Efficacy and Safety Study of Magnesium Iron Hydroxycarbonate for the Reduction of High Blood Phosphate in Hemodialysis Patients

Phase 2

Completed

Conditions: Chronic Kidney Failure

Interventions: Drug: Fermagate
Drug: Placebo

Registration Number: NCT00317694

Lead Sponsor: Ineos Healthcare Limited

Brief Summary: Magnesium iron hydroxycarbonate is a phosphate binder that absorbs phosphate from food, reducing the amount that the body can absorb.

The purpose of this study it to look at how effective and safe Magnesium iron hydroxycarbonate is in controlling levels of phosphate in the blood in patients who receive hemodialysis.

Detailed Description: High levels of phosphate in the blood are linked with serious effects, due to calcium imbalances (high levels of parathyroid hormone (PTH), bone disease, formation of calcium deposits in the body, and blood-vessel disease).

Current guidelines indicate that blood phosphorus levels should be maintained between 1.13 to 1.78 mmol/L in patients who receive hemodialysis.

This study is designed to investigate magnesium iron hydroxycarbonate's ability to lower and control patients' blood phosphate to the recommended levels and compare the average blood phosphate, calcium, calcium-phosphate product, PTH and magnesium concentrations and overall safety with placebo (or "dummy") tablets.

Recruitment & Eligibility

Status: COMPLETED

Sex: All

Target Recruitment: 111

Inclusion Criteria

Male or female subjects on active haemodialysis, aged 18 years or over.
Written informed consent given.
On a stable haemodialysis regimen (three times per week) for at least 3 months and be unlikely to change their dialysis prescription during the study period.
On a stable dose of a phosphate binder for at least 1 month prior to screening.
Willing to abstain from taking any phosphate binder or oral magnesium, aluminum or iron-containing products and preparations, other than the study medication.
Willing to avoid any intentional changes in diet such as fasting, dieting or overeating.
Willing to maintain their usual type and dose of Vitamin D supplementation.

Exclusion Criteria

Participation in any other clinical trial using an investigational product or device within the previous 4 months.
A significant history of alcohol, drug or solvent abuse in the opinion of the investigator.
Any disease or condition, physical or psychological, which in the opinion of the investigator would compromise the safety of the subject or increase the likelihood of the subject being withdrawn.
Clinically significant laboratory findings (for this subject population) in the opinion of the investigator.
Any malignancy requiring treatment within 5 years of screening with the exception of basal cell carcinoma and Bowen's disease.
A history of a motility disorder of the intestines, including, but not limited to, gastroparesis, ileus, pseudo-obstruction, megacolon, or mechanical obstruction.
A significant illness in the 4 weeks before screening.
Taking medication prescribed for seizures.
A history of haemochromatosis.
A history of high serum ferritin concentration of ≥ 1000ng/ml (excluding transient, treatment-induced ferritin elevation).
A history of dysphagia or swallowing disorders that might limit the subject's ability to swallow study medication in the opinion of the investigator.
Female subjects who are lactating or pregnant. Women of childbearing potential (pre-menopausal and not surgically sterilized) unless they are using a reliable contraceptive method, that is, barrier methods, hormones or intrauterine device.
Current haemoglobin concentration of < 10.00 g/dL.
Allergy to the IMP or its constituents.

Study & Design

Study Type: INTERVENTIONAL

Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
1	Fermagate	-
2	Placebo	-

Primary Outcome Measures

Name	Time	Method
Proportion of subjects who achieve controlled serum phosphate concentrations during the double-blind comparative phase	Mean of last two serum phosphate values in the double blind phase

Secondary Outcome Measures

Name	Time	Method
Change from baseline in mean serum phosphate concentration	Mean of last two serum phosphate values
Change from baseline in serum calcium	Specified visits throughout the study period
Change from baseline calcium-phosphate product	Specified visits throughout the study period
Change from baseline PTH	Specified visits throughout the study period
Change from baseline magnesium	Specified visits throughout the study period
Assessment of adverse events	Throughout the study period
Assessment of routine safety laboratory parameters	Specified visits throughout the study period
Assessment of physical examination	At screen and follow-up
Assessment of 12-lead electrocardiogram	At screen and follow-up
Assessment of bowel habits	Specified visits throughout the study period

Trial Locations

Locations (15): Nottingham Renal and Transplant Unit, Nottingham City Hospital
🇬🇧
Nottingham, United Kingdom
Richard Bright Renal Unit, Southmead Hospital
🇬🇧
Bristol, United Kingdom
Dialysis Unit, Broad Green Hospital
🇬🇧
Liverpool, United Kingdom
1614 West 42nd Street
🇺🇸
Pine Bluff, Arkansas, United States
Southeast Renal Associates
🇺🇸
Charlotte, North Carolina, United States
US Renal Care
🇺🇸
Stuttgart, Arkansas, United States
Renal Unit, Birmingham Heartlands Hospital
🇬🇧
Birmingham, United Kingdom
Davita Dialysis Center
🇺🇸
Charlotte, North Carolina, United States
Addenbrookes Dialysis Centre, Addenbrookes Hospital
🇬🇧
Cambridge, United Kingdom
Sheffield Kidney Unit, Northern General Hospital
🇬🇧
Sheffield, United Kingdom
Dept. of Nephrology, Morriston Hospital
🇬🇧
Swansea, United Kingdom
General Medicine and Nephrology, Norfolk and Norwich University Hospital
🇬🇧
Norwich, United Kingdom
St Lukes Hospital
🇬🇧
Bradford, United Kingdom
Renal Unit, Leicester General Hospital
🇬🇧
Leicester, United Kingdom
Royal Liverpool University Hospital
🇬🇧
Liverpool, United Kingdom