Diagnostic value of iron indices in hemodialysis patients receiving epoetin

James S. Kaufman; Domenic J. Reda; Carol L. Fye; David S. Goldfarb; William G. Henderson; Jack G. Kleinman; Carlos A. Vaamonde; J. S. Kaufman; R. A. Cxypoliski; P. London; E. Young; P. Rose; G. Schmitt; K. Bold; J. Briggs; V. Lee; D. Kaji; F. M. Ohsumi; H. Chen; M. B. Ganz; S. Nurko; D. G. Linn; R. E. Cronin; V. N. Kemp; M. G. Saklayen; S. Adams; Y. J. Jenkins; M. Davis; S. Sastrasinh; K. A. Lordi; Z. Nawab; B. Kepka; G. Dolson; R. Therappel; A. Bonner; H. Hasbargen; S. C. Nielsen; A. Frame; G. Shah; D. Lim; C. A. Vaamonde; L. Cason; J. Edelstein; C. Serrano; J. G. Kleinman; J. Schramm; E. Sheahan-Meyer; B. J. Jackson; V. Batuman; D. M. Archie; D. S. Goldfarb; R. Discipulo; T. E. Dixon; E. Lamonica; T. Albert; R. L. Jamison; D. L. Usi; P. M. Palevsky; P. Baltz Salai; S. Anderson; M. Wolfson; M. Cummings-Cosgrove; G. Feldman; M. S. Katz; J. A. Burns; S. C. Thomson; M. V. Meek; C. Rosado; P. Carde; J. Bou; U. F. Michael; L. F. Kirlin; J. S. Kaufman; C. L. Fye; D. S. Goldfarb; W. G. Henderson; D. J. Reda; J. G. Kleinman; C. A. Vaamonde; D. J. Reda; W. G. Henderson; D. Semlow; L. Anfinsen; B. Mackay; C. L. Fye; M. R. Sather; F. R. Chacon; M. Drago; W. H. Gagne; T. I. Steinman; A. Nissenson; R. D. Swartz; M. Symons; J. Feussner; S. Berkowitz; P. Huang; D. Deykin; J. Gold

doi:10.1046/j.1523-1755.2001.00800.x

Diagnostic value of iron indices in hemodialysis patients receiving epoetin

James S. Kaufman, Domenic J. Reda, Carol L. Fye, David S. Goldfarb, William G. Henderson, Jack G. Kleinman, Carlos A. Vaamonde, J. S. Kaufman, R. A. Cxypoliski, P. London, E. Young, P. Rose, G. Schmitt, K. Bold, J. Briggs, V. Lee, D. Kaji, F. M. Ohsumi, H. Chen, M. B. GanzS. Nurko, D. G. Linn, R. E. Cronin, V. N. Kemp, M. G. Saklayen, S. Adams, Y. J. Jenkins, M. Davis, S. Sastrasinh, K. A. Lordi, Z. Nawab, B. Kepka, G. Dolson, R. Therappel, A. Bonner, H. Hasbargen, S. C. Nielsen, A. Frame, G. Shah, D. Lim, C. A. Vaamonde, L. Cason, J. Edelstein, C. Serrano, J. G. Kleinman, J. Schramm, E. Sheahan-Meyer, B. J. Jackson, V. Batuman, D. M. Archie, D. S. Goldfarb, R. Discipulo, T. E. Dixon, E. Lamonica, T. Albert, R. L. Jamison, D. L. Usi, P. M. Palevsky, P. Baltz Salai, S. Anderson, M. Wolfson, M. Cummings-Cosgrove, G. Feldman, M. S. Katz, J. A. Burns, S. C. Thomson, M. V. Meek, C. Rosado, P. Carde, J. Bou, U. F. Michael, L. F. Kirlin, J. S. Kaufman, C. L. Fye, D. S. Goldfarb, W. G. Henderson, D. J. Reda, J. G. Kleinman, C. A. Vaamonde, D. J. Reda, W. G. Henderson, D. Semlow, L. Anfinsen, B. Mackay, C. L. Fye, M. R. Sather, F. R. Chacon, M. Drago, W. H. Gagne, T. I. Steinman, A. Nissenson, R. D. Swartz, M. Symons, J. Feussner, S. Berkowitz, P. Huang, D. Deykin, J. Gold

