However, there has not been any significant success in the prevention of diarrhoea caused by E. coli through vaccination. Epitope-based vaccine is gaining more attention due to its safety and specificity. Sequence variation of protective antigens of the pathogen has posed a new challenge in the development of epitope-based vaccines against the infection, leading to the necessity of multiepitope based design. In this study, immunoinformatics tools were used to design multiepitope vaccine candidates from plasmid genome sequences of multiple pathotypes of E. coli species involved in diarrhoea infections. The ability of the identified epitopes to be used as a cross-protect multiepitope vaccine was achieved by identifying conserved, immunogenic and antigenic peptides that can elicit CD4+ T-cell, CD8+ T-cell and B-cell and bind to MHC I and II HLA alleles. The molecular docking results of T-cell epitopes showed their well binding affinity to receptive protein and with a wider population coverage. The different multiepitope-based vaccines (MEVCs) candidates were constructed and based on the types of epitope linker they contained. The MEVCs exhibited very good binding interactions with the human immune receptor. Among multiepitope vaccines constructed, MEVC6, MEVCA and MEVCB are more promising as potential vaccine candidates for cross-protection against gastrointestinal infections according to the computational study. It is also hoped that after validation and testing, the predicted multiepitope-based vaccine candidates will probably resolve the challenge of immunological heterogeneity facing enteric vaccine development. • This research intends to design multiepitope vaccine candidates from Escherichia coli plasmid. • Three multiepitope-based vaccine candidates against diarrhoea were predicted from the genomes of diarrheagenic E. coli. • The multiepitopes vaccines predicted covered five pathotypes of E. coli. • The epitope linkers have effect on the properties of the constructed multiepitopes and should therefore be considered. [ABSTRACT FROM AUTHOR]

Published

2021

38. An evaluation of a recombinant multiepitope based antigen for detection of Toxoplasma gondii specific antibodies

Author

Rapeah Suppian, Zeehaida Mohamed, Khalid Hajissa, and Robaiza Zakaria

Subjects

0301 basic medicine, Blotting, Western, 030231 tropical medicine, Antibodies, Protozoan, Antigens, Protozoan, Enzyme-Linked Immunosorbent Assay, Elisa, Cross Reactions, Multiepitope, Sensitivity and Specificity, Recombinant antigens, Epitope, lcsh:Infectious and parasitic diseases, Serology, law.invention, Epitopes, 03 medical and health sciences, 0302 clinical medicine, Antigen, law, medicine, Humans, Serologic Tests, lcsh:RC109-216, Serodiagnosis, medicine.diagnostic_test, biology, T. Gondii, USM.TOXO1, Toxoplasma gondii, biology.organism_classification, medicine.disease, Virology, Recombinant Proteins, Toxoplasmosis, 030104 developmental biology, Infectious Diseases, Immunoglobulin M, Immunoglobulin G, Immunoassay, Recombinant DNA, biology.protein, Antibody, Toxoplasma, Research Article

Abstract

Background The inefficiency of the current tachyzoite antigen-based serological assays for the serodiagnosis of Toxoplasma gondii infection mandates the need for acquirement of reliable and standard diagnostic reagents. Recently, epitope-based antigens have emerged as an alternative diagnostic marker for the achievement of highly sensitive and specific capture antigens. In this study, the diagnostic utility of a recombinant multiepitope antigen (USM.TOXO1) for the serodiagnosis of human toxoplasmosis was evaluated. Methods An indirect enzyme-linked immunosorbent assay (ELISA) was developed to evaluate the usefulness of USM.TOXO1 antigen for the detection of IgG antibodies against Toxoplasma gondii in human sera. Whereas the reactivity of the developed antigen against IgM antibody was evaluated by western blot and Dot enzyme immunoassay (dot-EIA) analysis. Results The diagnostic performance of the new antigens in IgG ELISA was achieved at the maximum values of 85.43% and 81.25% for diagnostic sensitivity and specificity respectively. The USM.TOXO1 was also proven to be reactive with anti- T. gondii IgM antibody. Conclusions This finding makes the USM.TOXO1 antigen an attractive candidate for improving the toxoplasmosis serodiagnosis and demonstrates that multiepitope antigens could be a potential and promising diagnostic marker for the development of high sensitive and accurate assays.

Published

2017

39. Evaluation of a tandem Chlamydia psittaci Pgp3 multiepitope peptide vaccine against a pulmonary chlamydial challenge in mice.

