EffiCacy and sAfEty of Low doSe orAl iRon for Anaemia in IBD

Last updated: March 13, 2024
Sponsor: Liverpool University Hospitals NHS Foundation Trust
Overall Status: Active - Recruiting

Phase

3

Condition

Crohn's Disease (Pediatric)

Gastrointestinal Diseases And Disorders

Ulcerative Colitis

Treatment

Ferrous fumarate syrup 2.5ml/70mg(45mg elemental iron)

Ferrous fumarate syrup 2.5ml/70mg (22.5mg elemental iron)

Ferrous fumarate syrup 2.5ml/70mg (90mg elemental iron)

Clinical Study ID

NCT06321887
5155
  • Ages 18-79
  • All Genders
  • Accepts Healthy Volunteers

Study Summary

Iron deficiency anaemia (IDA) is common in inflammatory bowel disease (IBD). However, although iron is commonly prescribed, the amount of elemental iron needed to achieve clinical efficacy, and the optimal method of supplementation, are under debate. This pilot study aims to investigate the efficacy and safety of low dose and standard dose oral iron preparations for the treatment of IDA in patients with IBD.

Eligibility Criteria

Inclusion

Inclusion Criteria:

  • Patient is willing to participate in the study and has signed the informed consent.
  • Patients aged 18-80 years.
  • Patients diagnosed with Crohn's disease or ulcerative colitis diagnosed byconventional clinical, radiological and histological criteria.
  • Remission or active disease.
  • Haemoglobin level 7-13 g/dL men, 7-12 g/dL women and ferritin <30, normal B12 andfolate (or ferritin <100 but iron sats <16 in the presence of inflammation defined asCRP>5mg/L, faecal calprotectin>250 microgram/g and presence of endoscopicinflammation).

Exclusion

Exclusion Criteria:

  • Patients under 18 or unable to give informed consent.
  • Patients with advanced liver disease.
  • Patients with advanced renal disease with eGFR<45ml/min
  • Previous intolerance to even low doses of oral iron
  • Patients with severe cardiovascular disease defined as previous unstable angina and orprevious MI without intervention.
  • Participation in other trials in the last 3 months.
  • Serious inter-current infection or other clinically important active disease (including renal and hepatic disease) and recently diagnosed gastrointestinal tractcancers
  • Pregnant, post-partum (<3months) or breast feeding females
  • Erythropoietin therapy.
  • Recent blood transfusion within 30 days.
  • Recent iron infusion within 30 days.

Study Design

Total Participants: 30
Treatment Group(s): 3
Primary Treatment: Ferrous fumarate syrup 2.5ml/70mg(45mg elemental iron)
Phase: 3
Study Start date:
October 20, 2023
Estimated Completion Date:
October 01, 2025

Study Description

BACKGROUND:

Anaemia, particularly iron-deficiency anaemia, is a common complication of inflammatory bowel disease (IBD). The prevalence of anaemia (6-74%) and iron deficiency (36-90%) varies widely among reported studies. The predominant cause of iron deficiency in IBD is intestinal blood loss but other factors such as malabsorption and reduced intake may also play a role. Thus, the need for iron supplementation is an often encountered clinical problem in IBD. Although iron is commonly prescribed, the amount of elemental iron needed to achieve clinical efficacy, and the optimal method of supplementation, are under debate. As intravenous (IV) iron supplementation has become safer, calls for increased utilization have appeared. However, there are significant cost implications to using IV iron. On average, a 1-month supply of oral ferrous sulfate costs $12, in comparison with approximately $600-$700 for a treatment cycle of (IV) iron sucrose, excluding the cost of IV administration.

Overall, the comparative studies of IV vs. oral iron do not demonstrate a significant difference in haemoglobin repletion favouring IV iron therapy. Haemoglobin concentrations were similar at the end of treatment in all studies. A single study suggested a superiority for IV iron with a haemoglobin increase greater than 2 g/dl in 47% of the patients on oral iron compared with 66% on IV iron (P = 0.07). However, this could be accounted for by a high withdrawal rate (24%) in the oral iron group. In the largest comparative study, of 196 subjects, median haemoglobin improved similarly, from 8.7 to 12.3 g/dl in the IV group and from 9.1 to 12.1 g/dl in the ferrous sulfate group (P = 0.70). Thus, intravenous iron appears no more effective than oral iron in repletion of iron status as the rate-limiting step appears to be synthesis of red cells, which is not accelerated by IV iron delivery.

The main reason behind the preference of IV iron over oral iron is based on the concern that oral iron may exacerbate IBD. An often-cited study investigating whether oral iron worsens IBD in comparison with IV iron assessed disease activity in 19 IBD patients, 11 with CD and 8 with UC, randomized to either oral ferrous fumarate or IV iron sucrose over a 14-day period. Although the authors argued that disease activity was worsened by oral iron therapy, their use of numerous unconventional assessments weakens this conclusion. The trial was done as a crossover study with a minimum 6-week washout period, so the previous drug therapy may have affected the results. The number of subjects with IBD was small (N = 19). The authors created a synthesized overall disease activity score by combining UC and CD scales and also reported on subscales within activity indexes to identify significant differences. When the two groups were compared, however, there was no statistically significant difference in the overall synthesized disease activity score.

Another factor associated with intolerance of oral iron may be related to the dose of elemental iron administered. In order to maintain iron balance, adult men need to absorb 1-1.5 mg/d, menstruating women need 1-3 mg/d, and pregnant women need approximately 4-5 mg/d. Based on this, the recommended daily allowance of elemental iron is about 8 mg in adult men and postmenopausal women, 18 mg in premenopausal women, and 27 mg in pregnant women. However, most studies investigating the efficacy of oral iron have used a typical dose of 150-200mg/d of elemental iron, 10-20 fold in excess of the recommended daily allowance. Because of the 20% incidence level of intolerance at these conventional doses of elemental iron, recent studies have investigated the efficacy and side effects associated with low-dose oral iron supplementation. A study in the elderly (age >80) randomised 90 patients with iron-deficiency anaemia to 15, 50, or 150 mg of daily oral elemental iron over 2 months. All three dosage groups experienced a similar, statistically significant increase in haemoglobin after 2 months. These studies have not been done in IBD.

This pilot study aims to investigate the efficacy and safety of low dose and standard dose oral iron preparations.

HYPOTHESIS:

Low dose oral iron is effective and safe in the treatment of iron deficiency anaemia in inflammatory bowel disease.

Connect with a study center

  • Liverpool University Foundation NHS Trust

    Liverpool,
    United Kingdom

    Active - Recruiting

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