Skip to main content
Key Specialties
Cardiology Diabetology Endocrinology Gastroenterology Geriatrics and Gerontology Gynecology and Obstetrics Hematology Infectious Disease Internal Medicine Nephrology Neurology Oncology Pediatrics Respiratory Medicine Rheumatology Surgery
Congress Coverage
2024 ACC Congress 2023 ESMO Congress 2023 EASD Congress 2023 ERS Congress 2023 ESC Congress
Clinical Collections
Advances in Alzheimer’s

At a glance: The STEP trials

A round-up of the STEP phase 3 clinical trials evaluating semaglutide for weight loss in people with overweight or obesity.
ADVANCED SEARCH
Log in
Top
Pediatric Nephrology
Published in: Pediatric Nephrology 3/2005

01-03-2005 | Review

Orexigenic and anorexigenic mechanisms in the control of nutrition in chronic kidney disease

Authors: Robert H. Mak, Wai Cheung, Roger D. Cone, Daniel L. Marks

Published in: Pediatric Nephrology | Issue 3/2005

Login to get access

Abstract

Malnutrition is defined as abnormalities caused by an inadequate diet, but this term is often used inappropriately to describe the syndrome of loss of body weight with muscle mass being replaced by fatty tissue and declining serum proteins present in adults and children with chronic kidney disease (CKD). This syndrome is more accurately described as cachexia, and manifests as growth failure in children with CKD. Cachexia is common and is an important risk factor for poor quality of life and increased mortality and morbidity in both adults and children with CKD. Anorexia, acidosis and inflammation are important causes of cachexia, but the underlying molecular mechanism is not well understood. Dietary intake is often poor and resting metabolic rate is increased in CKD. The energy cost of growth is increased in experimental CKD. Circulating concentrations of cytokines, such as leptin, tumor necrosis factor-α and interleukins 1 and 6 are increased in patients with CKD and correlate with the degree of cachexia in these individuals. We hypothesize that cytokines signal through orexigenic neuropetides such as agouti-related peptide and neuropeptide Y (NPY), and anorexigenic neuropetides such as proopiomelanocortin and α-melanocyte-stimulating hormone in the arcuate nucleus in the hypothalamus. This signaling system also involves the NPY receptor and the melanocortin receptors and controls appetite and metabolic rate in health and disease. Furthermore, the first order neurons of this system are located outside the blood-brain barrier and can therefore sense the circulating levels of cytokines, as well as long-term satiety hormones such as leptin and insulin and short-term satiety hormones such as ghrelin and peptide (P) YY. There is experimental evidence that this hypothalamic neuropeptide signaling system may have an important role in the pathogenesis of cachexia in CKD. Understanding the molecular mechanism of cachexia in CKD may lead to novel therapeutic strategies.
Literature
1.
Mitch WE (2002) Malnutrition: a frequent misdiagnosis for hemodialysis patients. J Clin Invest 110:437–439CrossRef
2.
Mitch WE, Ramuzzi G (2004) Diets for patients with chronic kidney disease, still worth prescribing. J Am Soc Nephrol 113:115–123
3.
Owen W, Lew N, Liu Y et al. (1993) The urea reduction ratio and serum albumin concentrations as predictors of mortality in patients undergoing hemodialysis. New Engl J Med 329:1001–1008CrossRef
4.
Avram M, Mittman N, Bonomini L et al. (1995) Markers for survival in dialysis. A seven-year prospective study. Am J Kidney Dis 26:209–219
5.
Wong CS, Gipson DS, Gillen DL et al. (2000) Anthropometric measures and risk of death in children with end-stage renal disease. Am J Kidney Dis 36:811–819
6.
Wong CS, Hingorani S, Gillen Dl et al. (2002) Hypoalbuminemia and risk of death in pediatric patients with end-stage renal disease. Kidney Int 61:630–637CrossRef