Internal Medicine

Research output: Contribution to journal › Article › peer-review

20 Scopus citations

Abstract

Background. Iron deficiency remains a common cause of hyporesponsiveness to epoetin in hemodialysis patients. However, considerable controversy exists regarding the best strategies for diagnosis and treatment. Methods. As part of a multicenter randomized clinical trial of intravenous versus subcutaneous administration of epoetin, we made monthly determinations of serum iron, total iron binding capacity, percentage transferrin saturation, and serum ferritin. If a patient had serum ferritin <100 ng/mL or the combination of serum ferritin <400 ng/mL and a transferrin saturation <20%, he/she received parenteral iron, given as iron dextran 100 mg at ten consecutive dialysis sessions. We analyzed parenteral iron use during the trial, the effect of its administration on iron indices and epoetin dose, and the ability of the iron indices to predict a reduction in epoetin dose in response to parenteral iron administration. Results. Eighty-seven percent of the 208 patients required parenteral iron to maintain adequate iron stores at an average dose of 1516 mg over 41.7 weeks, or 36 mg/week. Only two of 180 patients experienced serious reactions to intravenous iron administration. Two thirds of the patients receiving parenteral iron had a decrease in their epoetin requirement of at least 30 U/kg/week compared with 29% of Patients who did not receive iron (P = 0.004). The average dose decrease 12 weeks after initiating iron therapy was 1763 U/week. A serum ferritin <200 ng/mL had the best positive predictive value (76%) for predicting a response to parenteral iron administration, but it still had limited clinical utility. Conclusions. Iron deficiency commonly develops during epoetin therapy, and parenteral iron administration may result in a clinically significant reduction in epoetin dose. The use of transferrin saturation or serum ferritin as an indicator for parenteral iron administration has limited utility.

Original language	English (US)
Pages (from-to)	300-308
Number of pages	9
Journal	Kidney international
Volume	60
Issue number	1
DOIs	https://doi.org/10.1046/j.1523-1755.2001.00800.x
State	Published - Jul 1 2001

Keywords

Anemia
Parenteral iron
Recombinant human erythropoietin
Serum ferritin
Transferrin saturation

ASJC Scopus subject areas

Nephrology

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10.1046/j.1523-1755.2001.00800.x

Cite this

Kaufman, J. S., Reda, D. J., Fye, C. L., Goldfarb, D. S., Henderson, W. G., Kleinman, J. G., Vaamonde, C. A., Kaufman, J. S., Cxypoliski, R. A., London, P., Young, E., Rose, P., Schmitt, G., Bold, K., Briggs, J., Lee, V., Kaji, D., Ohsumi, F. M., Chen, H., ... Gold, J. (2001). Diagnostic value of iron indices in hemodialysis patients receiving epoetin. Kidney international, 60(1), 300-308. https://doi.org/10.1046/j.1523-1755.2001.00800.x

Kaufman, JS, Reda, DJ, Fye, CL, Goldfarb, DS, Henderson, WG, Kleinman, JG, Vaamonde, CA, Kaufman, JS, Cxypoliski, RA, London, P, Young, E, Rose, P, Schmitt, G, Bold, K, Briggs, J, Lee, V, Kaji, D, Ohsumi, FM, Chen, H, Ganz, MB, Nurko, S, Linn, DG, Cronin, RE, Kemp, VN, Saklayen, MG, Adams, S, Jenkins, YJ, Davis, M, Sastrasinh, S, Lordi, KA, Nawab, Z, Kepka, B, Dolson, G, Therappel, R, Bonner, A, Hasbargen, H, Nielsen, SC, Frame, A, Shah, G, Lim, D, Vaamonde, CA, Cason, L, Edelstein, J, Serrano, C, Kleinman, JG, Schramm, J, Sheahan-Meyer, E, Jackson, BJ, Batuman, V, Archie, DM, Goldfarb, DS, Discipulo, R, Dixon, TE, Lamonica, E, Albert, T, Jamison, RL, Usi, DL, Palevsky, PM, Baltz Salai, P, Anderson, S, Wolfson, M, Cummings-Cosgrove, M, Feldman, G, Katz, MS, Burns, JA, Thomson, SC, Meek, MV, Rosado, C, Carde, P, Bou, J, Michael, UF, Kirlin, LF, Kaufman, JS, Fye, CL, Goldfarb, DS, Henderson, WG, Reda, DJ, Kleinman, JG, Vaamonde, CA, Reda, DJ, Henderson, WG, Semlow, D, Anfinsen, L, Mackay, B, Fye, CL, Sather, MR, Chacon, FR, Drago, M, Gagne, WH, Steinman, TI, Nissenson, A, Swartz, RD, Symons, M, Feussner, J, Berkowitz, S, Huang, P, Deykin, D & Gold, J 2001, 'Diagnostic value of iron indices in hemodialysis patients receiving epoetin', Kidney international, vol. 60, no. 1, pp. 300-308. https://doi.org/10.1046/j.1523-1755.2001.00800.x

