Early exposure to germs modifies kidney damage and inflammation after experimental ischemia-reperfusion injury
- Authors
- Jang H.R.; Gandolfo M.T.; Ko G.J.; Satpute S.; Racusen L.; Rabb H.
- Issue Date
- 2009
- Keywords
- Germ-free status; Immune modulation
- Citation
- American Journal of Physiology - Renal Physiology, v.297, no.5, pp F1457 - F1465
- Indexed
- SCOPUS
- Journal Title
- American Journal of Physiology - Renal Physiology
- Volume
- 297
- Number
- 5
- Start Page
- F1457
- End Page
- F1465
- URI
- https://scholarworks.korea.ac.kr/kumedicine/handle/2020.sw.kumedicine/16563
- DOI
- 10.1152/ajprenal.90769.2008
- ISSN
- 0363-6127
- Abstract
- Kidney ischemia-reperfusion injury (IRI) is, in part, mediated by immune and inflammatory factors. Since microbial stimuli are known to alter immune and inflammatory responses, we hypothesized that differences in perinatal microbial status would modify renal injury following IRI. We performed bilateral renal IRI on 6-wk-old germ-free and control mice and studied the effects on kidney lymphocyte trafficking, cytokines, function, and structure. Compared with control mice, normal kidneys of germ-free mice exhibited more NKT cells and lower IL-4 levels. Postischemia, more CD8 T cells trafficked into postischemic kidneys of germ-free mice compared with control mice. Renal structural injury and functional decline following IRI were more severe in germ-free mice compared with control mice. When germ-free mice were conventionalized with the addition of bacteria to their diet, the extent of renal injury after IRI became equivalent to age-matched control mice, with similar numbers and phenotypes of T cells and NKT cells, as well as cytokine expression in both normal kidneys and postischemic kidneys of conventionalized germ-free mice and age-matched control mice. Thus microbial stimuli influence the phenotype of renal lymphocytes and the expression of cytokines of normal kidneys and also modulate the outcome of IRI. Copyright © 2009 the American Physiological Society.
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Collections - 2. Clinical Science > Department of Nephrology and Hypertension > 1. Journal Articles
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