A gastrointestinal rotavirus infection mouse model for immune modulation studies

A gastrointestinal rotavirus infection mouse model for immune modulation studies

<p>Abstract</p> <p>Background</p> <p>Rotaviruses are the single most important cause of severe diarrhea in young children worldwide. The current study was conducted to assess whether colostrum containing rotavirus-specific antibodies (Gastrogard-R<sup>®</sup>...

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Main Authors: van Amerongen Geert, Crienen Annelies, McNeal Monica M, Knipping Karen, Garssen Johan, van't Land Belinda
Format: Article
Language:English
Published: BMC 2011-03-01
Series:Virology Journal
Online Access:http://www.virologyj.com/content/8/1/109
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spelling doaj-1145cdd58bda4785bb28f4c98b3231dd2020-11-24T21:32:57ZengBMCVirology Journal1743-422X2011-03-018110910.1186/1743-422X-8-109A gastrointestinal rotavirus infection mouse model for immune modulation studiesvan Amerongen GeertCrienen AnneliesMcNeal Monica MKnipping KarenGarssen Johanvan't Land Belinda<p>Abstract</p> <p>Background</p> <p>Rotaviruses are the single most important cause of severe diarrhea in young children worldwide. The current study was conducted to assess whether colostrum containing rotavirus-specific antibodies (Gastrogard-R<sup>®</sup>) could protect against rotavirus infection. In addition, this illness model was used to study modulatory effects of intervention on several immune parameters after re-infection.</p> <p>Methods</p> <p>BALB/c mice were treated by gavage once daily with Gastrogard-R<sup>® </sup>from the age of 4 to 10 days, and were inoculated with rhesus rotavirus (RRV) at 7 days of age. A secondary inoculation with epizootic-diarrhea infant-mouse (EDIM) virus was administered at 17 days of age. Disease symptoms were scored daily and viral shedding was measured in fecal samples during the post-inoculation periods. Rotavirus-specific IgM, IgG and IgG subclasses in serum, T cell proliferation and rotavirus-specific delayed-type hypersensitivity (DTH) responses were also measured.</p> <p>Results</p> <p>Primary inoculation with RRV induced a mild but consistent level of diarrhea during 3-4 days post-inoculation. All mice receiving Gastrogard-R<sup>® </sup>were 100% protected against rotavirus-induced diarrhea. Mice receiving both RRV and EDIM inoculation had a lower faecal-viral load following EDIM inoculation then mice receiving EDIM alone or Gastrogard-R<sup>®</sup>. Mice receiving Gastrogard-R<sup>® </sup>however displayed an enhanced rotavirus-specific T-cell proliferation whereas rotavirus-specific antibody subtypes were not affected.</p> <p>Conclusions</p> <p>Preventing RRV-induced diarrhea by Gastrogard-R<sup>® </sup>early in life showed a diminished protection against EDIM re-infection, but a rotavirus-specific immune response was developed including both B cell and T cell responses. In general, this intervention model can be used for studying clinical symptoms as well as the immune responses required for protection against viral re-infection.</p> http://www.virologyj.com/content/8/1/109
collection DOAJ
language English
format Article
sources DOAJ
author van Amerongen Geert
Crienen Annelies
McNeal Monica M
Knipping Karen
Garssen Johan
van't Land Belinda
spellingShingle van Amerongen Geert
Crienen Annelies
McNeal Monica M
Knipping Karen
Garssen Johan
van't Land Belinda
A gastrointestinal rotavirus infection mouse model for immune modulation studies
Virology Journal
author_facet van Amerongen Geert
Crienen Annelies
McNeal Monica M
Knipping Karen
Garssen Johan
van't Land Belinda
author_sort van Amerongen Geert
title A gastrointestinal rotavirus infection mouse model for immune modulation studies
title_short A gastrointestinal rotavirus infection mouse model for immune modulation studies
title_full A gastrointestinal rotavirus infection mouse model for immune modulation studies
title_fullStr A gastrointestinal rotavirus infection mouse model for immune modulation studies
title_full_unstemmed A gastrointestinal rotavirus infection mouse model for immune modulation studies
title_sort gastrointestinal rotavirus infection mouse model for immune modulation studies
publisher BMC
series Virology Journal
issn 1743-422X
publishDate 2011-03-01
description <p>Abstract</p> <p>Background</p> <p>Rotaviruses are the single most important cause of severe diarrhea in young children worldwide. The current study was conducted to assess whether colostrum containing rotavirus-specific antibodies (Gastrogard-R<sup>®</sup>) could protect against rotavirus infection. In addition, this illness model was used to study modulatory effects of intervention on several immune parameters after re-infection.</p> <p>Methods</p> <p>BALB/c mice were treated by gavage once daily with Gastrogard-R<sup>® </sup>from the age of 4 to 10 days, and were inoculated with rhesus rotavirus (RRV) at 7 days of age. A secondary inoculation with epizootic-diarrhea infant-mouse (EDIM) virus was administered at 17 days of age. Disease symptoms were scored daily and viral shedding was measured in fecal samples during the post-inoculation periods. Rotavirus-specific IgM, IgG and IgG subclasses in serum, T cell proliferation and rotavirus-specific delayed-type hypersensitivity (DTH) responses were also measured.</p> <p>Results</p> <p>Primary inoculation with RRV induced a mild but consistent level of diarrhea during 3-4 days post-inoculation. All mice receiving Gastrogard-R<sup>® </sup>were 100% protected against rotavirus-induced diarrhea. Mice receiving both RRV and EDIM inoculation had a lower faecal-viral load following EDIM inoculation then mice receiving EDIM alone or Gastrogard-R<sup>®</sup>. Mice receiving Gastrogard-R<sup>® </sup>however displayed an enhanced rotavirus-specific T-cell proliferation whereas rotavirus-specific antibody subtypes were not affected.</p> <p>Conclusions</p> <p>Preventing RRV-induced diarrhea by Gastrogard-R<sup>® </sup>early in life showed a diminished protection against EDIM re-infection, but a rotavirus-specific immune response was developed including both B cell and T cell responses. In general, this intervention model can be used for studying clinical symptoms as well as the immune responses required for protection against viral re-infection.</p>
url http://www.virologyj.com/content/8/1/109
work_keys_str_mv AT vanamerongengeert agastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT crienenannelies agastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT mcnealmonicam agastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT knippingkaren agastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT garssenjohan agastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT vantlandbelinda agastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT vanamerongengeert gastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT crienenannelies gastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT mcnealmonicam gastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT knippingkaren gastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT garssenjohan gastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
AT vantlandbelinda gastrointestinalrotavirusinfectionmousemodelforimmunemodulationstudies
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