Peritoneal Loss of Growth Hormone in Children on Automated Peritoneal Dialysis

Abstract

Objective

To provide quantitative data regarding the daily dialytic loss of growth hormone (GH) in children on peritoneal dialysis (PD).

Design

Prospective study involving 24-hour dialysate collections on 3 consecutive days in patients with and without recombinant human GH (rhGH) treatment.

Setting

Single-center outpatient PD program.

Patients

Twenty-six children undergoing automated PD (APD): 6 with and 20 without daily rhGH.

Main Outcome Measures

Daily peritoneal losses of GH, α₁-, β₂-microglobulin, transferrin, and albumin.

Results

The mean (±SEM) daily dialytic GH loss was 2.18 ± 0.62 μg/1.73 m² per day in rhGH-treated patients and 0.42 ± 0.28 μg/1.73 m² per day in untreated patients, (p < 0.05). The intraindividual coefficient of variation of daily GH loss was 65%. The peritoneal loss of GH was positively correlated with that of β₂-microglobulin (r = 0.77, p < 0.001) and α₁-microglobulin (r = 0.51, p < 0.01). The variability in β₂-microglobulin and α₁-microglobulin elimination, together with the use of rhGH, explained 66% of the total variability of daily GH excretion. In patients without rhGH therapy, the daily peritoneal GH loss was approximately 0.05% of the estimated daily endogenous production rate based on previous estimates in children with end-stage renal failure. In patients on rhGH therapy, less than 0.1% of the injected rhGH dose was eliminated by dialysis.

Conclusion

Peritoneal losses of GH in children on APD account only for a minute fraction of endogenous metabolic clearance, and do not explain the variability of the rhGH treatment response. The assessment of dialytic GH elimination may be used to estimate time-integrated mean plasma GH concentrations, and to monitor rhGH treatment compliance.

Keywords

Children growth hormone clearance nightly automated peritoneal dialysis

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References

Schaefer

, Mehls

Endocrine, metabolic and growth disorders in chronic renal failure. In: Holliday

M.A.

, Barratt

T.M.

, Avner

E.D.

, eds. Pediatric nephrology. 4th ed. Baltimore, MD: Williams & Wilkins, 1999: 1197–230.

Salusky

I.B.

, Fine

R.N.

, Nelson

, Blumenkrantz

M.J.

, Kopple

J.D.

Nutritional status of children undergoing continuous ambulatory peritoneal dialysis.

Am J Clin Nutr 1983; 38: 599–611.

Broyer

, Niaudet

, Champion

, Jean

, Chopin

, Czernichow

Nutritional and metabolic studies in children on continuous ambulatory peritoneal dialysis.

Kidney Int 1983; 24(Suppl 15): 106–10.

Quan

, and Baum

Protein losses in children on continuous cycler peritoneal dialysis.

Pediatr Nephrol 1996; 10: 728–31.

Schaefer

, Klaus

, Mehls

, and the Mid European Pediatric Peritoneal Dialysis Study Group. Peritoneal transport properties and dialysis dose affect growth and nutritional status in children on chronic peritoneal dialysis. J Am Soc Nephrol 1999 (in press).

Wühl

, Haffner

, Schaefer

, Mehls

, and the German Study Group for Growth Hormone Treatment in Children with Chronic Renal Failure. Short children on dialysis treatment respond less to growth hormone than patients with chronic renal failure prior to dialysis. Pediatr Nephrol 1996; 10: 294–8.

Haffner

, Wühl

, Schaefer

, Nissel

, Tönshoff

, Otto

Mehls

and The German Study Group for Growth Hormone Treatment in Chronic Renal Failure. Factors predictive of the short- and long-term efficacy of growth hormone treatment in prepubertal children with chronic renal failure. J Am Soc Nephrol 1998; 9: 1899–907.

Schaefer

, Langenbeck

, Heckert

K.H.

, Schärer

, Mehls

Evaluation of peritoneal solute transfer by the peritoneal equilibration test in children. In: Khanna

, Nolph

K.D.

, Prowant

B.F.

, Twardowski

Z.J.

, Oreopoulos

D.G.

, eds. Advances in peritoneal dialysis. Toronto: Peritoneal Dialysis Bulletin, 1992; 8: 410–15.

