1976

DOI: 10.1177/030098587601300105

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Naturally-Occurring Sendai Virus Infection of Athymic Nude Mice

¹

,

David P. Houchens

²

,

Michael J. Collins

³

et al.

Abstract: Abstract. Nude (nulnu) mice, Balb/c-derived, responded to a naturally-occurring Sendai virus infection in a different manner than conventional mice. They developed a chronic debilitating disease and a persistent viral infection of the respiratory tract with intranuclear inclusion bodies in tracheal, bronchial and bronchiolar epithelial cells, laryngeal and tracheal glandular epithelium and in type I and I1 alveolar cells. The infection was identified by serologic and tissue culture studies, the mouse antibody … Show more

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1977

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Cited by 44 publications

(30 citation statements)

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“…Sendai virus infection has been well described for mice (11)(12)(13), and recently the course of experimental infection in the rat has been reported (14). Sendai There are numerous systemic effects (Thble 1) that toxicologists and pathologists need to consider when interpreting the impact of Sendai virus infection upon study results (10,15).…”

Section: The Pathogenesis Of Natural and Experimentalmentioning

confidence: 99%

Infectious Diseases of the Upper Respiratory Tract: Implications for Toxicology Studies

1990

Environmental Health Perspectives

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The consequences of adventitious infectious agents upon the interpretation of toxicology studies performed in rats and mice are incompletely understood. Several prevalent murine pathogens cause alterations of the respiratory system that can confuse the assessment of chemically induced airway ixjury. In some instances the pathogenesis ofinfection with these agents has been relatively well studied in the lower respiratory tract. However, there are few well-controlled studies that have examined the upper respiratory region, which result in interpretive problems for toxicologic pathologists. The conduct and interpretation ofboth short-term and chronic rodent bioassays can be compromised by both the clinical and subclinical manifestations of infectious diseases. This paper reviews several important infectious diseases of the upper airway of rats and mice and discusses the potential influence of these conditions on the results of toxicology studies.

“…Sendai virus infection has been well described for mice (11)(12)(13), and recently the course of experimental infection in the rat has been reported (14). Sendai There are numerous systemic effects (Thble 1) that toxicologists and pathologists need to consider when interpreting the impact of Sendai virus infection upon study results (10,15).…”

Section: The Pathogenesis Of Natural and Experimentalmentioning

confidence: 99%

Infectious Diseases of the Upper Respiratory Tract: Implications for Toxicology Studies

1990

Environmental Health Perspectives

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The consequences of adventitious infectious agents upon the interpretation of toxicology studies performed in rats and mice are incompletely understood. Several prevalent murine pathogens cause alterations of the respiratory system that can confuse the assessment of chemically induced airway ixjury. In some instances the pathogenesis ofinfection with these agents has been relatively well studied in the lower respiratory tract. However, there are few well-controlled studies that have examined the upper respiratory region, which result in interpretive problems for toxicologic pathologists. The conduct and interpretation ofboth short-term and chronic rodent bioassays can be compromised by both the clinical and subclinical manifestations of infectious diseases. This paper reviews several important infectious diseases of the upper airway of rats and mice and discusses the potential influence of these conditions on the results of toxicology studies.

“…progression of lung lesions with persistent SeV [4,12,20,23]. In this study, we compared the pathogenicity of recombinant SeV with an inserted GFP gene (GFP-SeV) with that of its recombinant wild-type SeV (Wt-SeV) to determine the usefulness of the recombinant virus application for studying viral pathogenicity.…”

mentioning

confidence: 99%

“…In the lungs, SeV replicates in the bronchi-bronchiole epithelium and spreads to the alveolar wall, resulting in epithelial degeneration or proliferation accompanied by an inflammatory response of variable intensity, which is influenced by animal age, genotype, and immune status [3,5,11,13,17]. BALB/c nude (nu/nu) mice are known to be particularly susceptible to a wide range of infections that cause mild or no disease in normal (+/+) and heterozygotes (nu/+) mice [18,20,23]. A genetic deficiency in Tlymphocytes of the BALB/c nude mice causes the slow removed aseptically under ether anesthesia and exsanguination at 1, 2, 3, 5, 7, 10, 14, 30, 45 and 60 days after infection.…”

mentioning

confidence: 99%

Green Fluorescent Protein Gene Insertion of Sendai Virus Infection in Nude Mice: Possibility as an Infection Tracer.

