Acute infection in an animal model of chronic peritoneal dialysis (PD) induces structural changes in the peritoneum and alters functional characteristics of transport. These changes may compromise observations of the chronic effects of dialysis solutions. To test the hypothesis that antibiotics would prevent acute infection without affecting transport and structural properties, we characterized the frequency of infection in our rat model of PD and examined whether the inclusion of antibiotics in the dialysis solution altered the transport and structural properties of the peritoneum.
Design
Female Sprague–Dawley rats were aseptically injected daily under gas anesthesia with 30 – 40 mL of a sterile solution for 2 months via a peritoneal catheter tunneled to a subcutaneous port. Solutions used were Krebs–Ringer bicarbonate (KRB) alone, KRB with antibiotics (cefazolin 200 mg/L and gentamicin 2 mg/L), KRB with 4% glucose, and KRB with both glucose and antibiotics. After 2 months, osmotic filtration and solute transport were assessed in each animal and peritoneal fluid was collected for bacterial culture. Angiogenesis was evaluated by quantitative image analysis of tissue sections stained with CD31. Tissue content of collagen, hyaluronic acid, and sulfated glycosaminoglycan was determined.
Results
Technique survival (successful PD for 2 months) and infection rate were comparable among all treated groups. There were no differences between the groups in transport properties. Structural changes were comparable between groups, with or without antibiotics.
Conclusions
Addition of antibiotics to the dialysis solution did not affect the transport characteristics of the peritoneum or the pathologic reaction of the tissue to the PD solution.
VanholderR., van BiesenW.Incidence of infectious morbidity and mortality in dialysis patients.Blood Purif2002; 20: 477–80.
2.
WoodrowG., TurneyJ.H., BrownjohnA.M.Technique failure in peritoneal dialysis and its impact on patient survival.Perit Dial Int1997; 17: 360–4.
3.
TroidleL., Gorban-BrennanN., KligerA., FinkelsteinF.O.Continuous peritoneal dialysis-associated peritonitis: a review and current concepts.Semin Dial2003; 16: 428–37.
4.
AlbrektsenG.E., WideroeT.E., NilsenT.I., RomundstadP., RadtkeM., HallanS.Transperitoneal water transport before, during, and after episodes with infectious peritonitis in patients treated with CAPD.Am J Kidney Dis2004; 43: 485–91.
5.
ChenJ.B., PanH.H., LeeC.H., ChienY.S., LeeC.T., LiuT.T.Longitudinal change in peritoneal membrane function with continuous ambulatory peritoneal dialysis (CAPD) after peritonitis episodes.Chang Gung Med J2004; 27: 29–34.
6.
SmitW., van den BergN., SchoutenN., AikensE., StruijkD.G., KredietR.T.Free-water transport in fast transport status: a comparison between CAPD peritonitis and long-term PD.Kidney Int2004; 65: 298–303.
7.
NiJ., MoulinP., GianelloP., FeronO., BalligandJ.L., DevuystO.Mice that lack endothelial nitric oxide synthase are protected against functional and structural modifications induced by acute peritonitis.J Am Soc Nephrol2003; 14: 3205–16.
8.
WilliamsJ.D., CraigK.J., TopleyN., von RuhlandC., FallonM., NewmanG.R.Morphologic changes in the peritoneal membrane of patients with renal disease.J Am Soc Nephrol2002; 13: 470–9.
9.
WilliamsJ.D., CraigK.J., von RuhlandC., TopleyN., WilliamsG.T.The natural course of peritoneal membrane biology during peritoneal dialysis.Kidney Int Suppl2003; 88: S43–9.
10.
DevuystO., TopleyN., WilliamsJ.D.Morphological and functional changes in the dialysed peritoneal cavity: impact of more biocompatible solutions.Nephrol Dial Transplant2002; 17(Suppl 3): 12–15.
11.
WilliamsJ.D., CraigK.J., TopleyN., WilliamsG.T.Peritoneal dialysis: changes to the structure of the peritoneal membrane and potential for biocompatible solutions.Kidney Int Suppl2003; 84: S158–61.
12.
MortierS., De VrieseA.S., LeyssensA., VanackerN.J., FaictD., CornelissenM.Antibiotic administration in an animal model of chronic peritoneal dialysate exposure.Perit Dial Int2003; 23: 331–8.
13.
De VrieseA.S., MortierS., CornelissenM., PalmansE., VanackerN.J., LeyssensA.The effects of heparin administration in an animal model of chronic peritoneal dialysate exposure.Perit Dial Int2002; 22: 566–72.
14.
FlessnerM.F., SchwabA.Pressure threshold for fluid loss from the peritoneal cavity.Am J Physiol1996; 270: F377–F390.
FlessnerM.F.Small-solute transport across specific peritoneal tissue surfaces in the rat.J Am Soc Nephrol1996; 7: 225–33.
17.
FlessnerM.F.In vivo peritoneal chamber: linking structure and transport function.Perit Dial Int2001; 21(Suppl 3): S335–7.
18.
HasanJ., ByersR., JaysonG.C.Intra-tumoural microvessel density in human solid tumours.Br J Cancer2002; 86: 1566–77.
19.
VermeulenP.B., GaspariniG., FoxS.B., ToiM., MartinL., McCullochP.Quantification of angiogenesis in solid human tumours: an international consensus on the methodology and criteria of evaluation.Eur J Cancer1996; 32A: 2474–84.
