Adoptive transfer of EBV specific CD8+ T cell clones can transiently control EBV infection in humanized mice.
Epstein Barr virus (EBV) infection expands CD8+ T cells specific for lytic antigens to high frequencies during symptomatic primary infection, and maintains these at significant numbers during persistence. Despite this, the protective function of these lytic EBV antigen-specific cytotoxic CD8+ T cell...
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2014-08-01
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doaj-e25caa9499d24c2d95619727227fe2222021-04-21T17:53:35ZengPublic Library of Science (PLoS)PLoS Pathogens1553-73661553-73742014-08-01108e100433310.1371/journal.ppat.1004333Adoptive transfer of EBV specific CD8+ T cell clones can transiently control EBV infection in humanized mice.Olga AntsiferovaAnne MüllerPatrick C RämerObinna ChijiokeBithi ChatterjeeAna RaykovaRaquel PlanasMireia SospedraAnatoliy ShumilovMing-Han TsaiHenri-Jacques DelecluseChristian MünzEpstein Barr virus (EBV) infection expands CD8+ T cells specific for lytic antigens to high frequencies during symptomatic primary infection, and maintains these at significant numbers during persistence. Despite this, the protective function of these lytic EBV antigen-specific cytotoxic CD8+ T cells remains unclear. Here we demonstrate that lytic EBV replication does not significantly contribute to virus-induced B cell proliferation in vitro and in vivo in a mouse model with reconstituted human immune system components (huNSG mice). However, we report a trend to reduction of EBV-induced lymphoproliferation outside of lymphoid organs upon diminished lytic replication. Moreover, we could demonstrate that CD8+ T cells against the lytic EBV antigen BMLF1 can eliminate lytically replicating EBV-transformed B cells from lymphoblastoid cell lines (LCLs) and in vivo, thereby transiently controlling high viremia after adoptive transfer into EBV infected huNSG mice. These findings suggest a protective function for lytic EBV antigen-specific CD8+ T cells against EBV infection and against virus-associated tumors in extra-lymphoid organs. These specificities should be explored for EBV-specific vaccine development.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/25165855/?tool=EBI |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Olga Antsiferova Anne Müller Patrick C Rämer Obinna Chijioke Bithi Chatterjee Ana Raykova Raquel Planas Mireia Sospedra Anatoliy Shumilov Ming-Han Tsai Henri-Jacques Delecluse Christian Münz |
spellingShingle |
Olga Antsiferova Anne Müller Patrick C Rämer Obinna Chijioke Bithi Chatterjee Ana Raykova Raquel Planas Mireia Sospedra Anatoliy Shumilov Ming-Han Tsai Henri-Jacques Delecluse Christian Münz Adoptive transfer of EBV specific CD8+ T cell clones can transiently control EBV infection in humanized mice. PLoS Pathogens |
author_facet |
Olga Antsiferova Anne Müller Patrick C Rämer Obinna Chijioke Bithi Chatterjee Ana Raykova Raquel Planas Mireia Sospedra Anatoliy Shumilov Ming-Han Tsai Henri-Jacques Delecluse Christian Münz |
author_sort |
Olga Antsiferova |
title |
Adoptive transfer of EBV specific CD8+ T cell clones can transiently control EBV infection in humanized mice. |
title_short |
Adoptive transfer of EBV specific CD8+ T cell clones can transiently control EBV infection in humanized mice. |
title_full |
Adoptive transfer of EBV specific CD8+ T cell clones can transiently control EBV infection in humanized mice. |
title_fullStr |
Adoptive transfer of EBV specific CD8+ T cell clones can transiently control EBV infection in humanized mice. |
title_full_unstemmed |
Adoptive transfer of EBV specific CD8+ T cell clones can transiently control EBV infection in humanized mice. |
title_sort |
adoptive transfer of ebv specific cd8+ t cell clones can transiently control ebv infection in humanized mice. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS Pathogens |
issn |
1553-7366 1553-7374 |
publishDate |
2014-08-01 |
description |
Epstein Barr virus (EBV) infection expands CD8+ T cells specific for lytic antigens to high frequencies during symptomatic primary infection, and maintains these at significant numbers during persistence. Despite this, the protective function of these lytic EBV antigen-specific cytotoxic CD8+ T cells remains unclear. Here we demonstrate that lytic EBV replication does not significantly contribute to virus-induced B cell proliferation in vitro and in vivo in a mouse model with reconstituted human immune system components (huNSG mice). However, we report a trend to reduction of EBV-induced lymphoproliferation outside of lymphoid organs upon diminished lytic replication. Moreover, we could demonstrate that CD8+ T cells against the lytic EBV antigen BMLF1 can eliminate lytically replicating EBV-transformed B cells from lymphoblastoid cell lines (LCLs) and in vivo, thereby transiently controlling high viremia after adoptive transfer into EBV infected huNSG mice. These findings suggest a protective function for lytic EBV antigen-specific CD8+ T cells against EBV infection and against virus-associated tumors in extra-lymphoid organs. These specificities should be explored for EBV-specific vaccine development. |
url |
https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/25165855/?tool=EBI |
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