In vivo and in vitro models of demyelinating disease. XVII. The infectious process in athymic rats inoculated with JHM virus
Identifieur interne : 001D17 ( Main/Exploration ); précédent : 001D16; suivant : 001D18In vivo and in vitro models of demyelinating disease. XVII. The infectious process in athymic rats inoculated with JHM virus
Auteurs : O. Sorensen [Canada] ; A. Saravani [Canada] ; S. Dales [Canada]Source :
- Microbial Pathogenesis [ 0882-4010 ] ; 1987.
English descriptors
- Teeft :
- Acta neuropathol, Asymptomatic, Athymic, Athymic rats, Athymic rats inoculated, Cdna probes, Cell functions, Cellular, Cellular immunity, Cerebellum, Clin lmmunol lmmunopathol, Clinical symptoms, Demyelinating, Demyelinating disease, Demyelinating diseases, Disease process, Disease symptoms, Euthymic, Euthymic animals, Euthymic rats, Extensive destruction, Extensive infiltration, Heterozygous, Hind limbs, Hippocampal neurons, Hybridization, Infectious process, Infiltrates, Inoculated, Inoculation, Jhmv, Jhmv infection, Latency period, Lateral ventricle, Lesion, Microbial pathogenesis, Mononuclear, Mononuclear cells, Myelencephalon, Natural cytotoxicity, Neuron, Nude rats, Nude rats inoculated, Older rats, Paralysed, Present data, Primary explants, Rat, Rats inoculated, Sorensen, Spinal, Spinal cord, Target cells, Tissue damage, Tissue sections, Various ages, Virus infection, White matter, Wistar lewis.
Abstract
Abstract: Wistar Lewis (WL), Long Evans (LE) and other rat strains develop complete resistance to CNS disease when inoculated intracerebrally with murine hepatitis JHM virus (JHMV) after the 10th day of age.11Sorensen O, Percy D, Dales S. In vivo and in vitro models of demyelinating diseases. III. JHM virus infection of rats. Arch Neurol 1980; 37: 478-84. Two types of studies were conducted to ascertain the involvement of the cellular immune system in development of resistance. Immunosuppression of WL rats with cyclosporin A (CsA) following onset of the age-related resistance demonstrated that this drug was partially able to abrogate resistance. In the other studies nude (rnu/rnu) rats, their heterozygous (rnu/+) litter mates and genetically related LE rats of various ages were challenged with JHMV. The rnu/+ and LE animals became completely resistant before the age of weaning, whereas some rnu/rnu rats, challenged as late as 70 days of age, showed disease symptoms—albeit after a long latent period. These observations indicated that the cellular immune system plays an important role in suppressing the disease process in the CNS. When the infection of nude rats was initiated on or after the 15th day of life, the histological lesions were generally small and present in both grey and white matter but were seldom seen in the spinal cord. Mononuclear infiltrates were evident throughout the CNS. In some nude rats there was massive mononuclear cell infiltration towards the meningies and into ventricular spaces. By contrast in rnu/+, LE and WL rats with late-onset disease symptoms, demyelinating-type lesions were confined to the white matter and only minor infiltration of mononuclear cells was evident. JHMV RNA was detectable by dot-blotting analysis in the CNS of both paralysed and asymptomatic rnu/rnu and rnu/+ rats, but less RNA was usually detected in heterozygous animals. In-situ hybridization with cDNA probes for JHMV RNA showed that neurons in the hippocampus and cerebellum, as well as cells in the white matter, were frequently infected. The present data indicate that in the rat T cells have an important function in maintaining resistance to the JHMV related disease process. However, even without a functional T cell compartment nude rats challenged after 15 days of age did not develop an acute encephalitis, suggesting that an age-dependent, non-immunological mechanism is also involved in restricting the spread of infection. It is possible that resistance in euthymic rats sets in because: (1) at the time of weaning the CNS matures, so that the number of targets available for infection is reduced, (2) T cells prevent the late-onset disease by clearing persistent, low grade infections from the CNS.