Prader

, Largo

R.H.

, Molinari

, Issler

Physical growth of Swiss children from birth to 20 years of age.

Helv Paediatr Acta 1988; 52(Suppl): 1–125.

10.

Rolland–Cachera

M.F.

, Cole

T.J.

, Sempe

, Tichet

, Rossignol

, Charraud

Body mass index variations: centiles from birth to 87 years.

Eur J Clin Nutr 1991; 45: 13–21.

11.

Bradford

M.M.

A rapid and sensitive method for the quantitation of microgram quantities of protein utilizing the principle of protein dye binding.

Anal Biochem 1976; 72: 248–54.

12.

Main

, Philips

, Jorgensen

, Skakkebæk

N.E.

Urinary growth hormone excretion in 657 healthy children and adults: normal values, inter- and intra-individual variations.

Horm Res 1991; 36: 174–82.

13.

Warady

B.A.

, Alexander

S.R.

, Hossli

, Vonesh

, Geary

, Watkin

Peritoneal membrane transport function in children receiving long-term dialysis.

J Am Soc Nephrol 1996; 7: 2385–91.

14.

Schaefer

Adequacy of peritoneal dialysis in children. In: Fine

R.N.

, Warady

B.A.

, eds. CAPD/CCPD in children. 2nd ed. Boston, MA: Kluwer Academic Publishers, 1998: 99–118.

15.

Schaefer

, Veldhuis

J.D.

, Stanhope

, Jones

, and The Cooperative Study Group on Pubertal Development in Chronic Renal Failure. Alterations in growth hormone secretion and clearance in peripubertal boys with chronic renal failure and after transplantation. J Clin Endocrinol Metab 1994; 78: 1298–306.

16.

Kagan

, Zadik

, Gertler

, Ulman

, Bar-Khayim

Serum concentrations and peritoneal loss of growth hormone and growth-hormone binding protein activity in older adults undergoing continuous ambulatory peritoneal dialysis: comparison with haemodialysis patients and normal subjects.

Nephrol Dial Transplant 1993; 8: 352–6.

17.

Albertson–Wikland

, Rosberg

, Libre

, Lundberg

L–O

, Groth

Growth hormone secretory rates in children as estimated by deconvolution analysis of 24-h plasma concentration profiles.

Am J Physiol 1989; 257: E809–14.

18.

Martha

P.M.

, Gorman

K.M.

, Blizzard

R.M.

, Rogol

A.D.

, Veldhuis

J.D.

Endogenous growth hormone secretion and clearance rates in normal boys, as determined by deconvolution analysis: relationship to age, pubertal status, and body mass.

J Clin Endocrinol Metab 1992; 74: 336–44.

19.

Haffner

, Schaefer

, Girard

, Ritz

, Mehls

Metabolic clearance of human growth hormone in health and chronic renal failure.

J Clin Invest 1994; 93: 1163–71.

20.

Kagan

, Bar-Khayim

, Schafer

, and Fainaru

Kinetics of peritoneal protein loss during CAPD: I. Different characteristics for low and high molecular weight proteins.

Kidney Int 1990; 37: 971–9.

21.

Kabanda

, Goffin

, Bernard

, Lauwerys

, and van Ypersele de Strihou

Factors influencing serum levels and peritoneal clearances of low molecular weight proteins in continuous ambulatory peritoneal dialysis.

Kidney Int 1995; 48: 1946–52.

22.

Rippe

, Haraldsson

Transport of macromolecules across microvascular walls: the two-pore theory.

Physiol Rev 1994; 74: 163–219.

23.

Rippe

A three-pore model of peritoneal dialysis transport.

Perit Dial Int 1993; 13(Suppl 2): S35–8.

24.

Donaldson

D.L.

, Hollowell

J.G.

, Pan

, Gifford

R.A.

, Moore

W.W.

Growth hormone secretory profiles: variation on consecutive days.

J Pediatr 1989; 115: 51–6.

25.

Bereket

, Bereket

, Lang

C.H.

, Kaskel

F.J.

Peritoneal loss of insulin-like growth factor-I and binding proteins in end-stage renal disease.

Pediatr Nephrol 1998; 12: 581–8.