Mouse Adenovirus Type 1 Infection in SCID Mice: an Experimental Model for Antiviral Therapy of Systemic Adenovirus Infections

Lenaerts, Liesbeth; Verbeken, Erik; Clercq, Erik De; Naesens, Lieve

doi:10.1128/aac.49.11.4689-4699.2005

Cited by 32 publications

(47 citation statements)

References 54 publications

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“…The C3H/3T3 mouse embryonic fibroblast cell line was cultured as described previously (27). For the virus neutralization assays, the concentration of heat-inactivated newborn calf serum was reduced to 2%.…”

Section: Cells and Virusesmentioning

confidence: 99%

“…For the analysis of MAV-1 titers in tissues of infected mice, cardiac perfusion with PBS and dissection were performed and organs were recovered, homogenized, and subjected to DNA extraction according to the tissue protocol of the QIAamp DNA mini kit (Qiagen, Hilden, Germany). MAV-1 DNA was quantified by real-time PCR analysis using an ABI Prism 7000 apparatus (Applied Biosystems, Foster City, CA) and a previously published protocol (27). To correct for experimental variations, the primerprobe set of the 18S genomic endogenous control kit (Eurogentec, Seraing, Belgium) was included in the same PCR mixture as the target primer-probe set.…”

Section: Cells and Virusesmentioning

confidence: 99%

“…Virus stocks were prepared in C3H/3T3 cells as described before (27). The titer of the virus stocks, determined by a standard plaque assay, was ϳ8 ϫ 10 5 PFU per ml.…”

Section: Cells and Virusesmentioning

confidence: 99%

“…From the following organs, parts were fixated in 4% formaldehyde for 24 h and then embedded in paraffin: spleen, kidney, adrenal glands, liver, small intestine, lung, heart, and brain. Tissue sections, 4 m thick, were stained with hematoxylin and eosin for routine histologic examination and immunohistochemically with a rabbit polyclonal antibody to the MAV-1 E3 class 1 protein by using a standard avidin-biotin immunoperoxidase staining procedure, as previously described (27).…”

Section: Cells and Virusesmentioning

confidence: 99%

“…We previously demonstrated that continued antiviral treatment with cidofovir causes a marked delay in MAV-1-induced disease but cannot prevent a fatal outcome in severe combined immunodeficient (SCID) mice (27). In other studies, mice with genetic deficiencies in specific immunological functions were used to investigate the roles of distinct leukocyte subsets in MAV-1 infection (31,32).…”

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confidence: 99%

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Recovery of Humoral Immunity Is Critical for Successful Antiviral Therapy in Disseminated Mouse Adenovirus Type 1 Infection

Lenaerts

Kelchtermans

Geboes

et al. 2008

Antimicrob Agents Chemother

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Severe adenovirus infections in transplant recipients undergoing immunosuppressive therapy are of increasing concern. Controversy exists on the contribution of antiviral therapy and the host immune response to recovery from these infections. Here, we established a systemic mouse adenovirus type 1 (MAV-1) infection in cyclophosphamide (CyP)-treated BALB/c mice. CyP was administered at 100 mg per kg of body weight every other day for 2, 3, or 4 weeks, thereby inducing general but reversible leukopenia, with a major suppression of the B-cell numbers and functionality that was more pronounced than that seen with T cells. The outcome of MAV-1 infection was dependent on the duration of CyP therapy, as the mice with the most severe immunosuppression were the most vulnerable to MAV-1-induced hemorrhagic enteritis and mortality. The protective effect of concomitant antiviral therapy with cidofovir depended on the level of immunosuppression. The combination of cidofovir treatment with the withdrawal of immunosuppression was the most successful regimen for increasing survival rates. Survival was clearly correlated with the clearance of virus and increased titers of MAV-1-specific antibodies in sera. In addition, the passive transfer of MAV-1-specific immunoglobulin G into MAV-1-infected SCID BALB/c mice caused a marked delay in mortality, the extent of the delay being dependent on the titer of MAV-1-specific antibodies. Based on the critical role of the humoral immune response in the early defense against disseminated adenovirus infection, the concomitant use of adenovirus-specific immunoglobulins and antiviral therapy should be considered for transplant patients at risk for severe adenovirus infections.