Author

Wang, Chuan, Li, Yumeng, Wang, Shuzhi, Yan, Xiaoliang, Xiao, Jian, Chen, Yuqing, Zheng, Kang, Tan, Yuan, Yu, Jian, Lu, Chunxue, and Wu, Yimou

Subjects

*BACTERIAL vaccines, *CHLAMYDIA infections, *HUMORAL immunity, *LUNG infections, *VACCINES, *MICE

Abstract

Chlamydia psittaci is the pathogen of psittacosis, and it has emerged as a significant public health threat. Because most infections are easily overlooked, a vaccine is recognized as the best solution to control the spread of C. psittaci. Our previous study showed that Pgp3 protein is efficacious as a subunit vaccine while not the best candidate due to the negative effects. Thus, in this study, we tested the ability of a tandem epitope vaccine candidate designated SP based on Pgp3-dominant epitopes to induce protective immunity against pulmonary chlamydial infection. BALB/c mice were intraperitoneally inoculated with multiepitope peptide antigens followed by intranasal infection with C. psittaci. We found that the multiepitope peptide antigens induced strong humoral and cellular immune responses with high Th1-related (IFN-γ and IL-2) and proinflammatory (IL-6) cytokine levels. Meanwhile, the pathogen burden and inflammatory infiltration were significantly reduced in lungs of SP-immunized mice after chlamydial challenge. In addition, the IFN-γ and IL-6 secretion levels in the infected lungs were substantially reduced. Overall, our findings demonstrate that the peptide vaccine SP plays a significant role with good immunogenicity and protective efficacy against C. psittaci lung infection in BALB/c mice, providing important insights towards understanding the potential of peptide vaccines as new vaccine antigens for inducing protective immunity against chlamydial infection. • Construct a Pgp3 mutiepitope vaccine SP based on bioinformatics analysis. • The peptide vaccine induced strong humoral and cellular immune responses. • The peptide vaccine shows good protective efficacy against C. psittaci lung infection. • Provides important insights towards understanding the potential of peptide vaccines. [ABSTRACT FROM AUTHOR]

Published

2020

40. Reverse vaccinology approach towards the in-silico multiepitope vaccine development against SARS-CoV-2.

Author

Kumar V, Kancharla S, Kolli P, and Jena M

Subjects

Defensins immunology, Escherichia coli, Humans, Molecular Docking Simulation, Molecular Dynamics Simulation, Vaccines, Subunit immunology, COVID-19, COVID-19 Vaccines immunology, Epitopes immunology, Immunogenicity, Vaccine, Vaccinology methods

Abstract

Background : The novel severe acute respiratory syndrome related corona virus-2 (SARS-CoV-2) belongs to the "Coronaviridae" family and order "Nidovirales", which has caused the pandemic coronavirus disease 2019 (COVID-19). SARS-CoV-2 has been spread in more than a 100 countries, and more than a million have lost their lives. Vaccination and immunization could be an effective strategy to combat fatal COVID-19. Methods : For identification of effective vaccine candidate against COVID-19, various immunoinformatics online tools and softwares were used to predict epitopes. Cytotoxic T cell epitopes, helper T cell epitopes, and B cell epitopes from three structural polyproteins (Spike, Membrane, and Nucleocapsid (SMN) based on the binding affinity towards MHC, antigenicity, non-allergenicity, and non-toxicity) were identified for vaccine development. The multiepitope based vaccine was constructed linking two additional adjuvants human beta-defensin-3 and human beta-defensin-2 at N and C terminal, respectively. Results : The constructed vaccine sequence was found to be a good antigen and non-allergen for the human body. The constructed vaccine was docked with the TLR-3 receptor.  The docked complex was further taken for molecular dynamics simulations and RMSD was calculated, which showed stable binding of the complex. The codon adaptation index (CAI) of 0.92 and GC content of 55.5% for E. coli (K12 strain) suggested efficient expression of the predicted vaccine. Conclusion : The current study can be helpful in the reduction of time and cost for further experimental validations and could give a valuable contribution against this pandemic., Competing Interests: No competing interests were disclosed., (Copyright: © 2021 Kumar V et al.)

Published

2021

41. Mucosal immunization with PLGA-microencapsulated DNA primes a SIV-specific CTL response revealed by boosting with cognate recombinant modified vaccinia virus Ankara

Author

Tomáš Hanke, Stuart D. Dowall, Sally Sharpe, Mike Dennis, Andrew J. McMichael, Martin P. Cranage, and Anne Margaret Tinsley-Bown

Subjects

Time Factors, Immunogen, Lymphoid Tissue, Polymers, Drug Compounding, Immunization, Secondary, Pilot Projects, Vaccinia virus, chemical and pharmacologic phenomena, Microparticles, Biology, Multiepitope, medicine.disease_cause, Epitope, Virus, law.invention, chemistry.chemical_compound, Polylactic Acid-Polyglycolic Acid Copolymer, Administration, Rectal, law, Virology, Vaccines, DNA, medicine, Animals, Cytotoxic T cell, Lactic Acid, Intestinal Mucosa, AIDS Vaccines, Drug Carriers, Vaccination, HIV, DNA, MVA, Simian immunodeficiency virus, Cytotoxicity Tests, Immunologic, Macaca mulatta, CTL, chemistry, Immunology, Recombinant DNA, Simian Immunodeficiency Virus, Vaccinia, Vaccine, Macaque, Polyglycolic Acid, T-Lymphocytes, Cytotoxic

Abstract

Systemically administered DNA encoding a recombinant human immunodeficiency virus (HIV) derived immunogen effectively primes a cytotoxic T lymphocyte (CTL) response in macaques. In this further pilot study we have evaluated mucosal delivery of DNA as an alternative priming strategy. Plasmid DNA, pTH.HW, encoding a multi-CTL epitope gene, was incorporated into poly(d,l-lactic-co-glycolic acid) microparticles of less than 10 μm in diameter. Five intrarectal immunizations failed to stimulate a circulating vaccine-specific CTL response in 2 Mamu-A*01+ rhesus macaques. However, 1 week after intradermal immunization with a cognate modified vaccinia virus Ankara vaccine MVA.HW, CTL responses were detected in both animals that persisted until analysis postmortem, 12 weeks after the final boost. In contrast, a weaker and less durable response was seen in an animal vaccinated with the MVA construct alone. Analysis of lymphoid tissues revealed a disseminated CTL response in peripheral and regional lymph nodes but not the spleen of both mucosally primed animals.

