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Viral Gastroenteritis

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Cover of 'Viral Gastroenteritis'

Table of Contents

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    Book Overview
  2. Altmetric Badge
    Chapter 1 Introduction
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    Chapter 2 Overview of viral gastroenteritis.
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    Chapter 3 Rotavirus structure: interactions between the structural proteins
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    Chapter 4 Structure and function of rotavirus nonstructural protein NSP3
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    Chapter 5 Genome rearrangements of rotaviruses.
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    Chapter 6 Structure and function of rotavirus NSP1
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    Chapter 7 Identification of the minimal replicase and the minimal promoter of (—)-strand synthesis, functional in rotavirus RNA replication in vitro
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    Chapter 8 Rotavirus protein expression is important for virus assembly and pathogenesis
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    Chapter 9 A hypothesis about the mechanism of assembly of double-shelled rotavirus particles
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    Chapter 10 Development of rotavirus molecular epidemiology: electropherotyping
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    Chapter 11 Molecular epidemiology of human rotaviruses: genogrouping by RNA-RNA hybridization
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    Chapter 12 Classification of rotavirus VP4 and VP7 serotypes
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    Chapter 13 VP4 and VP7 typing using monoclonal antibodies.
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    Chapter 14 Natural history of human rotavirus infection.
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    Chapter 15 Protective immunity against group A rotavirus infection and illness in infants
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    Chapter 16 Rotavirus immunity in the mouse
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    Chapter 17 The gnotobiotic piglet as a model for studies of disease pathogenesis and immunity to human rotaviruses.
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    Chapter 18 Jennerian and modified Jennerian approach to vaccination against rotavirus diarrhea using a quadrivalent rhesus rotavirus (RRV) and human-RRV reassortant vaccine
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    Chapter 19 Trials of oral bovine and rhesus rotavirus vaccines in Finland: a historical account and present status
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    Chapter 20 WC3 reassortant vaccines in children
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    Chapter 21 Rotavirus subunit vaccines.
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    Chapter 22 DNA vaccines against rotavirus infections
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    Chapter 23 Prophylaxis of rotavirus gastroenteritis using immunoglobulin
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    Chapter 24 Historical background and classification of caliciviruses and astroviruses
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    Chapter 25 Structure of Norwalk virus.
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    Chapter 26 Recombinant Norwalk virus-like particles as an oral vaccine
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    Chapter 27 Genetic and antigenic diversity of human caliciviruses (HuCVs) using RT-PCR and new EIAs.
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    Chapter 28 The epidemiology of human calicivirus/Sapporo/82/Japan
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    Chapter 29 Reverse transcription-polymerase chain reaction detection and sequence analysis of small round-structured viruses in Japan
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    Chapter 30 The molecular biology of astroviruses
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    Chapter 31 The changing epidemiology of astrovirus-associated gastroenteritis: a review.
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    Chapter 32 Structural features unique to enteric adenoviruses
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    Chapter 33 Closing remarks
Attention for Chapter 21: Rotavirus subunit vaccines.
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Chapter title
Rotavirus subunit vaccines.
Chapter number 21
Book title
Viral Gastroenteritis
Published in
Archives of virology Supplementum, January 1996
DOI 10.1007/978-3-7091-6553-9_21
Pubmed ID
Book ISBNs
978-3-21-182875-5, 978-3-70-916553-9
Authors

Margaret E. Conner, S. E. Crawford, C. Barone, C. O’Neal, Y.-J. Zhou, F. Fernandez, A. Parwani, L. J. Saif, J. Cohen, M. K. Estes, Conner, Margaret E., Crawford, S. E., Barone, C., O’Neal, C., Zhou, Y.-J., Fernandez, F., Parwani, A., Saif, L. J., Cohen, J., Estes, M. K.

Abstract

We evaluated rotavirus subunit vaccines for use in humans and animals. Insect cells were co-infected with combinations of individual baculovirus recombinants expressing human, bovine or simian rotavirus VP2, VP4, VP6 or VP7 to produce virus-like particles (VLPs). To determine whether immunization with VLPs could induce active protective immunity, VLPs were administered parenterally to rabbits, and the immune response and protection from rabbit ALA rotavirus challenge were evaluated. Complete or partial protection was attained, showing that parenteral immunization with VLPs induces active protective immunity. We also examined whether heterotypic immune responses could be induced with a limited number of broadly reactive VP7 proteins or with chimeric particles (multiple VP7 types on individual particles). The feasibility of this approach was determined by immunizing mice with VLPs containing a G3 VP7 or G1 VP7 and chimeric G1/G3 VLPs. Broadly reactive neutralizing antibody was induced by the G1 VLPs. VLPs also have been successfully used to boost lactogenic (colostral and milk) immunity in dairy cows. Taken together, these results show that VLPs can be effective immunogens in rabbits, mice and dairy cattle when administered parenterally, a limited number of VLPs may be sufficient to produce a broadly protective vaccine, and G3 VLPs may serve as an effective subunit vaccine for use in bovines.

Mendeley readers

Mendeley readers

The data shown below were compiled from readership statistics for 23 Mendeley readers of this research output. Click here to see the associated Mendeley record.

Geographical breakdown

Country Count As %
United States 1 4%
Unknown 22 96%

Demographic breakdown

Readers by professional status Count As %
Student > Ph. D. Student 4 17%
Researcher 4 17%
Other 3 13%
Professor 3 13%
Student > Master 2 9%
Other 3 13%
Unknown 4 17%
Readers by discipline Count As %
Agricultural and Biological Sciences 9 39%
Veterinary Science and Veterinary Medicine 2 9%
Biochemistry, Genetics and Molecular Biology 2 9%
Pharmacology, Toxicology and Pharmaceutical Science 1 4%
Environmental Science 1 4%
Other 1 4%
Unknown 7 30%