@article{493fa49a5db54b35bf695a096dddf981,

title = "Diagnostic value of iron indices in hemodialysis patients receiving epoetin",

abstract = "Background. Iron deficiency remains a common cause of hyporesponsiveness to epoetin in hemodialysis patients. However, considerable controversy exists regarding the best strategies for diagnosis and treatment. Methods. As part of a multicenter randomized clinical trial of intravenous versus subcutaneous administration of epoetin, we made monthly determinations of serum iron, total iron binding capacity, percentage transferrin saturation, and serum ferritin. If a patient had serum ferritin <100 ng/mL or the combination of serum ferritin <400 ng/mL and a transferrin saturation <20%, he/she received parenteral iron, given as iron dextran 100 mg at ten consecutive dialysis sessions. We analyzed parenteral iron use during the trial, the effect of its administration on iron indices and epoetin dose, and the ability of the iron indices to predict a reduction in epoetin dose in response to parenteral iron administration. Results. Eighty-seven percent of the 208 patients required parenteral iron to maintain adequate iron stores at an average dose of 1516 mg over 41.7 weeks, or 36 mg/week. Only two of 180 patients experienced serious reactions to intravenous iron administration. Two thirds of the patients receiving parenteral iron had a decrease in their epoetin requirement of at least 30 U/kg/week compared with 29% of Patients who did not receive iron (P = 0.004). The average dose decrease 12 weeks after initiating iron therapy was 1763 U/week. A serum ferritin <200 ng/mL had the best positive predictive value (76%) for predicting a response to parenteral iron administration, but it still had limited clinical utility. Conclusions. Iron deficiency commonly develops during epoetin therapy, and parenteral iron administration may result in a clinically significant reduction in epoetin dose. The use of transferrin saturation or serum ferritin as an indicator for parenteral iron administration has limited utility.",

keywords = "Anemia, Parenteral iron, Recombinant human erythropoietin, Serum ferritin, Transferrin saturation",

author = "Kaufman, {James S.} and Reda, {Domenic J.} and Fye, {Carol L.} and Goldfarb, {David S.} and Henderson, {William G.} and Kleinman, {Jack G.} and Vaamonde, {Carlos A.} and Kaufman, {J. S.} and Cxypoliski, {R. A.} and P. London and E. Young and P. Rose and G. Schmitt and K. Bold and J. Briggs and V. Lee and D. Kaji and Ohsumi, {F. M.} and H. Chen and Ganz, {M. B.} and S. Nurko and Linn, {D. G.} and Cronin, {R. E.} and Kemp, {V. N.} and Saklayen, {M. G.} and S. Adams and Jenkins, {Y. J.} and M. Davis and S. Sastrasinh and Lordi, {K. A.} and Z. Nawab and B. Kepka and G. Dolson and R. Therappel and A. Bonner and H. Hasbargen and Nielsen, {S. C.} and A. Frame and G. Shah and D. Lim and Vaamonde, {C. A.} and L. Cason and J. Edelstein and C. Serrano and Kleinman, {J. G.} and J. Schramm and E. Sheahan-Meyer and Jackson, {B. J.} and V. Batuman and Archie, {D. M.} and Goldfarb, {D. S.} and R. Discipulo and Dixon, {T. E.} and E. Lamonica and T. Albert and Jamison, {R. L.} and Usi, {D. L.} and Palevsky, {P. M.} and {Baltz Salai}, P. and S. Anderson and M. Wolfson and M. Cummings-Cosgrove and G. Feldman and Katz, {M. S.} and Burns, {J. A.} and Thomson, {S. C.} and Meek, {M. V.} and C. Rosado and P. Carde and J. Bou and Michael, {U. F.} and Kirlin, {L. F.} and Kaufman, {J. S.} and Fye, {C. L.} and Goldfarb, {D. S.} and Henderson, {W. G.} and Reda, {D. J.} and Kleinman, {J. G.} and Vaamonde, {C. A.} and Reda, {D. J.} and Henderson, {W. G.} and D. Semlow and L. Anfinsen and B. Mackay and Fye, {C. L.} and Sather, {M. R.} and Chacon, {F. R.} and M. Drago and Gagne, {W. H.} and Steinman, {T. I.} and A. Nissenson and Swartz, {R. D.} and M. Symons and J. Feussner and S. Berkowitz and P. Huang and D. Deykin and J. Gold",

