Intravenous iron in clinical concentrations does not impair haemoglobin measurement

Background Intravenous iron is commonly administered to anaemic patients to treat iron deficiency, but due to its ferric colouration, it may interfere with the spectrophotometric assessment of haemoglobin concentrations. This paper investigates the potential interference of three clinically used int...

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Bibliographic Details
Published in:Annals of clinical biochemistry 2016-03, Vol.53 (2), p.285-287
Main Authors: O’Loughlin, Edmond, Garnett, Peter BJ, Falkner, Nathalie M, Williams, Robin
Format: Article
Language:English
Subjects:
Hemoglobins - analysis
Humans
Infusions, Intravenous
Iron - administration & dosage
Spectrophotometry
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Summary:Background Intravenous iron is commonly administered to anaemic patients to treat iron deficiency, but due to its ferric colouration, it may interfere with the spectrophotometric assessment of haemoglobin concentrations. This paper investigates the potential interference of three clinically used intravenous iron preparations on the measurement of haemoglobin. Methods Haemoglobin concentration was measured for neat and Hartmann’s solution-diluted iron polymaltose, carboxymaltose and sucrose solutions using bedside (Radiometer HemoCue®), point-of-care (Radiometer ABL800 Flex) and laboratory (Abbott CellDyne Sapphire™) devices. Haemoglobin concentration was then assessed with the same devices utilizing anaemic whole blood with the iron solutions added. Results Neat iron preparations registered clinically significant haemoglobin concentrations on bedside and laboratory measurements. When intravenous iron preparations were diluted to clinical concentrations, their effect on haemoglobin measurements, either in isolation or mixed with anaemic blood, was negligible. Conclusion Although neat preparations of intravenous iron do interfere with spectrophotometric analysis of haemoglobin, concentrations likely to be seen post iron infusion do not significantly interfere with haemoglobin measurement.
ISSN:0004-5632
1758-1001
DOI:10.1177/0004563215581401