The Natural Time Course of Membrane Alterations during Peritoneal Dialysis is Partly Altered by Peritonitis

Author:

van Esch Sadie12,Struijk Dirk G.13,Krediet Raymond T.1

Affiliation:

1. Division of Nephrology, Academic Medical Centre, University of Amsterdam, Amsterdam

2. Nephrology Department and Internal Medicine, St. Elisabeth Hospital, Tilburg

3. Dianet, Amsterdam–Utrecht, Netherlands

Abstract

Background The quality of the peritoneal membrane can deteriorate over time. Exposure to glucose-based dialysis solutions is the most likely culprit. Because peritonitis is a common complication of peritoneal dialysis (PD), distinguishing between the effect of glucose exposure and a possible additive effect of peritonitis is difficult. The aim of the present study was to compare the time-course of peritoneal transport characteristics in patients without a single episode of peritonitis—representing the natural course—and in patients who experienced 1 or more episodes of peritonitis during long-term follow-up. Methods This prospective, single-center cohort study enrolled incident adult PD patients who started PD during 1990–2010. A standard peritoneal permeability analysis was performed in the first year of PD treatment and was repeated every year. The results in patients without a single episode of peritonitis (“no-peritonitis group”) were compared with the results obtained in patients who experienced 1 or more peritonitis episodes (“peritonitis group”) during a follow-up of 4 years. Results The 124 patients analyzed included 54 in the no-peritonitis group and 70 in the peritonitis group. The time-course of small-solute transport was different in the groups, with the peritonitis group showing an earlier and more pronounced increase in the mass transfer area coefficient for creatinine ( p = 0.07) and in glucose absorption ( p = 0.048). In the no-peritonitis group, the net ultrafiltration rate (NUFR) and the transcapillary ultrafiltration rate (TCUFR) both showed a steep increase from the 1st to the 2nd year of PD that was absent in the peritonitis group. Both groups showed a decrease in the NUFR after year 3. A decrease in the TCUFR occurred only in the peritonitis group. That decrease was already present after the year 1 in patients with severe peritonitis. The time-course of free water transport showed a continuous increase in the patients without peritonitis, but a decrease in the patients who experienced peritonitis ( p < 0.01). No difference was observed in the time-course of the effective lymphatic absorption rate. The time-courses of immunoglobulin G and α2-macroglobulin clearances showed a decrease in both patient groups, with a concomitant increase of the restriction coefficient. Those changes were not evidently influenced by peritonitis. The two groups showed a similar decrease in the mesothelial cell mass marker cancer antigen 125 during follow-up. Conclusions On top of the natural course of peritoneal function, peritonitis episodes to some extent influence the time-course of small-solute and fluid transport—especially the transport of solute-free water. Those modifications increase the risk for overhydration.

Publisher

SAGE Publications

Subject

Nephrology,General Medicine

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