note = "Funding Information: The study was supported by the Cooperative Studies Program of the Department of Veterans Affairs Research and Development Service, by the Agency for Healthcare Research and Quality, and by an unrestricted grant to Friends of Medical Research (a not-for-profit foundation) from Amgen. We are indebted to Amgen for supplying epoetin alfa (Epogen{\textregistered}), to Schein Pharmaceutical, for supplying parenteral iron dextran (INFeD{\textregistered}), and to Central Pharmaceuticals-Schwarz Pharma for supplying polysaccharide-iron complex (Niferex-150{\textregistered}). Portions of this article were presented at the 1996 and 1998 annual meetings of the American Society of Nephrology, and were published in abstract form (J Am Soc Nephrol 7:1450, 1996, and J Am Soc Nephrol 9:213A, 1998).",

year = "2001",

month = jul,

day = "1",

doi = "10.1046/j.1523-1755.2001.00800.x",

language = "English (US)",

volume = "60",

pages = "300--308",

journal = "Kidney international",

issn = "0085-2538",

publisher = "Nature Publishing Group",

number = "1",

}

TY - JOUR

T1 - Diagnostic value of iron indices in hemodialysis patients receiving epoetin

AU - Kaufman, James S.

AU - Reda, Domenic J.

AU - Fye, Carol L.

AU - Goldfarb, David S.

AU - Henderson, William G.

AU - Kleinman, Jack G.

AU - Vaamonde, Carlos A.

AU - Kaufman, J. S.

AU - Cxypoliski, R. A.

AU - London, P.

AU - Young, E.

AU - Rose, P.

AU - Schmitt, G.

AU - Bold, K.

AU - Briggs, J.

AU - Lee, V.

AU - Kaji, D.

AU - Ohsumi, F. M.

AU - Chen, H.

AU - Ganz, M. B.

AU - Nurko, S.

AU - Linn, D. G.

AU - Cronin, R. E.

AU - Kemp, V. N.

AU - Saklayen, M. G.

AU - Adams, S.

AU - Jenkins, Y. J.

AU - Davis, M.

AU - Sastrasinh, S.

AU - Lordi, K. A.

AU - Nawab, Z.

AU - Kepka, B.

AU - Dolson, G.

AU - Therappel, R.

AU - Bonner, A.

AU - Hasbargen, H.

AU - Nielsen, S. C.

AU - Frame, A.

AU - Shah, G.

AU - Lim, D.

AU - Vaamonde, C. A.

AU - Cason, L.

AU - Edelstein, J.

AU - Serrano, C.

AU - Kleinman, J. G.

AU - Schramm, J.

AU - Sheahan-Meyer, E.

AU - Jackson, B. J.

AU - Batuman, V.

AU - Archie, D. M.

AU - Goldfarb, D. S.

AU - Discipulo, R.

AU - Dixon, T. E.

AU - Lamonica, E.

AU - Albert, T.

AU - Jamison, R. L.

AU - Usi, D. L.

AU - Palevsky, P. M.

AU - Baltz Salai, P.

AU - Anderson, S.

AU - Wolfson, M.

AU - Cummings-Cosgrove, M.

AU - Feldman, G.

AU - Katz, M. S.

AU - Burns, J. A.

AU - Thomson, S. C.

AU - Meek, M. V.

AU - Rosado, C.

AU - Carde, P.

AU - Bou, J.

AU - Michael, U. F.

AU - Kirlin, L. F.

AU - Kaufman, J. S.

AU - Fye, C. L.

AU - Goldfarb, D. S.

AU - Henderson, W. G.

AU - Reda, D. J.

AU - Kleinman, J. G.

AU - Vaamonde, C. A.

AU - Reda, D. J.

AU - Henderson, W. G.

AU - Semlow, D.

AU - Anfinsen, L.

AU - Mackay, B.

AU - Fye, C. L.

AU - Sather, M. R.

AU - Chacon, F. R.

AU - Drago, M.

AU - Gagne, W. H.

AU - Steinman, T. I.

AU - Nissenson, A.

AU - Swartz, R. D.

AU - Symons, M.

AU - Feussner, J.

AU - Berkowitz, S.

AU - Huang, P.

AU - Deykin, D.

AU - Gold, J.

