2019 Chung ALTEX.pdf (9.77 MB)
An ex vivo porcine spleen perfusion as a model of bacterial sepsis.
journal contribution
posted on 2019-05-23, 10:28 authored by WY Chung, JJ Wanford, R Kumar, JD Isherwood, RD Haigh, MR Oggioni, AR Dennison, G ErcoliAn ex vivo, porcine spleen perfusion model was established to study the early events occurring in the spleen prior to the onset of bacterial sepsis, using organs retrieved from animals slaughtered for food production. Porcine spleens were harvested from adult pigs and connected to a normothermic extracorporeal perfusion circuit. A constant perfusion of heparinized blood was performed for 6 hours. After injection of Streptococcus pneumoniae to the circuit serial samples of both blood and spleen biopsies were collected and analysed. Functionality of the perfused organs was assessed by monitoring the blood-gas parameters, flow rate and filtering capability of the organ. Interestingly, we observed full clearance of bacteria from the blood and an increase in bacterial counts in the spleen. Classical histology and immunohistochemistry on biopsies also confirmed no major damages in the organ architecture and changes in the immune cell distribution, other than the presence of clusters of pneumococci. A time-course study confirmed that each focus of infection derived from the replication of single pneumococcal cells within splenic macrophages. The model proposed - in line with the 3Rs principles - has utility in the replacement of experimental animals in infection research. Murine models are prevalently used to study pneumococcal infections, but are often not predictive for humans due to substantial differences in the immune systems of the two species. This model is designed to overcome these limitations, since porcine immunology and splenic architecture in particular, closely resemble those of humans.
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Citation
ALTEX, 2019, 36 (1), pp. 29-38Author affiliation
/Organisation/COLLEGE OF LIFE SCIENCES/Biological Sciences/Genetics and Genome BiologyVersion
- VoR (Version of Record)
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ALTEXPublisher
ALTEX Editionissn
1868-596XAcceptance date
2018-07-27Copyright date
2018Available date
2019-05-23Publisher DOI
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https://www.altex.org/index.php/altex/article/view/1006Language
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