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Vaccine Design

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Cover of 'Vaccine Design'

Table of Contents

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    Book Overview
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    Chapter 1 Challenges in Veterinary Vaccine Development and Immunization.
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    Chapter 2 Development of Mycoplasma hyopneumoniae Recombinant Vaccines.
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    Chapter 3 Computational Prediction of Immunodominant Epitopes on Outer Membrane Protein (Omp) H of Pasteurella multocida Toward Designing of a Peptide Vaccine.
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    Chapter 4 DNA Vaccines Against Maedi-Visna Virus.
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    Chapter 5 Detection of Avian Antigen-Specific T Cells Induced by Viral Vaccines.
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    Chapter 6 Generation of Newcastle Disease Virus (NDV) Recombinants Expressing the Infectious Laryngotracheitis Virus (ILTV) Glycoprotein gB or gD as Dual Vaccines.
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    Chapter 7 Vaccine Design
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    Chapter 8 Development of Fasciola Vaccine in an Animal Model.
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    Chapter 9 Development of Experimental Vaccines Against Liver Flukes.
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    Chapter 10 Vaccine Design
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    Chapter 11 DNA Vaccination in Chickens.
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    Chapter 12 Selection of Vaccine Candidates for Fish Pasteurellosis Using Reverse Vaccinology and an In Vitro Screening Approach.
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    Chapter 13 Development of Vaccines Against Nocardiosis in Fishes.
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    Chapter 14 Design of an Immersion Vaccine Against Aeromonad Septicemia in Perch (Perca fluviatilis L.).
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    Chapter 15 Prokaryotic Production of Virus-Like Particle Vaccine of Betanodavirus.
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    Chapter 16 Design and Construction of Shrimp Antiviral DNA Vaccines Expressing Long and Short Hairpins for Protection by RNA Interference.
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    Chapter 17 Developing Anti-tick Vaccines.
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    Chapter 18 Host Immunization with Recombinant Proteins to Screen Antigens for Tick Control.
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    Chapter 19 Vaccinomics Approach to Tick Vaccine Development.
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    Chapter 20 Vaccine Design
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    Chapter 21 Vaccine Design
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    Chapter 22 Alphavirus-Based Vaccines.
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    Chapter 23 Vaccine Design: Replication-Defective Adenovirus Vectors.
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    Chapter 24 Generation of Lymphocytic Choriomeningitis Virus Based Vaccine Vectors.
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    Chapter 25 Production of Japanese Encephalitis Virus-Like Particles Using Insect Cell Expression Systems.
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    Chapter 26 Subunit Protein Vaccine Delivery System for Tuberculosis Based on Hepatitis B Virus Core VLP (HBc-VLP) Particles.
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    Chapter 27 Formulation Studies During Preclinical Development of Influenza Hemagglutinin and Virus-Like Particle Vaccine Candidates.
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    Chapter 28 Strategies for Vaccine Design Using Phage Display-Derived Peptides.
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    Chapter 29 Production of Well-Characterized Virus-like Particles in an Escherichia coli-Based Expression Platform for Preclinical Vaccine Assessments.
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    Chapter 30 Vaccine Design
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    Chapter 31 Vaccine Design
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    Chapter 32 Vaccine Design
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    Chapter 33 Facile Method for the Production of Recombinant Cholera Toxin B Subunit in E. coli.
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    Chapter 34 Immunoproteomic Approach for Screening Vaccine Candidates from Bacterial Outer Membrane Proteins.
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    Chapter 35 Vaccine Design
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    Chapter 36 Oral Rabies Vaccine Design for Expression in Plants.
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    Chapter 37 Purification of Virus-Like Particles (VLPs) from Plants.
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    Chapter 38 Transient Expression of Viral Proteins in Plants Using Agrobacterium tumefaciens.
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    Chapter 39 Vaccine Design
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    Chapter 40 Recombinant Botulinum Toxoids: A Practical Guide for Production.
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    Chapter 41 Preparation of Multifunctional Liposomes as a Stable Vaccine Delivery-Adjuvant System by Procedure of Emulsification-Lyophilization.
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    Chapter 42 Preparation of the Multifunctional Liposome-Containing Microneedle Arrays as an Oral Cavity Mucosal Vaccine Adjuvant-Delivery System.
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    Chapter 43 Preparation and Characterization of PLGA Encapsulated Protective Antigen Domain 4 Nanoformulation.
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    Chapter 44 Attenuated Salmonella sp. as a DNA Delivery System for Trypanosoma cruzi Antigens.
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    Chapter 45 Poly-ε-caprolactone/Chitosan and Chitosan Particles: Two Recombinant Antigen Delivery Systems for Intranasal Vaccination.
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    Chapter 46 Micro-fractional Epidermal Powder Delivery for Skin Vaccination.
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    Chapter 47 Vaccine Design
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    Chapter 48 The Web-Based DNA Vaccine Database DNAVaxDB and Its Usage for Rational DNA Vaccine Design.
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    Chapter 49 MetaMHCpan, A Meta Approach for Pan-Specific MHC Peptide Binding Prediction.
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    Chapter 50 A Cohesive and Integrated Platform for Immunogenicity Prediction.
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    Chapter 51 The Regulatory Evaluation of Vaccines for Human Use.
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    Chapter 52 Vaccines and IP Rights: A Multifaceted Relationship.
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    Chapter 53 From the Bench to the Pharmacy: Protecting Innovation During Vaccine Development and Commercialization.
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    Chapter 54 Intellectual Property in Vaccine Innovation: Impact of Recent Patent Developments.
Attention for Chapter 26: Subunit Protein Vaccine Delivery System for Tuberculosis Based on Hepatitis B Virus Core VLP (HBc-VLP) Particles.
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Chapter title
Subunit Protein Vaccine Delivery System for Tuberculosis Based on Hepatitis B Virus Core VLP (HBc-VLP) Particles.
Chapter number 26
Book title
Vaccine Design
Published in
Methods in molecular biology, January 2016
DOI 10.1007/978-1-4939-3389-1_26
Pubmed ID
Book ISBNs
978-1-4939-3388-4, 978-1-4939-3389-1
Authors

