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Independent Effects of Systemic and Peritoneal Inflammation on Peritoneal Dialysis Survival

Authors
Lambie, MarkChess, JamesDonovan, Kieron L.Kim, Yong LimDo, Jun YoungLee, Hi BahlNoh, HyunjinWilliams, Paul F.Williams, Andrew J.Davison, SaraDorval, MarcSummers, AngelaWilliams, John D.Bankart, JohnDavies, Simon J.Topley, Nicholas
Issue Date
Dec-2013
Publisher
Lippincott Williams & Wilkins Ltd.
Keywords
신장내과
Citation
Journal of the American Society of Nephrology : JASN, v.24, no.12, pp 2071 - 2080
Pages
10
Journal Title
Journal of the American Society of Nephrology : JASN
Volume
24
Number
12
Start Page
2071
End Page
2080
URI
https://scholarworks.bwise.kr/sch/handle/2021.sw.sch/13173
DOI
10.1681/ASN.2013030314
ISSN
1046-6673
1533-3450
Abstract
Systemic inflammation, as evidenced by elevated inflammatory cytokines, is a feature of advanced renal failure and predicts worse survival. Dialysate IL-6 concentrations associate with variability in peritoneal small solute transport rate (PSTR), which has also been linked to patient survival. Here, we determined the link between systemic and intraperitoneal inflammation with regards to peritoneal membrane function and patient survival as part of the Global Fluid Study, a multinational, multicenter, prospective, combined incident and prevalent cohort study (n=959 patients) with up to 8 years of follow-up. Data collected included patient demographic characteristics, comorbidity, modality, dialysis prescription, and peritoneal membrane function. Dialysate and plasma cytokines were measured by electrochemiluminescence. A total of 426 survival endpoints occurred in 559 incident and 358 prevalent patients from 10 centers in Korea, Canada, and the United Kingdom. On patient entry to the study, systemic and intraperitoneal cytokine networks were dissociated, with evidence of local cytokine production within the peritoneum. After adjustment for multiple covariates, systemic inflammation was associated with age and comorbidity and independently predicted patient survival in both incident and prevalent cohorts. In contrast, intraperitoneal inflammation was the most important determinant of PSTR but did not affect survival. In prevalent patients, the relationship between local inflammation and membrane function persisted but did not account for an increased mortality associated with faster PSTR. These data suggest that systemic and local intraperitoneal inflammation reflect distinct processes and consequences in patients treated with peritoneal dialysis, so their prevention may require different therapeutic approaches; the significance of intraperitoneal inflammation requires further elucidation.
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