Published

2016

42. Construction and immune response characterization of a recombinant pseudorabies virus co-expressing capsid precursor protein (P1) and a multiepitope peptide of foot-and-mouth disease virus in swine

Author

He, Yannan, Qian, Ping, Zhang, Keshan, Yao, Qingxia, Wang, Dang, Xu, Zhuofei, Wu, Bin, Jin, Meilin, Xiao, Shaobo, and Chen, Huanchun

Published

2008

43. Induction of Humoral and Cellular Immune Responses in Mice by Multiepitope Vaccines Composing of Both T and B Lymphocyte Epitopes of MAGE-A3 which are Recombined into HBcAg.

Author

Chen Q, Li W, Wang P, Shao H, Ding Y, Wang W, Cen D, Cai Y, Xue X, Zhang L, and Zhu G

Subjects

Animals, Cell Proliferation, Cell Survival, Escherichia coli, Female, Humans, Immunity, Cellular, Immunity, Humoral, Immunogenicity, Vaccine, Mice, Inbred BALB C, Stomach Neoplasms immunology, T-Lymphocytes, Cytotoxic metabolism, Vaccines, Combined immunology, Antigens, Neoplasm immunology, Cancer Vaccines immunology, Epitopes, B-Lymphocyte immunology, Epitopes, T-Lymphocyte immunology, Hepatitis B Core Antigens immunology, Neoplasm Proteins immunology

Abstract

Background: Melanoma-associated antigen-A3 (MAGE-A3) is a tumor specific antigen and a potential candidate for cancer immunotherapy. We had screened three immunodominant multiepitopes of MAGE-A3, and identified these multiepitope peptides had significantly higher reactivity to serum samples from gastric cancer patients. However, the immune responses of three multiepitope peptides carried by HBcAg in mice have not been investigated., Objectives: The main objective of this study was to analyze the humoral and cellular immune responses in mice induced by these three multiepitope vaccines of MAGE-A3., Methods: Three multiepitopes of MAGE-A3 (MAGE-A3(EPI-1, or -2, or -3)) were respectively inserted at HBcAg major immunodominant region (HBcAg(MIR)) of the pET21a(+)/HBcAg(MIR) recombinant plasmid. These recombinant chimeras were identified by PCR, and transfected respectively into E. Coli Ressotta strain. The expression products of rHBcAg(MIR)/MAGE-A3(EPI-1, or -2, or -3) were purified respectively by Ni2+ chelated affinity column, and then confirmed by SDS-PAGE and Western-blot analysis.Purified three rHBcAg(MIR)/MAGE-A3 multiepitopes were administrated respectively into BALB/c (H-2Kd) mice by intradermal injection. The production of rHBcAg(MIR)/MAGE-A3(EPI-1, or -2, or -3) specific IgG in serum from immunized mice were measured by ELISA. Spleen cells from all immunized mice were harvested after one week of last immunization for lymphocyte proliferation assay and cytotoxic T-lymphocyte assay., Results: PCR and Sequencing analysis showed the presence of the required gene fragment in pET21a(+)/ HBcAg(MIR)/MAGE-A3(EPI-1, or -2, or -3) recombinant plasmid. Purified rHBcAg(MIR)/MAGE-A3(EPI-1, or -2, or -3) could be probed specifically by McAb of 6×his-tag. ELISA analysis indicated that serum from immunized mice with rHBcAg(MIR)/MAGE-A3(EPI-1, -2, or -3) proteins could be discerned specifically by complete MAGE-A3 protein, and high level of antibodies in immune serum were obtained, and all antibody titers could reach above 1:1600. The splenocytes from groups of rHBcAg(MIR)/MAGE-A3(EPI-1,-2, or -3), stimulated respectively with corresponding peptides showed the higher proliferative responses comparing with control groups of HBcAg(MIR) or PBS (p<0.05, respectively). Splenocytes from mice immunized with rHBcAg(MIR)/MAGE-A3 (EPI-1, or -2, or -3) could killed target cells effectively, and there were significant difference of CTL activities compared with control groups of HBcAg(MIR), or PBS (p<0.05, respectively) at any ratio of effector : target., Conclusion: Our results indicated MIR in HBcAg presenting platform could present MAGE-A3 multiepitopes efficiently and induced significant humoral or cellular immunity. The immune strategy based on multiepitopeimmunization could have potential for preventing or controlling MAGE-A3 associated malignant disease., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.)

Published

2017