To elucidate the importance of possible trapping of macromolecules in peritoneal tissue on the calculation of peritoneal lymphatic drainage, we compared the transport of inulin administered i.v. and i.p. in nine continuous ambulatory peritoneal dialysis (CAPD) patients on two separate days. In the intraperitoneal study inulin (5 g) was added to the dialysate and in the intravenous study inulin (5 g) was given i.v. 3 h before the test. No differences were found in the mass transfer area coefficients (MTC) of urea, creatinine, and glucose between the two tests. The MTC after inulin i.p. was 3.2 ± 0.7 mLlmin (mean ± SD) and after inulin i.v. 1.8 ± 0.5 (p < 10-5). As the difference in transport kinetics between i.v. and i.p. administration is likely to be caused by lymphatic absorption, a mean lymphatic flow of 1.4 mLlmin could be calculated. This value corresponds to the data obtained with macromolecules. Our results therefore favor the hypothesis that no local accumulation of macromolecules in the peritoneal tissues takes place and that their disappearance from the peritoneal cavity represents lymphatic absorption.
NolphK.D., MactierR.A., KhannaR.The kinetics of ultrafiltration during peritoneal dialysis: The role of lymphatics.Kidney Int.1987; 32: 219–226.
2.
MactierR.A., KhannaR., TwardowskiZ.Contribution of lymphatic absorption to loss of ultrafiltration and solute clearances in continuous ambulatory peritoneal dialysis.J Clin Invest.1987; 80: 1311–1316.
3.
MactierR.A., KhannaR., TwardowskiZ.J.Ultrafiltration failure in continuous ambulatory peritoneal dialysis due to excessive peritoneal cavity lymphatic absorption.Am J Kidney Dis.1987; 10: 461–466.
De PaepeM., SchelstraeteK., BelpaireF.Comparison of different volume markers in peritoneal dialysis.J Lab Clin Med.1988; 111: 421–429.
6.
CanaudB., Liendo-LiendoC., ClaretG.Etude “in situ” de la cinétique de I'ultrafiltration en cours de dialyse peritoneale avec périodes de diffusion prolongué.Néphrologie.1980; 1: 126–132.
7.
KredietR.T., BoeschotenE.W., ZuyderhoudtF.M.J.Simple assessment of the efficacy of peritoneal transport in continuous ambulatory peritoneal dialysis patients.Blood Purif1986; 4: 194–203.
8.
KredietR.T., ZuyderhoudtF.M.J., BoeschotenE.W.Alterations in the peritoneal transport of water and solutes during peritonitis in continuous ambulatory peritoneal dialysis patients.Eur J Clin Invest.1987; 17: 43–52.
9.
RippeB., StelinG., AhlmenJ.Lymph flow from the peritoneal cavity in CAPD patients. In: MaherJ.F., WinchesterJ.F., eds. Frontiers in Peritoneal Dialysis.New York: Field, Rich, and Associates:1986: 279–282.
10.
SpencerP.C., FarrellP.C.Solute and water transfer kinetics in CAPD. In: GokalR., ed. Continuous Ambulatory Peritoneal Dialysis.London: Churchill Livingstone; 1986: 38–55.
11.
FlessnerM.F., ParkerR.J., SieberS.M.Peritoneallymphatic uptake of fibrinogen and erythrocytes in the rat.Am J Physiol.1983; 244: H89–H96.
12.
FlessnerM.F., FenstermacherJ.D., BlasbergR.G.Peritoneal absorption of macromolecules studied by quantitative autoradiography.Am J Physiol.1985; 148: H26–H32.
13.
AlvingA.S., MillerB.F.A practical method for the measurement of glomerular filtration rate (inulin clearance).Arch Int Med.1940; 66: 306–318.
14.
GaudinoM., LevittM.F.Inulin space as a measure of extracellular fluid.Am J Physiol.1957; 157: 387–393.
15.
GarredL.J., CanaudB., FarrellP.C.A simple kinetic model for assessing peritoneal mass transfer in chronic ambulatory peritoneal dialysis.ASAIO J.1983; 6: 131137.
16.
BrownP., NolphK.D.Chemical measurements of inulin concentrations in peritoneal dialysis solution.Clin Chim Acta.1977; 76: 103–112.
17.
KredietR.T., StruijkD.G., BoeschotenE.W.Measurement of intraperitoneal fluid kinetics in CAPD patients by means of autologous haemoglobin.Neth J Med.1988; 33: 281–290.
KredietR.T., BoeschotenE.W., StruijkD.G., AriszL.Pharmacokinetics of intraperitoneally administered 5-fluorocytosine in continuous ambulatory peritoneal dialysis.Nephrol Dial Transplant.1987; 2: 453.
20.
BabbA.L., JohansenP.J., StrandM.J., TenckhoffH., ScribnerB.H.Bi-directional permeability of the human peritoneum to middle molecules.Proc Eur Dial Transplant Assoc.1973; 10: 247–262.
21.
KredietR.T., KoomenG.C.M., KoopmanM.G.The peritoneal transport of serum proteins and neutral dextran in CAPD patients.Kidney Int.1989; 35: 1064–1072.
22.
KredietR.T., StruijkD.G., KoomenG.C.M., HoekF.J., AriszL.The disappearance of macromolecules from the peritoneal cavity during CAPD is not dependent on molecular size.Perit Dial Int.1990; 10: 147–152.
23.
JanickeD.M., MorseG.D., ApicellaM.A., JuskoW.J., WalsheJ.J.Pharmacokinetic modeling of bidirectional transfer during peritoneal dialysis.Clin Pharmacol Ther.1986; 40: 209–218.
24.
GrimE., SimondsA., OeljenC.Inulin and mannitol distribution volumes in canine small intestinal tissues in vivo.Am J Physiol.1973; 224: 186–190.
25.
EdelmanI.S., LeibmanJ.Anatomy of body water and electrolytes.Am J Med.1959; 27: 256–277.
26.
MactierR.A., KhannaR.Absorption of fluid and solutes from the peritoneal cavity.Trans Am Soc Artif Intern Organs.1989; 35: 122–131.
27.
RippeB., StelinG.Simulations of peritoneal solute transport during CAPD. Application of two-pore formalism.Kidney Int.1989; 35: 1234–1244.
28.
HirszelP., DonohueT.S., ChakrabartiE., MontcalmE., MaherJ.F.The role of the capillary wall in restricting diffusion of macromolecules.Nephron.1988; 49: 58–61.
29.
FlessnerM.F., DedrickR.L., SchultzJ.S.Exchange of macromolecules between peritoneal cavity and plasma.Am J Physiol.1985; H15–H25.
30.
CheekT.R., TwardowskiZ.J., MooreH.L.High molecular weight (MW) gelatin isocyanate absorption from the peritoneal cavity in rats.Perit Dial Bull.1987; 7: S16.
31.
CoatedG., BushR.S., AspinN.A study of ascites using Iymphoscintigraphy with 99mTc-sulfur colloid.Radiology.1973; 107: 577–583.
32.
BronskillM.J., BushR.S., EgeG.N.A quantitative measurement of peritoneal drainage in malignant ascites.Cancer.1977; 40: 2375–2380.
