Hypersensitivity reactions and deaths associated with intravenous iron preparations

doi:10.1093/ndt/gfh820

NDT Advance Access originally published online on April 26, 2005
Nephrology Dialysis Transplantation 2005 20(7):1443-1449; doi:10.1093/ndt/gfh820

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Original Article

Hypersensitivity reactions and deaths associated with intravenous iron preparations

George R. Bailie¹^,2^,3, John A. Clark⁴, Christi E. Lane⁴ and Peter L. Lane⁵

¹ Albany Nephrology Pharmacy (ANephRx) Group, Albany, NY, ² Nephrology Pharmacy Associates, Inc., Ann Arbor, MI, ³ Renal Research Institute, LLC, New York, NY, ⁴ Galt Associates, Blue Bell, PA and ⁵ Luitpold Pharmaceuticals, Inc., Norristown, PA, USA

Correspondence and offprint requests to: George R. Bailie, PharmD, PhD, Albany College of Pharmacy, 106 New Scotland Avenue, Albany, NY 12208, USA. Email: bailieg{at}acp.edu

Background. Parenteral iron therapy is an accepted adjunctivemanagement of anaemia in kidney disease. Newer agents may havefewer severe hypersensitivity adverse events (AE) compared withiron dextrans (ID). The rate of type 1 AE to iron sucrose (IS)and sodium ferric gluconate (SFG) relative to ID is unclear.We used the US Food and Drug Administration's Freedom of Information(FOI) surveillance database to compare the type 1 AE profilesfor the three intravenous iron preparations available in theUnited States.

Methods. We tabulated reports received by the FOI database betweenJanuary 1997 and September 2002, and calculated 100 mg doseequivalents for the treated population for each agent. We developedfour clinical categories describing hypersensitivity AE (anaphylaxis,anaphylactoid reaction, urticaria and angioedema) and an algorithmdescribing anaphylaxis, for specific analyses.

Results. All-event reporting rates were 29.2, 10.5 and 4.2 reports/million100 mg dose equivalents, while all-fatal-event reporting rateswere 1.4, 0.6 and 0.0 reports/million 100 mg dose equivalentsfor ID, SFG and IS, respectively. ID had the highest reportingrates in all four clinical categories and the anaphylaxis algorithm.SFG had intermediate reporting rates for urticaria, anaphylactoidreaction and the anaphylaxis algorithm, and a zero reportingrate for the anaphylaxis clinical category. IS had either thelowest or a zero reporting rate in all clinical categories/algorithm.

Conclusions. These findings confirm a higher risk for AE, especiallyserious type 1 reactions, with ID therapy than with newer intravenousiron products and also suggest that IS carries the lowest riskfor hypersensitivity reactions.

Keywords: hypersensitivity reactions; intravenous iron; iron dextran; iron sucrose; sodium ferric gluconate; type 1 reactions

The authors wish it to be known that P.L. Lane died before thismanuscript was completed.

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