Url:
DOI: 10.1016/0882-4010(87)90100-8
Affiliations:
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XVII. The infectious process in athymic rats inoculated with JHM virus</title><author><name sortKey="Sorensen, O" sort="Sorensen, O" uniqKey="Sorensen O" first="O." last="Sorensen">O. Sorensen</name><affiliation wicri:level="1"><country>Canada</country><wicri:regionArea>Cytobiology Group, Department of Microbiology and Immunology, University of Western Ontario, London, Ontario</wicri:regionArea><wicri:noRegion>Ontario</wicri:noRegion></affiliation></author><author><name sortKey="Saravani, A" sort="Saravani, A" uniqKey="Saravani A" first="A." last="Saravani">A. Saravani</name><affiliation wicri:level="1"><country>Canada</country><wicri:regionArea>Cytobiology Group, Department of Microbiology and Immunology, University of Western Ontario, London, Ontario</wicri:regionArea><wicri:noRegion>Ontario</wicri:noRegion></affiliation></author><author><name sortKey="Dales, S" sort="Dales, S" uniqKey="Dales S" first="S." last="Dales">S. Dales</name><affiliation wicri:level="1"><country>Canada</country><wicri:regionArea>Cytobiology Group, Department of Microbiology and Immunology, University of Western Ontario, London, Ontario</wicri:regionArea><wicri:noRegion>Ontario</wicri:noRegion></affiliation></author></analytic><monogr></monogr><series><title level="j">Microbial Pathogenesis</title><title level="j" type="abbrev">YMPAT</title><idno type="ISSN">0882-4010</idno><imprint><publisher>ELSEVIER</publisher><date type="published" when="1987">1987</date><biblScope unit="volume">2</biblScope><biblScope unit="issue">2</biblScope><biblScope unit="page" from="79">79</biblScope><biblScope unit="page" to="90">90</biblScope></imprint><idno type="ISSN">0882-4010</idno></series></biblStruct></sourceDesc><seriesStmt><idno type="ISSN">0882-4010</idno></seriesStmt></fileDesc><profileDesc><textClass><keywords scheme="Teeft" xml:lang="en"><term>Acta neuropathol</term><term>Asymptomatic</term><term>Athymic</term><term>Athymic rats</term><term>Athymic rats inoculated</term><term>Cdna probes</term><term>Cell functions</term><term>Cellular</term><term>Cellular immunity</term><term>Cerebellum</term><term>Clin lmmunol lmmunopathol</term><term>Clinical symptoms</term><term>Demyelinating</term><term>Demyelinating disease</term><term>Demyelinating diseases</term><term>Disease process</term><term>Disease symptoms</term><term>Euthymic</term><term>Euthymic animals</term><term>Euthymic rats</term><term>Extensive destruction</term><term>Extensive infiltration</term><term>Heterozygous</term><term>Hind limbs</term><term>Hippocampal neurons</term><term>Hybridization</term><term>Infectious process</term><term>Infiltrates</term><term>Inoculated</term><term>Inoculation</term><term>Jhmv</term><term>Jhmv infection</term><term>Latency period</term><term>Lateral ventricle</term><term>Lesion</term><term>Microbial pathogenesis</term><term>Mononuclear</term><term>Mononuclear cells</term><term>Myelencephalon</term><term>Natural cytotoxicity</term><term>Neuron</term><term>Nude rats</term><term>Nude rats inoculated</term><term>Older rats</term><term>Paralysed</term><term>Present data</term><term>Primary explants</term><term>Rat</term><term>Rats inoculated</term><term>Sorensen</term><term>Spinal</term><term>Spinal cord</term><term>Target cells</term><term>Tissue damage</term><term>Tissue sections</term><term>Various ages</term><term>Virus infection</term><term>White matter</term><term>Wistar lewis</term></keywords></textClass><langUsage><language ident="en">en</language></langUsage></profileDesc></teiHeader><front><div type="abstract" xml:lang="en">Abstract: Wistar Lewis (WL), Long Evans (LE) and other rat strains develop complete resistance to CNS disease when inoculated intracerebrally with murine hepatitis JHM virus (JHMV) after the 10th day of age.11Sorensen O, Percy D, Dales S. In vivo and in vitro models of demyelinating diseases. III. JHM virus infection of rats. Arch Neurol 1980; 37: 478-84. Two types of studies were conducted to ascertain the involvement of the cellular immune system in development of resistance. Immunosuppression of WL rats with cyclosporin A (CsA) following onset of the age-related resistance demonstrated that this drug was partially able to abrogate resistance. In the other studies nude (rnu/rnu) rats, their heterozygous (rnu/+) litter mates and genetically related LE rats of various ages were challenged with JHMV. The rnu/+ and LE animals became completely resistant before the age of weaning, whereas some rnu/rnu rats, challenged as late as 70 days of age, showed disease symptoms—albeit after a long latent period. These observations indicated that the cellular immune system plays an important role in suppressing the disease process in the CNS. When the infection of nude rats was initiated on or after the 15th day of life, the histological lesions were generally small and present in both grey and white matter but were seldom seen in the spinal cord. Mononuclear infiltrates were evident throughout the CNS. In some nude rats there was massive mononuclear cell infiltration towards the meningies and into ventricular spaces. By contrast in rnu/+, LE and WL rats with late-onset disease symptoms, demyelinating-type lesions were confined to the white matter and only minor infiltration of mononuclear cells was evident. JHMV RNA was detectable by dot-blotting analysis in the CNS of both paralysed and asymptomatic rnu/rnu and rnu/+ rats, but less RNA was usually detected in heterozygous animals. In-situ hybridization with cDNA probes for JHMV RNA showed that neurons in the hippocampus and cerebellum, as well as cells in the white matter, were frequently infected. The present data indicate that in the rat T cells have an important function in maintaining resistance to the JHMV related disease process. However, even without a functional T cell compartment nude rats challenged after 15 days of age did not develop an acute encephalitis, suggesting that an age-dependent, non-immunological mechanism is also involved in restricting the spread of infection. It is possible that resistance in euthymic rats sets in because: (1) at the time of weaning the CNS matures, so that the number of targets available for infection is reduced, (2) T cells prevent the late-onset disease by clearing persistent, low grade infections from the CNS.</div></front></TEI><affiliations><list><country><li>Canada</li></country></list><tree><country name="Canada"><noRegion><name sortKey="Sorensen, O" sort="Sorensen, O" uniqKey="Sorensen O" first="O." last="Sorensen">O. Sorensen</name></noRegion><name sortKey="Dales, S" sort="Dales, S" uniqKey="Dales S" first="S." last="Dales">S. Dales</name><name sortKey="Saravani, A" sort="Saravani, A" uniqKey="Saravani A" first="A." last="Saravani">A. Saravani</name></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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