7.
Holliday MA (1972) Calorie deficiency in children with uremia: effect upon growth. Pediatrics 50:590–595
8.
Kuhlmann U, Schwickardi M, Trebst R, Lange R (2001) Resting metabolic rate in chronic renal failure. J Renal Nutr 11:202–206CrossRef
9.
Betts PR, McGrath G (1974) Growth patterns and dietary intake of children with chronic renal insufficiency. Brit Med J 2:189–193
10.
Simmons JM, Wilson CJ, Potter DE, Holliday MA (1971) Relation of calorie deficiency to growth failure in children on hemodialysis and the growth response to calorie supplementation. New Engl J Med 285:653–656
11.
Arnold WC, Danford D, Holliday M (1983) Effects of calorie supplementation on growth in children with uremia. Kidney Int 24:205–209PubMed
12.
Mehls O, Ritz E, Gilli G, Bartholome K, Beibbrath H, Hohenegger M, Schafnitzel W (1980) Nitrogen metabolism and growth in experimental uremia. Int J Ped Nephrol 1:34–41
13.
Mehls O, Ritz E, Hunziker EB, Eggli P, Henrich U, Zapf J (1988) Improvement of growth and food utilization by human recombinant growth hormone in uremia. Kidney Int 33:45–52PubMed
14.
Betts PR, McGrath G, White RHR (1977) Role of energy supplementation in growth of children with chronic renal insufficiency. Brit Med J 1:416–421
15.
El-Bishti M, Burke J, Gill d, Jones RW, Counahan R, Chantler C (1981) Body composition in children on regular hemodialysis. Clin Nephrol 15:53–60
16.
Jones RW, Ridgen SP, Barratt TM, Chantler C (1982) The effects of chronic renal failure in infancy on growth, nutritional status and body composition. Pediatr Res 16:784–791
17.
Daschner M, Tonshoff B, Blum WF et al. (1998) Inappropriate elevation of serum leptin in children with chronic renal failure. European Study Group for Nutritional Treatment of Chronic Renal Failure in Childhood. J Am Soc Nephrol 9:1074–1079
18.
Schwartz MW, Morton GJ (2002) Obesity: Keeping hunger at bay. Nature 418:595–597CrossRef
19.
Batterham RL, Cowley MA, Small CJ et al. (2002) Gut hormone PYY(3–36) physiologically inhibits food intake. Nature 418:650–654CrossRefPubMed
20.
21.
Larkin M (1998) Thwarting the dwindling progression of cachexia. Lancet 351:1336CrossRef
22.
Inui A (1999) Cancer anorexia-cachexia syndrome: are neuropeptides the key? Cancer Res 59:4493–4501
23.
Kotler DP, Tierney AR, Wang J, Pierson RNJ (1989) Magnitude of body-cell-mass depletion and the timing of death from wasting in AIDS. Am J Clin Nutr 50:444–447PubMed
24.
Plata-Salaman CR (1989) Immunomodulators and feeding regulation: a humoral link between the immune and nervous systems. Brain Behav Immunol 3:193–213CrossRef
25.
Plata-Salaman CR, Borkoski JP(1994) Chemokines/intercrines and central regulation of feeding. Am J Physiol 275:R1711–R1715
26.
Sherry BA, Gelin J, Fong Y, Marano M, Wei H, Cerami A, Lowry SF, Lundholm KG, Moldawer LL (1989) Anticachectin/tumor necrosis factor-alpha antibodies attenuate development of cachexia in tumor models. FASEB J 3:1956–62
27.
Fong Y, Moldawer LL, Marano M et al. (1989) Cachectin/TNF or IL-1 alpha induces cachexia with redistribution of body proteins. Am J Physiol 256(3 Pt 2):R659–65
28.
Plata-Salaman CR, Sonti G, Borkoski JP, Wilson CD, French-Mullen JM (1996) Anorexia induced by chronic central administration of cytokines at estimated pathophysiological concentrations. Physiol Behav 60(3):867–75CrossRef
29.
Marks DL, Ling N, Cone RD (2001) Role of central melanocortin system in cachexia. Cancer Res 61:1432–1438
30.
31.
Halaas J, Gajiwala K, Maffei M et al. (1995) Weight-reducing effects of plasma protein encoded by the obese gene. Science 269:543–549
32.
Sharma K, Considine RV, Michael B et al. (1997) Plasma leptin is partly cleared by the kidney and is elevated in hemodialysis patients. Kidney Int 51(6):1980–5
33.
