About: Abstract The presence of maternal antibodies protected suckling C57BL/6 mice from the clinical manifestations of the acute encephalomyelitis caused by mouse hepatitis virus, strain JHM (MHV-JHM), a coronavirus, even though histological evidence of encephalomyelitis was found at early times after inoculation. 100% of infected suckling mice developed a fatal disease in the absence of maternal antibody. By 14 days after inoculation, the brains of all antibody-protected mice examined were nearly normal on histological examination. At 3–8 weeks post-inoculation, approximately 40% of the antibody-protected mice developed a neurological disease characterized by hindlimb paralysis and wasting. Evidence of inflammation and demyelination was apparent in the spinal cord and brainstem. The mice that remained asymptomatic at this time showed few signs of inflammation and none developed clinical disease over the following 9 months. Viral antigen could be detected in most of the mice examined at all times after inoculation, whether symptomatic or not, and was particularly evident in the animals with hindlimb paralysis. MHV-JHM could be consistently cultured from the mice with hindlimb paralysis. These results show that maternal immune factors can completely protect susceptible mice from the acute, fatal, clinical encephalomyelitis caused by MHV-JHM, but cannot prevent the establishment of a latent state and subsequent development of virus-induced, clinically evident, demyelinating disease. This model will be useful for studying the virus and host factors important for the development of MHV-JHM latency and subsequent virus-induced demyelination.

Facets (new session)
Description
Metadata
Settings
- owl:sameAs
- Inference Rule:

About: Abstract The presence of maternal antibodies protected suckling C57BL/6 mice from the clinical manifestations of the acute encephalomyelitis caused by mouse hepatitis virus, strain JHM (MHV-JHM), a coronavirus, even though histological evidence of encephalomyelitis was found at early times after inoculation. 100% of infected suckling mice developed a fatal disease in the absence of maternal antibody. By 14 days after inoculation, the brains of all antibody-protected mice examined were nearly normal on histological examination. At 3–8 weeks post-inoculation, approximately 40% of the antibody-protected mice developed a neurological disease characterized by hindlimb paralysis and wasting. Evidence of inflammation and demyelination was apparent in the spinal cord and brainstem. The mice that remained asymptomatic at this time showed few signs of inflammation and none developed clinical disease over the following 9 months. Viral antigen could be detected in most of the mice examined at all times after inoculation, whether symptomatic or not, and was particularly evident in the animals with hindlimb paralysis. MHV-JHM could be consistently cultured from the mice with hindlimb paralysis. These results show that maternal immune factors can completely protect susceptible mice from the acute, fatal, clinical encephalomyelitis caused by MHV-JHM, but cannot prevent the establishment of a latent state and subsequent development of virus-induced, clinically evident, demyelinating disease. This model will be useful for studying the virus and host factors important for the development of MHV-JHM latency and subsequent virus-induced demyelination. Goto Sponge NotDistinct Permalink

An Entity of Type : fabio:Abstract, within Data Space : wasabi.inria.fr associated with source document(s)

Attributes	Values
type	abstract
value	Abstract The presence of maternal antibodies protected suckling C57BL/6 mice from the clinical manifestations of the acute encephalomyelitis caused by mouse hepatitis virus, strain JHM (MHV-JHM), a coronavirus, even though histological evidence of encephalomyelitis was found at early times after inoculation. 100% of infected suckling mice developed a fatal disease in the absence of maternal antibody. By 14 days after inoculation, the brains of all antibody-protected mice examined were nearly normal on histological examination. At 3–8 weeks post-inoculation, approximately 40% of the antibody-protected mice developed a neurological disease characterized by hindlimb paralysis and wasting. Evidence of inflammation and demyelination was apparent in the spinal cord and brainstem. The mice that remained asymptomatic at this time showed few signs of inflammation and none developed clinical disease over the following 9 months. Viral antigen could be detected in most of the mice examined at all times after inoculation, whether symptomatic or not, and was particularly evident in the animals with hindlimb paralysis. MHV-JHM could be consistently cultured from the mice with hindlimb paralysis. These results show that maternal immune factors can completely protect susceptible mice from the acute, fatal, clinical encephalomyelitis caused by MHV-JHM, but cannot prevent the establishment of a latent state and subsequent development of virus-induced, clinically evident, demyelinating disease. This model will be useful for studying the virus and host factors important for the development of MHV-JHM latency and subsequent virus-induced demyelination.
Subject	Pathology Immunology Mice Antibodies Rodents Animals bred for albinism on a large scale Inflammatory diseases of the central nervous system Mammal common names
part of	Late onset, symptomatic, demyelinating encephalomyelitis in mice infected with MHV-JHM in the presence of maternal antibody
is abstract of	Late onset, symptomatic, demyelinating encephalomyelitis in mice infected with MHV-JHM in the presence of maternal antibody
is hasSource of	covid:ann/target/9e8860a7bad5b5207702f08082f880ee0de0ef1a covid:ann/target/453508bae16d7f68d15a2ec0875859decb62d3f8 covid:ann/target/85e8f283862b148861309da06780dd718e4d6ab0 covid:ann/target/6020b85d72dc82acd738b31ff0e027a7cc09c553 covid:ann/target/2863af31346096ce1ae6d33d627851b32ae388ae covid:ann/target/6ac8a8adb0a4c8e4acb48122f7d93114ec70b9ae covid:ann/target/deeb1470d2b3e026e8dd2b04da3a21d2dd93fe41 covid:ann/target/c4b29058a2dde9f1e5a7f457a7850a3668c26a77 covid:ann/target/81740b9dcc04dd017aad0bc83ea70f0086fbb169 covid:ann/target/26395f6836dba4806a77561fc1349bb793df9ad2 covid:ann/target/48be658f56a3e052ce8fc5beb4e574c82b301768 covid:ann/target/6a1a32b3e85356a02ba8cd3c8f5cd77d3ca2675a covid:ann/target/5ac26f940a6cb070ac2c8ae292cefc375d6eba72 covid:ann/target/8763687e022492ffbbdc6683a7a6fe1449eb9d4e covid:ann/target/fa97cf5fd1ba7252652f2e71212b78c85b04a476 covid:ann/target/574e7c8d01f29e50753f83ebd61c18f3eb6ee2b3 covid:ann/target/d31e2a8ae61380dc2f6aca7a226ca2cf007a6b0d covid:ann/target/476c6026808eb00620805679dbfd5aed2b07bfc2 covid:ann/target/860ef30560e1972f4af1390429426ae073f5f0c1 covid:ann/target/a36176cf5446ab072e99ae6df9936889f8e6445a covid:ann/target/ee558e311048fa815a46e41c928ba41b2db87571 covid:ann/target/8fe02b1563e148756eeae826b670291ed21f3dc1 covid:ann/target/c4ad0ba7d2da62199b0f9fa4ec7ebabe4468d6da covid:ann/target/e4cf68ab4917f16df3b898d8a05b86be6e299291 covid:ann/target/2d4ee5fb79a2c1f7b9fd4e56e5939ab1e5c77eff

Faceted Search & Find service v1.13.91 as of Mar 24 2020

Alternative Linked Data Documents: Sponger | ODE Content Formats:

RDF

ODATA

Microdata

About

OpenLink Virtuoso version 07.20.3229 as of Jul 10 2020, on Linux (x86_64-pc-linux-gnu), Single-Server Edition (94 GB total memory)
Data on this page belongs to its respective rights holders.
Virtuoso Faceted Browser Copyright © 2009-2025 OpenLink Software