Dhananjayan Dhanasooraj, R. Ajay Kumar, Sathish Mundayoor

Editors

Sunil Thomas

Abstract

Despite the development of modern medicine, tuberculosis (TB), caused by the pathogenic bacterium, Mycobacterium tuberculosis (Mtb), remains one of the deadliest diseases. This bacterium can lay dormant in individuals and get activated when immunity goes down and has also shown considerable prowess in mutating into drug resistant forms. The global emergence of such drug resistant Mtb and the lack of efficacy of Bacille Calmette Guérin (BCG), the only vaccine available so far, have resulted in a situation which cries out for a safe and effective tuberculosis vaccine.Number of different strategies has been used for developing new anti-TB vaccines and several protective antigens have been identified so far. One strategy, the use of protein subunits, has the potential to develop into a powerful tuberculosis vaccine, not only because of its efficacy and safety, but also because they are economical. The proper delivery of protein subunit vaccines with adjuvants or novel delivery systems is necessary for inducing protective immune responses. The available adjuvants or delivery systems are inadequate for generating such a response. In the present method, we have constructed a vaccine delivery system for tuberculosis based on Virus-Like Particles (VLPs). Hepatitis B Virus core antigen gene was recombinantly modified using Overlap Extension PCR (OEPCR). The final construct was designed to express HBc-VLP carrying external antigen (fusion VLP). Mycobacterium tuberculosis antigen CFP-10 was used for the construction of fusion VLP. The recombinant gene for the construct was cloned into a pET expression system and transformed into E. coli BL21(DE3) and induced with IPTG to express the protein. The fusion protein was purified using the Histidine tag and allowed to form VLPs. The preformed VLPs were purified by sucrose density gradient centrifugation. The VLPs were characterized using Transmission Electron Microscopy (TEM).

Mendeley readers

Mendeley readers

The data shown below were compiled from readership statistics for 34 Mendeley readers of this research output. Click here to see the associated Mendeley record.

Geographical breakdown

Country Count As %
Canada 1 3%
Unknown 33 97%

Demographic breakdown

Readers by professional status Count As %
Student > Bachelor 8 24%
Student > Master 4 12%
Student > Doctoral Student 3 9%
Student > Ph. D. Student 3 9%
Other 2 6%
Other 5 15%
Unknown 9 26%
Readers by discipline Count As %
Medicine and Dentistry 8 24%
Biochemistry, Genetics and Molecular Biology 7 21%
Agricultural and Biological Sciences 4 12%
Nursing and Health Professions 1 3%
Immunology and Microbiology 1 3%
Other 4 12%
Unknown 9 26%