Johansen KL, Mulligan K, Tai V, Schambelan M (1998) Leptin, body composition and indices of malnutrition in patients on dialysis. J Am Soc Nephrol 9:1080–1984
34.
Stenvinkel P, Heimburger O, Lonnqvist F (1997) Serum leptin concentrations correlate to plasma insulin concentrations independent of body fat content in chronic renal failure. Nephrol Dial Transpl 12:1321–1325CrossRef
35.
Pecoits-Filho R, Nordfors L, Heimburger O, Lindholm B, Anderstam B, Marchlewska A, Stenvinkel P (2002) Soluble leptin receptors and serum leptin in end-stage renal disease: relationship with inflammation and body composition. Eur J Clin Invest 32:811–817CrossRef
36.
Wolf G, Chen S, Han DC, Ziyadeh FN (2002) Leptin and renal disease. Am J Kidney Dis 39:1–11CrossRef
37.
Yoshimoto A, Mori K, Sugawara A et al. (2002) Plasma ghrelin and desacyl ghrelin concentrations in renal failure. J Am Soc Nephrol 13:2748–2752
38.
Rodriguez Ayala E, Pecoits-Filho R, Heimburger O, Lindholm B, Nordfors L, Stenvinkel P (2004) Associations between plasma ghrelin levels and body composition in end-stage renal disease: a longitudinal study. Nephrol Dial Transpl 19:421–426CrossRef
39.
Stenvinkel P, Pecoits-Filho R, Lindholm B (2003) Leptin, ghrelin and proinflammatory cytokines: compounds with nutritional impact in chronic kidney disease? Advances Renal Replace Th 10:332–345CrossRef
40.
Herbelin A, Nguyen AT, Zingraff J, Urena P, Descamps-Latscha B (1990) Influence of uremia and hemodialysis on circulating interleukin-1 and tumor necrosis factor alpha. Kidney Int 37(1):116–25
41.
Bologa RM, Levine DM, Parker TS, Cheigh JS, Serur D, Stenzel KH, Rubin AL (1998) Interleukin-6 predicts hypoalbuminemia, hypocholesterolemia, and mortality in hemodialysis patients. Am J Kidney Dis 32(1):107–14
42.
Goodman MN (1994) Interleukin-6 induces skeletal muscle protein breakdown in rats. P Soc Exp Biol Med 205:182–185
43.
Tsujinaka T, Fujita J, Ebisuri C et al. (1996) Interleukin 6 receptor antibody inhibits muscle atrophy and modulates proteolytic systems in Interleukin 6 transgenic mice. J Clin Invest 97:244–249PubMed
44.
Aguilera A, Codoceo R, Selgas R et al. (1998) Anorexigen (TNF alpha, cholecystokinin) and orexigen (neuropeptide Y) in peritoneal dialysis patients. Their relationship with nutritional parameters. Nephrol Dial Transpl 13:1476–1483CrossRef
45.
Guttridge DC, Mayo MW, Madrid LV et al. (2000) NF-κB induced loss of MyoD messenger RNA: possible role in muscle decay and cachexia. Science 289:2363–2365CrossRef
46.
Plata-Salaman CR (1998) Cytokines and anorexia: a brief overview. Semin Oncol 25:4–11
47.
Airaghi L, Garofalo L, Cutuli MG et al. (2000) Plasma concentrations of alpha melanocyte-stimulating hormone are elevated in patients on chronic haemodialysis. Nephrol Dial Transpl 15:1212–1216CrossRef
48.
Cheung W, Marks DL, Yu PX, Cone RD, Mak RH (2003) Role of the central melanocortin system in the cachexia of uremia. J Am Soc Nephrol 14:326A
Metadata
Title
Orexigenic and anorexigenic mechanisms in the control of nutrition in chronic kidney disease
Authors
Robert H. Mak
Wai Cheung
Roger D. Cone
Daniel L. Marks
Publication date
01-03-2005
Publisher
Springer-Verlag
Published in
Pediatric Nephrology / Issue 3/2005
Print ISSN: 0931-041X
Electronic ISSN: 1432-198X
DOI
https://doi.org/10.1007/s00467-004-1789-1

Other articles of this Issue 3/2005

Pediatric Nephrology 3/2005 Go to the issue

Review

Genomic and non-genomic actions of sex steroids in the growth plate

Review

Genetic regulation of bone mass: from bone density to bone strength

Review

The growth hormone-insulin like growth factor axis revisited: lessons from IGF-1 and IGF-1 receptor gene targeting

Original Article

Rapid development of glomerular injury and renal failure in mice lacking p53R2

Review

The therapeutic potential of novel phosphate binders

Review

Steroid withdrawal in pediatric and adult renal transplant recipients