N1 - Funding Information: The study was supported by the Cooperative Studies Program of the Department of Veterans Affairs Research and Development Service, by the Agency for Healthcare Research and Quality, and by an unrestricted grant to Friends of Medical Research (a not-for-profit foundation) from Amgen. We are indebted to Amgen for supplying epoetin alfa (Epogen®), to Schein Pharmaceutical, for supplying parenteral iron dextran (INFeD®), and to Central Pharmaceuticals-Schwarz Pharma for supplying polysaccharide-iron complex (Niferex-150®). Portions of this article were presented at the 1996 and 1998 annual meetings of the American Society of Nephrology, and were published in abstract form (J Am Soc Nephrol 7:1450, 1996, and J Am Soc Nephrol 9:213A, 1998).

PY - 2001/7/1

Y1 - 2001/7/1

N2 - Background. Iron deficiency remains a common cause of hyporesponsiveness to epoetin in hemodialysis patients. However, considerable controversy exists regarding the best strategies for diagnosis and treatment. Methods. As part of a multicenter randomized clinical trial of intravenous versus subcutaneous administration of epoetin, we made monthly determinations of serum iron, total iron binding capacity, percentage transferrin saturation, and serum ferritin. If a patient had serum ferritin <100 ng/mL or the combination of serum ferritin <400 ng/mL and a transferrin saturation <20%, he/she received parenteral iron, given as iron dextran 100 mg at ten consecutive dialysis sessions. We analyzed parenteral iron use during the trial, the effect of its administration on iron indices and epoetin dose, and the ability of the iron indices to predict a reduction in epoetin dose in response to parenteral iron administration. Results. Eighty-seven percent of the 208 patients required parenteral iron to maintain adequate iron stores at an average dose of 1516 mg over 41.7 weeks, or 36 mg/week. Only two of 180 patients experienced serious reactions to intravenous iron administration. Two thirds of the patients receiving parenteral iron had a decrease in their epoetin requirement of at least 30 U/kg/week compared with 29% of Patients who did not receive iron (P = 0.004). The average dose decrease 12 weeks after initiating iron therapy was 1763 U/week. A serum ferritin <200 ng/mL had the best positive predictive value (76%) for predicting a response to parenteral iron administration, but it still had limited clinical utility. Conclusions. Iron deficiency commonly develops during epoetin therapy, and parenteral iron administration may result in a clinically significant reduction in epoetin dose. The use of transferrin saturation or serum ferritin as an indicator for parenteral iron administration has limited utility.

AB - Background. Iron deficiency remains a common cause of hyporesponsiveness to epoetin in hemodialysis patients. However, considerable controversy exists regarding the best strategies for diagnosis and treatment. Methods. As part of a multicenter randomized clinical trial of intravenous versus subcutaneous administration of epoetin, we made monthly determinations of serum iron, total iron binding capacity, percentage transferrin saturation, and serum ferritin. If a patient had serum ferritin <100 ng/mL or the combination of serum ferritin <400 ng/mL and a transferrin saturation <20%, he/she received parenteral iron, given as iron dextran 100 mg at ten consecutive dialysis sessions. We analyzed parenteral iron use during the trial, the effect of its administration on iron indices and epoetin dose, and the ability of the iron indices to predict a reduction in epoetin dose in response to parenteral iron administration. Results. Eighty-seven percent of the 208 patients required parenteral iron to maintain adequate iron stores at an average dose of 1516 mg over 41.7 weeks, or 36 mg/week. Only two of 180 patients experienced serious reactions to intravenous iron administration. Two thirds of the patients receiving parenteral iron had a decrease in their epoetin requirement of at least 30 U/kg/week compared with 29% of Patients who did not receive iron (P = 0.004). The average dose decrease 12 weeks after initiating iron therapy was 1763 U/week. A serum ferritin <200 ng/mL had the best positive predictive value (76%) for predicting a response to parenteral iron administration, but it still had limited clinical utility. Conclusions. Iron deficiency commonly develops during epoetin therapy, and parenteral iron administration may result in a clinically significant reduction in epoetin dose. The use of transferrin saturation or serum ferritin as an indicator for parenteral iron administration has limited utility.

KW - Anemia

KW - Parenteral iron

KW - Recombinant human erythropoietin

KW - Serum ferritin

KW - Transferrin saturation

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UR - http://www.scopus.com/inward/citedby.url?scp=0034955115&partnerID=8YFLogxK

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DO - 10.1046/j.1523-1755.2001.00800.x

M3 - Article

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AN - SCOPUS:0034955115

SN - 0085-2538

VL - 60

SP - 300

EP - 308

JO - Kidney international

JF - Kidney international

IS - 1

ER -

Diagnostic value of iron indices in hemodialysis patients receiving epoetin

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