The production of antibody by invading B cells is required for the clearance of rabies virus from the central nervous system.

The production of antibody by invading B cells is required for the clearance of rabies virus from the central nervous system.

The pathogenesis of rabies is associated with the inability to deliver immune effectors across the blood-brain barrier and to clear virulent rabies virus from CNS tissues. However, the mechanisms that facilitate immune effector entry into CNS tissues are induced by infection with attenuated rabies v...

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Main Authors: D Craig Hooper, Timothy W Phares, Marzena J Fabis, Anirban Roy
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2009-10-01
Series:PLoS Neglected Tropical Diseases
Online Access:http://europepmc.org/articles/PMC2754506?pdf=render
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spelling doaj-16aef94df1964848ab361647f19e63102020-11-24T20:45:00ZengPublic Library of Science (PLoS)PLoS Neglected Tropical Diseases1935-27271935-27352009-10-01310e53510.1371/journal.pntd.0000535The production of antibody by invading B cells is required for the clearance of rabies virus from the central nervous system.D Craig HooperTimothy W PharesMarzena J FabisAnirban RoyThe pathogenesis of rabies is associated with the inability to deliver immune effectors across the blood-brain barrier and to clear virulent rabies virus from CNS tissues. However, the mechanisms that facilitate immune effector entry into CNS tissues are induced by infection with attenuated rabies virus.Infection of normal mice with attenuated rabies virus but not immunization with killed virus can promote the clearance of pathogenic rabies virus from the CNS. T cell activity in B cell-deficient mice can control the replication of attenuated virus in the CNS, but viral mRNA persists. Low levels of passively administered rabies virus-neutralizing antibody reach infected cells in the cerebellum of B cell-deficient mice but are not sufficient to mediate virus clearance. Production of rabies virus-specific antibody by B cells invading CNS tissues is required for this process, and a substantial proportion of the B cells that accumulate in the CNS of mice infected with attenuated rabies virus produce virus-specific antibodies.The mechanisms required for immune effectors to enter rabies virus-infected tissues are induced by infection with attenuated rabies virus but not by infection with pathogenic rabies viruses or immunization with killed virus. T cell activities can inhibit rabies virus replication, but the production of rabies virus-specific antibodies by infiltrating B cells, as opposed to the leakage of circulating antibody across the BBB, is critical to elimination of the virus. These findings suggest that a pathogenic rabies virus infection may be treatable after the virus has reached the CNS tissues, providing that the appropriate immune effectors can be targeted to the infected tissues.http://europepmc.org/articles/PMC2754506?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author D Craig Hooper
Timothy W Phares
Marzena J Fabis
Anirban Roy
spellingShingle D Craig Hooper
Timothy W Phares
Marzena J Fabis
Anirban Roy
The production of antibody by invading B cells is required for the clearance of rabies virus from the central nervous system.
PLoS Neglected Tropical Diseases
author_facet D Craig Hooper
Timothy W Phares
Marzena J Fabis
Anirban Roy
author_sort D Craig Hooper
title The production of antibody by invading B cells is required for the clearance of rabies virus from the central nervous system.
title_short The production of antibody by invading B cells is required for the clearance of rabies virus from the central nervous system.
title_full The production of antibody by invading B cells is required for the clearance of rabies virus from the central nervous system.
title_fullStr The production of antibody by invading B cells is required for the clearance of rabies virus from the central nervous system.
title_full_unstemmed The production of antibody by invading B cells is required for the clearance of rabies virus from the central nervous system.
title_sort production of antibody by invading b cells is required for the clearance of rabies virus from the central nervous system.
publisher Public Library of Science (PLoS)
series PLoS Neglected Tropical Diseases
issn 1935-2727
1935-2735
publishDate 2009-10-01
description The pathogenesis of rabies is associated with the inability to deliver immune effectors across the blood-brain barrier and to clear virulent rabies virus from CNS tissues. However, the mechanisms that facilitate immune effector entry into CNS tissues are induced by infection with attenuated rabies virus.Infection of normal mice with attenuated rabies virus but not immunization with killed virus can promote the clearance of pathogenic rabies virus from the CNS. T cell activity in B cell-deficient mice can control the replication of attenuated virus in the CNS, but viral mRNA persists. Low levels of passively administered rabies virus-neutralizing antibody reach infected cells in the cerebellum of B cell-deficient mice but are not sufficient to mediate virus clearance. Production of rabies virus-specific antibody by B cells invading CNS tissues is required for this process, and a substantial proportion of the B cells that accumulate in the CNS of mice infected with attenuated rabies virus produce virus-specific antibodies.The mechanisms required for immune effectors to enter rabies virus-infected tissues are induced by infection with attenuated rabies virus but not by infection with pathogenic rabies viruses or immunization with killed virus. T cell activities can inhibit rabies virus replication, but the production of rabies virus-specific antibodies by infiltrating B cells, as opposed to the leakage of circulating antibody across the BBB, is critical to elimination of the virus. These findings suggest that a pathogenic rabies virus infection may be treatable after the virus has reached the CNS tissues, providing that the appropriate immune effectors can be targeted to the infected tissues.
url http://europepmc.org/articles/PMC2754506?pdf=render
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