Management of iron overload in dialysis patients.

Acquired hemosiderosis resulting from massive iron deposits in various organs, including heart, liver, and pancreas, may lead to architectural and functional disturbances of these organs. Even though iron overload can occur in nonuremic as well as in uremic individuals, the dialysis patient is at particular risk for developing hemosiderosis. Many dialysis patients receive exogenous iron from either oral iron therapy or blood transfusions. In addition, these patients seem to be at high risk for retaining iron. A diagnosis of excess iron deposition should be considered if the patient has unexplained cardiomyopathy, hepatic cirrhosis, proximal myopathy, diabetes mellitus, arthropathy, or immune dysfunction such as listeriosis. Several techniques are available for determining iron overload. Diagnostic tests include measuring serum ferritin levels, staining bone marrow preparations for excess iron, measuring tissue hemosiderin concentrations, magnetic resonance imaging, and the deferoxamine (DFO; Desferal) "challenge test." The simplest treatment for iron overload in nonuremic patients is removal of iron by venesection. However, in patients in whom venesection is not feasible, the chelating agent DFO can effectively remove excess iron. In the dialysis patient, DFO therapy can be combined with either dialysis or hemoperfusion to remove the iron-DFO complex that would otherwise be removed by the kidney. DFO therapy in the nondialyzed individual has proven to be successful, but before treatment, the benefits of the treatment must be weighed against possible adverse side effects such as cataracts, changes in color vision, and anaphylaxis. In the dialysis patient, indications for iron removal are less clearly defined.(ABSTRACT TRUNCATED AT 250 WORDS)

[1]  S. Ott,et al.  Changes in bone histology after treatment with desferrioxamine. , 1986, Kidney international. Supplement.

[2]  J. Sondheimer,et al.  Listeriosis in patients with long-term hemodialysis and transfusional iron overload. , 1985, The American journal of medicine.

[3]  R. Dluhy,et al.  Long-term efficacy of deferoxamine iron chelation therapy in adults with acquired transfusional iron overload. , 1985, Archives of internal medicine.

[4]  S. Colan,et al.  Prevention of cardiac disease by subcutaneous deferoxamine in patients with thalassemia major. , 1985, The New England journal of medicine.

[5]  S. Underwood,et al.  DESFERRIOXAMINE TO IMPROVE CARDIAC FUNCTION IN IRON-OVERLOADED PATIENTS WITH THALASSAEMIA MAJOR , 1984, The Lancet.

[6]  D. Rice,et al.  Ferritin Structure and Function , 1984 .

[7]  P. Barré,et al.  EFFECT OF DESFERRIOXAMINE ON REMOVAL OF ALUMINIUM AND IRON BY COATED CHARCOAL HAEMOPERFUSION AND HAEMODIALYSIS , 1983, The Lancet.

[8]  G. Arden,et al.  OCULAR TOXICITY OF HIGH-DOSE INTRAVENOUS DESFERRIOXAMINE , 1983, The Lancet.

[9]  D. Cook,et al.  Osteomalacia in patients with chronic renal failure before dialysis or transplantation. , 1983, The Quarterly journal of medicine.

[10]  R. Falk,et al.  Iron removal during continuous ambulatory peritoneal dialysis using deferoxamine. , 1983, Kidney international.

[11]  E. Björn-Rasmussen IRON ABSORPTION: PRESENT KNOWLEDGE AND CONTROVERSIES , 1983, The Lancet.

[12]  O. Castro,et al.  N,N-dimethylglycine for epilepsy. , 1983 .

[13]  J. Tripp,et al.  Magnetic-susceptibility measurement of human iron stores. , 1982, The New England journal of medicine.

[14]  B. Ma,et al.  Don't overlook iron overload. , 1982 .

[15]  M. rd,et al.  Hemosiderosis in a dialysis patient: treatment with hemofiltration and deferoxamine chelation therapy. , 1982 .

[16]  C. Finch,et al.  Perspectives in iron metabolism. , 1982, The New England journal of medicine.

[17]  B. V. van Oost,et al.  Listeria monocytogenes meningitis and decreased phagocytosis associated with iron overload. , 1982, British medical journal.

[18]  A. Norman,et al.  Vitamin-D-resistant osteomalacia in hemodialysis patients lacking secondary hyperparathyroidism. , 1981, Annals of internal medicine.

[19]  E. Gómez,et al.  SERUM FERRITIN AND HLA ANTIGENS IN PATIENTS ON MAINTENANCE HAEMODIALYSIS , 1981, The Lancet.

[20]  D. Weatherall,et al.  IRON CHELATION WITH ORAL DESFERRIOXAMINE , 1980, The Lancet.

[21]  J. Winchester,et al.  IRON-OVERLOAD-ASSOCIATED MYOPATHY IN PATIENTS ON MAINTENANCE HÆMODIALYSIS: A HISTOCOMPATIBILITY-LINKED DISORDER , 1980, The Lancet.

[22]  R. Green,et al.  CLINICAL TRIAL OF DESFERRIOXAMINE ENTRAPPED IN RED CELL GHOSTS , 1980, The Lancet.

[23]  Jimmy D Bell,et al.  Serum ferritin assay and bone-marrow iron stores in patients on maintenance hemodialysis. , 1980, Kidney international.

[24]  D. Weatherall,et al.  Iron metabolism in haemodialysis patients. A study of the management of iron therapy and overload. , 1979, The Quarterly journal of medicine.

[25]  D. Weatherall,et al.  Iron induced increase in red cell size in haemodialysis patients. , 1979, The Quarterly journal of medicine.

[26]  R. Fauchet,et al.  Idiopathic hemochromatosis. Demonstration of recessive transmission and early detection by family HLA typing. , 1977, The New England journal of medicine.

[27]  J. Cook,et al.  Effect of blood donation on iron stores as evaluated by serum ferritin , 1977 .

[28]  W. Anderson,et al.  Continuous Subcutaneous Administration of Deferoxamine in Patients with Iron Overload , 1977 .

[29]  N. Milman,et al.  Iron absorption in non-dialysed patients with chronic renal failure, in patients on regular hemodialysis, and in renal transplanted patients. , 1977, Danish medical bulletin.

[30]  P. Ackrill,et al.  Hemosiderosis in a patient on regular hemodialysis: treatment by desferrioxamine. , 1976, Clinical nephrology.

[31]  A. Harmuth-Hoene,et al.  Pharmacology and therapeutic applications of agents used in heavy metal poisoning , 1976 .

[32]  J. Cook,et al.  A clinical evaluation of serum ferritin as an index of iron stores. , 1974, The New England journal of medicine.

[33]  L. Harker,et al.  Evaluation of storage iron by chelates. , 1968, The American journal of medicine.