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²

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³

et al. 2000

Journal of Veterinary Medical Science

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ABSTRACT. The green fluorescent protein (GFP) marker from jellyfish Aequorea victoria is considered to have potential use in the study of host-pathogen relationships, by tracing infections in living cells, organs and animals. We compared the pathogenicity of Sendai virus with an inserted GFP gene (GFP-SeV) with that of its wild-type (Wt-SeV) to determine the usefulness of the recombinant virus in long-term infection of BALB/c nude (nu/nu) mice. The results indicated that the presence of GFP in infected cells could be analyzed easily and sensitively. GFP helped in identifying and in understanding the cellular sites of viral replication in vitro and in vivo. However, the GFP insertion into the Wt-SeV genome, led to decreased pathogenicity, altering the in vivo viral kinetics.-KEY WORDS: BALB/c nude (nu/nu) mouse, green fluorescent protein, recombinant Sendai virus.

“…21 Other opportunistic infections recognized to date include fatal septicemia associated with either Proteus mirabilis infectionsI9 or alpha hemolytic streptococcal infections1* and acute mortality associated with mouse hepatitis virus infe~tion.~ Sendai virus infections are relatively common in conventional colonies of laboratory mice,14 and depending on the circumstances, including genetic background, lesions may vary from minimal to m a~k e d .~.~ Athymic nude BALBlc mice are very susceptible to the disease. 22 The purpose of this study was to determine the degree of susceptibility of SCID-beige mice on either the C.B-17 or C57BL genetic background to Sendai virus. prepared from the lungs of inoculated mice, and this was used as our standard inoculum.…”

mentioning

confidence: 99%

Signs and Lesions of Experimental Sendai Virus Infection in Two Genetically Distinct Strains of SCID/Beige Mice

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²

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³

1994

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Abstract. The pathogenesis of Sendai virus infection was studied in genetically immunodeficient mice of genotype scidlscid. bglbg (SCID-beige) using C.B-17 SCID-beige mice, a BALB/c-related strain that expresses the same major histocompatibility complex as the Sendai virus-susceptible DBA/2 (H-2d). Mice were inoculated intranasally with isolate 771076 of Sendai virus, then killed at 2-day intervals beginning on day 4 postinoculation. Clinical signs were evident beginning at 8 to 10 days post-inoculation, and all animals remaining were killed in extremis by 14 to 17 days post-inoculation. Lesions in inoculated mice were confined to the respiratory tract. In the nasal passages, a nonresolving rhinitis, with epithelial hyperplasialmetaplasia occurred. Cranioventral bronchopneumonitis was characterized by marked hyperplasia and necrosis of epithelial cells lining airways and with leukocytic infiltration. At the alveolar level, there was marked hypertrophy and hyperplasia of type I1 pneumocytes, mobilization of alveolar macrophages, and obliteration of the normal architecture in severely affected areas. Viral antigen was evident beginning at 4 days post-inoculation and persisted in affected areas throughout the duration of the study. Because immunocompetent C57BLl6 mice are known to be genetically resistant to Sendai virus, the susceptibility of C57BL/6 SCID-beige to Sendai virus was then compared to that of C.B-17 SCID-beige mice. In age-matched animals of the two strains, there was no evidence of natural resistance to Sendai virus infection in the immunodeficient C57BL/6 strain compared to the C.B-17 mice. These studies indicate that the genetic differences in susceptibility of two strains of immunocompetent mice to Sendai virus infection are eliminated by expression of the mutations scid and beige.

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