20.
ReddyG.K., EnwemekaC.S.A simplified method for the analysis of hydroxyproline in biological tissues.Clin Biochem1996; 29: 225–9.
21.
HekkingL.H., AaldersM.C., van GelderopE., ZweersM.M., StruijkD.G., HavenithC.E.Effect of peritoneal dialysis fluid measured in vivo in a rat-model of continuous peritoneal dialysis.Adv Perit Dial1998; 14: 14–18.
22.
Wieczorowska-TobisK., KorybalskaK., PolubinskaA., RadkowskiM., BreborowiczA., OreopoulosD.G.In vivo model to study the biocompatibility of peritoneal dialysis solutions.Int J Artif Organs1997; 20: 673–7.
23.
ter WeeP.M., BeelenR.H., van den BornJ.The application of animal models to study the biocompatibility of bicarbonate-buffered peritoneal dialysis solutions.Kidney Int Suppl2003; 88: S75–83.
24.
van BiesenW., VeysN., VanholderR., LameireN.New concepts in peritoneal dialysis: new wine in old barrels?Artif Organs2003; 27: 398–405.
25.
PengW.X., GuoQ.Y., LiuS.M., LiuC.Z., LindholmB., WangT.Comparison of three chronic dialysis models.Adv Perit Dial2000; 16: 51–4.
26.
GormanS.P., JonesD.S., MawhinneyW.M., McGovernJ.G., AdairC.G.Conditioning fluid influences on the surface properties of silicone and polyurethane peritoneal catheters: implications for infection.J Mater Sci Mater Med1997; 8: 631–5.
27.
SwartzR., MessanaJ., HolmesC., WilliamsJ.Biofilm formation on peritoneal catheters does not require the presence of infection.ASAIO Trans1991; 37: 626–34.
28.
MarrieT.J., NobleM.A., CostertonJ.W.Examination of the morphology of bacteria adhering to peritoneal dialysis catheters by scanning and transmission electron microscopy.J Clin Microbiol1983; 18: 1388–98.
29.
KimD.K., YooT.H., RyuD.R., XuZ.G., KimH.J., ChoiK.H.Changes in causative organisms and their antimicrobial susceptibilities in CAPD peritonitis: a single center's experience over one decade.Perit Dial Int2004; 24: 424–32.
30.
FernandezM.A., OrtizA.M., ValenzuelaM., MoralesR.A.Peritoneal dialysis in chronic renal failure patients over 65 years of age.Adv Perit Dial2004; 20: 128–31.
31.
NakamotoH., HashikitaY., ItabashiA., KobayashiT., SuzukiH.Changes in the organisms of resistant peritonitis in patients on continuous ambulatory peritoneal dialysis.Adv Perit Dial2004; 20: 52–7.
32.
StrijackC., HardingG.K., ArianoR.E., ZelenitskyS.A.Peritoneal fluid titer test for peritoneal dialysis-related peritonitis.Antimicrob Agents Chemother2004; 48: 1719–26.
33.
MusiB., BraideM., CarlssonO., WieslanderA., AlbrektssonA., KettelerM.Biocompatibility of peritoneal dialysis fluids: long-term exposure of nonuremic rats.Perit Dial Int2004; 24: 37–47.
34.
MortierS., FaictD., SchalkwijkC.G., LameireN.H., De VrieseA.S.Long-term exposure to new peritoneal dialysis solutions: effects on the peritoneal membrane.Kidney Int2004; 66: 1257–65.
35.
MargettsP.J., GyorffyS., KolbM., YuL., HoffC.M., HolmesC.J.Antiangiogenic and antifibrotic gene therapy in a chronic infusion model of peritoneal dialysis in rats.J Am Soc Nephrol2002; 13: 721–8.
36.
MatsukiT., DulingB.R.TNF-alpha modulates arteriolar reactivity secondary to a change in intimal permeability.Microcirculation2000; 7: 411–18.
37.
HenryC.B., DulingB.R.TNF-alpha increases entry of macromolecules into luminal endothelial cell glycocalyx.Am J Physiol Heart Circ Physiol2000; 279: H2815–H2823.
38.
WangT., HeimburgerO., QureshiA.R., WaniewskiJ., BergstromJ., LindholmB.Physiological saline is not a biocompatible peritoneal dialysis solution.Int J Artif Organs1999; 22: 88–93.
FlessnerM.F., FenstermacherJ.D., DedrickR.L., BlasbergR.G.A distributed model of peritoneal-plasma transport: tissue concentration gradients.Am J Physiol1985; 248: F425–F435.
45.
van WestrhenenR., de WaartD.R., AkmanS., KredietR.T.Assessment of peritoneal fibrosis by conventional light microscopy and hydroxyproline measurements.Perit Dial Int2004; 24: 290–2.
46.
De VrieseA.S., FlyvbjergA., MortierS., TiltonR.G., LameireN.H.Inhibition of the interaction of AGE-RAGE prevents hyperglycemia-induced fibrosis of the peritoneal membrane.J Am Soc Nephrol2003; 14: 2109–18.
47.
FlessnerM.F., LofthouseJ., WilliamsA.Chronic alteration of subperitoneal tissue and peritoneal transport.Adv Perit Dial2002; 18: 12–14.
