NIMO-CKD-UK: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney disease

NIMO-CKD-UK: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney disease

Abstract Background Intravenous iron is often used to treat iron deficiency anaemia in non-dialysis chronic kidney disease (ND-CKD), but the optimal dosing regimen remains unclear. We evaluated the impact of high- versus low-dose intravenous iron isomaltoside on the probability of retreatment with i...

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Main Authors: Philip A. Kalra, Sunil Bhandari, Michael Spyridon, Rachel Davison, Sarah Lawman, Ashraf Mikhail, David Reaich, Nick Pritchard, Kieran McCafferty, Jason Moore
Format: Article
Language:English
Published: BMC 2020-12-01
Series:BMC Nephrology
Subjects:
Anaemia
Chronic kidney disease
Ferric derisomaltose
Intravenous iron
Iron deficiency
Iron isomaltoside 1000
Online Access:https://doi.org/10.1186/s12882-020-02180-2
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spelling doaj-3a9f5cfdaf81468393396691dd1293802020-12-13T12:39:27ZengBMCBMC Nephrology1471-23692020-12-0121111010.1186/s12882-020-02180-2NIMO-CKD-UK: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney diseasePhilip A. Kalra0Sunil Bhandari1Michael Spyridon2Rachel Davison3Sarah Lawman4Ashraf Mikhail5David Reaich6Nick Pritchard7Kieran McCafferty8Jason Moore9Salford Royal NHS Foundation TrustHull University Teaching Hospitals NHS TrustPharmacosmos UKSunderland Royal HospitalRoyal Sussex County HospitalMorriston HospitalThe James Cook University HospitalAddenbrooke’s University HospitalRoyal London University HospitalRoyal Devon and Exeter University HospitalAbstract Background Intravenous iron is often used to treat iron deficiency anaemia in non-dialysis chronic kidney disease (ND-CKD), but the optimal dosing regimen remains unclear. We evaluated the impact of high- versus low-dose intravenous iron isomaltoside on the probability of retreatment with intravenous iron in iron-deficient ND-CKD patients. Methods This real-world, prospective, observational study collected data from 256 ND-CKD patients treated for anaemia in the UK. Following an initial course of iron isomaltoside, patients were followed for ≥12 months. Iron dose and the need for retreatment were determined at the investigators’ discretion. The primary study outcome was the need for retreatment at 52 weeks compared between patients who received >1000 mg of iron during Course 1 and those who received ≤1000 mg. Safety was evaluated through adverse drug reactions. Results The probability of retreatment at Week 52 was significantly lower in the >1000 mg iron group (n = 58) versus the ≤1000 mg group (n = 198); hazard ratio (95% confidence interval [CI]): 0.46 (0.20, 0.91); p = 0.012. Mean (95% CI) haemoglobin increased by 6.58 (4.94, 8.21) g/L in the ≤1000 mg group and by 10.59 (7.52, 13.66) g/L in the >1000 mg group (p = 0.024). Changes in other blood and iron parameters were not significantly different between the two groups. Administering >1000 mg of iron isomaltoside saved 8.6 appointments per 100 patients compared to ≤1000 mg. No serious adverse drug reactions were reported. Of the patients who received ≤1000 mg of iron in this study, 82.3% were eligible for a dose >1000 mg. Conclusions The >1000 mg iron isomaltoside regimen reduced the probability of retreatment, achieved a greater haemoglobin response irrespective of erythropoiesis-stimulating agent treatment, and reduced the total number of appointments required, compared to the ≤1000 mg regimen. Many of the patients who received ≤1000 mg of iron were eligible for >1000 mg, indicating that there was considerable underdosing in this study. Trial registration ClinicalTrials.gov NCT02546154 , 10 September 2015.https://doi.org/10.1186/s12882-020-02180-2AnaemiaChronic kidney diseaseFerric derisomaltoseIntravenous ironIron deficiencyIron isomaltoside 1000
collection DOAJ
language English
format Article
sources DOAJ
author Philip A. Kalra
Sunil Bhandari
Michael Spyridon
Rachel Davison
Sarah Lawman
Ashraf Mikhail
David Reaich
Nick Pritchard
Kieran McCafferty
Jason Moore
spellingShingle Philip A. Kalra
Sunil Bhandari
Michael Spyridon
Rachel Davison
Sarah Lawman
Ashraf Mikhail
David Reaich
Nick Pritchard
Kieran McCafferty
Jason Moore
NIMO-CKD-UK: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney disease
BMC Nephrology
Anaemia
Chronic kidney disease
Ferric derisomaltose
Intravenous iron
Iron deficiency
Iron isomaltoside 1000
author_facet Philip A. Kalra
Sunil Bhandari
Michael Spyridon
Rachel Davison
Sarah Lawman
Ashraf Mikhail
David Reaich
Nick Pritchard
Kieran McCafferty
Jason Moore
author_sort Philip A. Kalra
title NIMO-CKD-UK: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney disease
title_short NIMO-CKD-UK: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney disease
title_full NIMO-CKD-UK: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney disease
title_fullStr NIMO-CKD-UK: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney disease
title_full_unstemmed NIMO-CKD-UK: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney disease
title_sort nimo-ckd-uk: a real-world, observational study of iron isomaltoside in patients with iron deficiency anaemia and chronic kidney disease
publisher BMC
series BMC Nephrology
issn 1471-2369
publishDate 2020-12-01
description Abstract Background Intravenous iron is often used to treat iron deficiency anaemia in non-dialysis chronic kidney disease (ND-CKD), but the optimal dosing regimen remains unclear. We evaluated the impact of high- versus low-dose intravenous iron isomaltoside on the probability of retreatment with intravenous iron in iron-deficient ND-CKD patients. Methods This real-world, prospective, observational study collected data from 256 ND-CKD patients treated for anaemia in the UK. Following an initial course of iron isomaltoside, patients were followed for ≥12 months. Iron dose and the need for retreatment were determined at the investigators’ discretion. The primary study outcome was the need for retreatment at 52 weeks compared between patients who received >1000 mg of iron during Course 1 and those who received ≤1000 mg. Safety was evaluated through adverse drug reactions. Results The probability of retreatment at Week 52 was significantly lower in the >1000 mg iron group (n = 58) versus the ≤1000 mg group (n = 198); hazard ratio (95% confidence interval [CI]): 0.46 (0.20, 0.91); p = 0.012. Mean (95% CI) haemoglobin increased by 6.58 (4.94, 8.21) g/L in the ≤1000 mg group and by 10.59 (7.52, 13.66) g/L in the >1000 mg group (p = 0.024). Changes in other blood and iron parameters were not significantly different between the two groups. Administering >1000 mg of iron isomaltoside saved 8.6 appointments per 100 patients compared to ≤1000 mg. No serious adverse drug reactions were reported. Of the patients who received ≤1000 mg of iron in this study, 82.3% were eligible for a dose >1000 mg. Conclusions The >1000 mg iron isomaltoside regimen reduced the probability of retreatment, achieved a greater haemoglobin response irrespective of erythropoiesis-stimulating agent treatment, and reduced the total number of appointments required, compared to the ≤1000 mg regimen. Many of the patients who received ≤1000 mg of iron were eligible for >1000 mg, indicating that there was considerable underdosing in this study. Trial registration ClinicalTrials.gov NCT02546154 , 10 September 2015.
topic Anaemia
Chronic kidney disease
Ferric derisomaltose
Intravenous iron
Iron deficiency
Iron isomaltoside 1000
url https://doi.org/10.1186/s12882-020-02180-2
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