Iron Sucrose in Stage 3/4 Kidney Disease

Melbourne Health

Status and phase

Completed

Phase 3

Conditions

Anemia

Kidney Failure

Treatments

Drug: Iron sucrose

Study type

Interventional

Funder types

Other

Identifiers

NCT00202345

Iron Sucrose 61864

Details and patient eligibility

About

One of the complications of late stage kidney disease is the development of a low red blood cell count (anaemia/low haemoglobin concentration). The Australian Commonwealth government limits funding of medications (called erythropoietic stimulating agents) to those patients who have already developed anaemia.

There is evidence supporting the beneficial effects of maintaining a higher haemoglobin in these patients. Higher haemoglobin can delay the onset of dialysis and reduce the development of heart enlargement. However, the administration of erythropoietic stimulating agents is not without risk, including a high financial burden, worsening of high blood pressure and a rare complication called pure red cell aplasia.

Previous studies have shown that patients with chronic kidney disease require additional iron to maintain the production of red blood cells. Thus it would be timely to determine if the administration of iron sucrose to these patients can maintain a near normal haemoglobin concentration, without the need to start an erythropoietic stimulating agent and possibly delaying dialysis.

Study Hypothesis: That administration of iron sucrose is superior to standard care in the prevention of anaemia in patients with stage 3 /4 kidney disease.

Full description

Eligible patients will be approached. Those who agree to partake in the study will, after enrolment (including informed consent), be randomized to one of 2 groups.

Group A: To receive intravenous iron sucrose to maintain supra-physiological measures of iron status ) Group A will be targeted to have ferritin levels between 300 and 500µg/L and/or a transferrin saturation of between 25 and 50%. Between 100 and 200mg of intravenous iron sucrose will be administered by slow bolus injection one- to two-monthly to achieve these levels.

Oral iron will not be used routinely in this group.

Group B: Will have oral iron therapy if required to maintain ferritin levels between 100 and 150µg/L and/or transferrin saturations >20% but <25%. Patients in Group B who are unable to tolerate oral iron will be administered iron sucrose if necessary to maintain acceptable iron levels.

Patients in Group B will therefore differ from those in Group A (a) through the routine use of iron sucrose and (b) through the maintenance of different ferritin and transferrin saturation levels.

Sex

All

Ages

18 to 80 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Initial Hb concentrations ≥ 110g/L (males and females)
Calculated GFR ≤ 35mL/min (≤ 50mL/min for diabetics)
Demonstration of a clinically significant rise in creatinine and/or a drop in Hb concentration in the previous 18 months. If such data are not available, the investigator will make a decision regarding eligibility based on the clinical circumstances.

Exclusion criteria

Age > 80
Pregnancy*
Unstable ischaemic heart disease*
Uncontrolled, severe, congestive cardiac failure
Haemochromatosis or iron overload* (ferritin >300µg/L and TSAT >25%)
Liver failure
Myelodysplastic syndromes or monoclonal gammopathies
Active malignancy or gastrointestinal bleeding*
Persistent sepsis* or significant chronic inflammation (CRP > 25)*
Iron deficiency* (Ferritin <30ug/L and Tsat <15%)or other haematinic disorder
Active and significant haemolysis*
Previous organ transplantation
Concurrent or significant past (>6 months) immuno-suppression
Adult polycystic kidney disease
Current use of an ESA
On dialysis *: patients can still be considered eligible after condition is reversed or treated