Accelerated rejection of murine cardiac allografts by murine cytomegalovirus-infected recipients. Lack of haplotype specificity.

Carlquist, John F.; Shelby, Jane; Shao, Yuanlin; Greenwood, Jay H.; Hammond, M. Elizabeth; Anderson, Jeffrey L.

doi:10.1172/jci116499

Cited by 15 publications

(12 citation statements)

References 18 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Greater than 7-fold increases in IL-6 quantities were produced by MRC-5 cells treated with 10 Ϫ1 and 10 Ϫ2 dilutions of CMV-UV (A 450 and , respec-1.61 ‫ע‬ 0. 3 1.48 ‫ע‬ 0.27 tively, vs. A 450 for control cells; , unpaired 0.13 ‫ע‬ 0.003 P ! .001 t test).…”

Section: Il-6 Production Induced By Cmv-infected Cells and Cells Treamentioning

confidence: 96%

“…Other complications associated with CMV infection suggest interactions with host immune and cellular mechanisms. For example, CMV infection has been shown to be a risk factor for graft rejection among cardiac and renal transplant recipients [1,2], and the ability of CMV to actually accelerate graft rejection has been demonstrated in animal models [3]. Among cardiac transplant recipients, CMV infection promotes the development of posttransplant graft atherosclerosis, the leading cause of graft loss and mortality in recipients surviving 11 year [2].…”

mentioning

confidence: 99%

See 1 more Smart Citation

Cytomegalovirus Induction of Interleukin‐6 in Lung Fibroblasts Occurs Independently of Active Infection and Involves a G Protein and the Transcription Factor, NF‐𝛋B

Carlquist¹,

Edelman²,

Bennion³

et al. 1999

J INFECT DIS

View full text Add to dashboard Cite

Cytomegalovirus (CMV) infection induces the proinflammatory cytokine, interleukin (IL)-6, which may contribute to the pathology of the infection. In vitro CMV induction of IL-6 by human lung fibroblasts was studied. The quantity of cytokine in culture supernatants was maximal 20 h after infection and decreased thereafter. Transcription of the IL-6 gene and IL-6 protein expression were equally stimulated by infectious and UV-inactivated virus (CMV-UV). CMV-UV-stimulated IL-6 was inhibited by pyrrolidinedithiocarbamate (an inhibitor of the transcription factor, NF-kappaB) and by pertussis toxin (suggesting the involvement of a G protein) and occurred in the absence of CMV immediate-early antigen transcription. Neutralizing antibodies to IL-1beta or tumor necrosis factor-alpha did not affect CMV-UV-induced IL-6, but expression was inhibited by antibody to the CMV attachment glycoprotein. IL-6 production by fibroblasts occurs independently from productive infection but has characteristics that suggest a ligand receptor-mediated pathway. This function may be important in pathology or disease resolution.

show abstract

Section: Il-6 Production Induced By Cmv-infected Cells and Cells Treamentioning

confidence: 96%

mentioning

confidence: 99%

Cytomegalovirus Induction of Interleukin‐6 in Lung Fibroblasts Occurs Independently of Active Infection and Involves a G Protein and the Transcription Factor, NF‐𝛋B

Carlquist¹,

Edelman²,

Bennion³

et al. 1999

J INFECT DIS

View full text Add to dashboard Cite

show abstract

“…The broad cell tropism of CMV suggests that both local and systemic effects of CMV infection are likely to impact on early alloreactivity and long-term graft outcome. Acute infections of mice with MCMV in the peri-transplant period across different allogeneic combinations 36 , as have the re-activation of latent MCMV infection 37 . Furthermore, the impact of infection on graft survival in mice was greater with some types of viral infections, such as LCMV and Pichinde virus, compared with other viruses, and when infection occurred at or shortly after transplantation 38,39 .…”

Section: Timing Of Infections Relative To Transplantationmentioning

confidence: 99%

The impact of infection and tissue damage in solid-organ transplantation

2012

View full text Add to dashboard Cite

Preface Investigations over the past two decades are revealing the complexity in the regulation of the innate immune response, and how it, in turn, modulates adaptive immunity. Microbial exposure and tissue damage that accompany transplantation result in the release of both pathogen- and damage-associated molecular patterns, as well as the generation of cross-reactive alloreactive T cells. Here, we review these triggers of innate and adaptive immunity in the context of transplantation, and discuss the many ways infections and tissue damage might impact on alloreactivity and the outcome of transplanted allografts.

show abstract

“…CMV has an obvious well established association with graft loss following human transplantation (reviewed in [25]). Because we have recently shown that latent MCMV can influence allograft acceptance for murine cardiac transplantation [5], and others have shown accelerated cardiac allograft rejection in mice following acute infection [26, 27], we were interested to evaluate tissues from “naïve” mice with unexpected graft losses. There is a strikingly high rate of graft failure associated with occult MCMV suggested by the current report, although this finding is admittedly circumstantial.…”

Section: Discussionmentioning

confidence: 99%

Occult cytomegalovirus in vivarium-housed mice may influence transplant allograft acceptance

Thomas¹,

Forster²,

Bickerstaff³

et al. 2010

Transplant Immunology

View full text Add to dashboard Cite

We have recently shown that latent murine cytomegalovirus (MCMV) can influence murine transplant allograft acceptance. During these studies we became aware that vivarium-housed control mice can acquire occult MCMV infection. The purpose of this investigation was to confirm occult MCMV transmission and determine the timing, vehicle, and possible consequences of transmission. Mice arriving from a commercial vendor were negative for MCMV both by commercial serologic testing and by our nested PCR. Mice housed in our vivarium became positive for MCMV DNA 30-60 days after arrival, but remained negative for MCMV by commercial serologic testing. To confirm MCMV we sequenced PCR products for several genes and showed >99% homology to MCMV. Further sequence analyses show that the occult MCMV is similar to a laboratory strain of MCMV, but the vehicle of transmission remains unclear. Control tissues from historical experiments with unexplained graft losses were evaluated for occult MCMV, and mice with unexplained allograft losses showed significantly higher incidence of occult MCMV than did allograft acceptors. Deliberate infection with very low titer MCMV confirmed that viral transmission can occur without measurable virus specific antibody or T-cell responses. These data suggest that vivarium-housed mice can develop occult MCMV that is missed by currently available commercial serologic testing, and that these infections may influence transplant allograft acceptance.

show abstract

Accelerated rejection of murine cardiac allografts by murine cytomegalovirus-infected recipients. Lack of haplotype specificity.

Cited by 15 publications

References 18 publications

Cytomegalovirus Induction of Interleukin‐6 in Lung Fibroblasts Occurs Independently of Active Infection and Involves a G Protein and the Transcription Factor, NF‐𝛋B

Cytomegalovirus Induction of Interleukin‐6 in Lung Fibroblasts Occurs Independently of Active Infection and Involves a G Protein and the Transcription Factor, NF‐𝛋B

The impact of infection and tissue damage in solid-organ transplantation

Occult cytomegalovirus in vivarium-housed mice may influence transplant allograft acceptance

Contact Info

Product

Resources

About