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Section: Cells and Virusesmentioning

confidence: 99%

Section: Cells and Virusesmentioning

confidence: 99%

“…Virus stocks were prepared in C3H/3T3 cells as described before (27). The titer of the virus stocks, determined by a standard plaque assay, was ϳ8 ϫ 10 5 PFU per ml.…”

Section: Cells and Virusesmentioning

confidence: 99%

Section: Cells and Virusesmentioning

confidence: 99%

mentioning

confidence: 99%

See 3 more Smart Citations

Recovery of Humoral Immunity Is Critical for Successful Antiviral Therapy in Disseminated Mouse Adenovirus Type 1 Infection

Lenaerts

Kelchtermans

Geboes

et al. 2008

Antimicrob Agents Chemother

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Mouse

Percy¹,

Barthold

2007

Pathology of Laboratory Rodents and Rabbits

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The laboratory mouse is an artificial creation, and there is no true "wildtype" laboratory mouse. Furthermore, there is no such thing as "normal" microflora, since laboratory mice are maintained in microbially pristine environments devoid of pathogens and opportunistic pathogens, as well as other commensal flora/fauna. House mice, from which laboratory mice originated, are represented by several species and subspecies native to the Old World. Laboratory mice are largely derived from domesticated "fancy mice" that arose from many years of trading of mouse variants among fanciers in Europe, Asia, North America, and Australia. The laboratory mouse genome, including its retroelements, is a mosaic derived from different subspecies of the Mus musculus complex, including M.m. domesticus, M.m. musculus, M.m. castaneus, M.m. molossinus (a natural hybrid of M.m. musculus and M.m. castaneus), and M. bactrianus.The genome of M.m. domesticus is the predominant contributor to most strains of mice, but many inbred strains share a common "Eve" with a mitochondrial genome of M.m. musculus origin, and a common "Adam" that contributed their Y chromosome from Asian mice. In addition, there is evidence that other Mus species, outside of the M. musculus complex, may have contributed to the genome of some laboratory mouse strains. The C57BL mouse genome contains a contribution from M. spretus. The 1st inbred mouse (DBA), and other strains with DBA genetic contributions, was partially derived from Japanese waltzing mice with M. bactrianus parentage. Perhaps the only laboratory mouse that is derived from a single species (subspecies), M.m. domesticus, is the "Swiss" mouse, but there is a high likelihood that several Swiss stocks and strains have been genetically corrupted.There are over 450 inbred strains of laboratory mice that have arisen during the last century, and these strains, which were selectively inbred to pan-genomic homozygosity for purposes entirely unrelated to modern research, are the foundation upon which literally thousands of spontaneous mutants and GEMs have been built. Additional inbred strains have been developed from wild mice (M.m. castaneus, M. spretus, etc.). Furthermore, "outbred" mice (mostly Swiss mice) are highly homozygous and nearly inbred. There is no such thing as an outbred laboratory mouse with a fully heterozygous genome representative of wildtype M. musculus, and there is no wild mouse genetic counterpart of the laboratory mouse. When working with mice, the pathologist must also become facile with hybrids,

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Mouse adenovirus type 1 and human adenovirus type 5 differ in endothelial cell tropism and liver targeting

Lenaerts

McVey

Baker

et al. 2008

The Journal of Gene Medicine

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Mouse Adenovirus Type 1 Infection in SCID Mice: an Experimental Model for Antiviral Therapy of Systemic Adenovirus Infections

Cited by 32 publications

References 54 publications

Recovery of Humoral Immunity Is Critical for Successful Antiviral Therapy in Disseminated Mouse Adenovirus Type 1 Infection

Recovery of Humoral Immunity Is Critical for Successful Antiviral Therapy in Disseminated Mouse Adenovirus Type 1 Infection

Mouse

Mouse adenovirus type 1 and human adenovirus type 5 differ in endothelial cell tropism and liver targeting

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