Mi-iron - Moderately Increased Iron - is Reducing Iron Overload Necessary?
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Purpose
Haemochromatosis is a preventable genetic iron overload disorder. Untreated, it can shorten life due mainly to liver cirrhosis and cancer. It can be prevented by blood donation to maintain normal iron levels. It is unclear, however, whether treatment is necessary when individuals have moderate elevation of iron in the body. This research project will study the effects of treatment in this group by assessing a number of scans, questionnaires and blood tests in treated and untreated individuals.
| Condition | Intervention |
|---|---|
|
Hereditary Haemochromatosis |
Procedure: Erythrocytapheresis Procedure: Plasmapheresis |
| Study Type: | Interventional |
| Study Design: | Allocation: Randomized Intervention Model: Single Group Assignment Masking: Single Blind (Subject) Primary Purpose: Treatment |
| Official Title: | Mi-Iron - Moderately Increased Iron - is Reducing Iron Overload Necessary? |
- Fatigue [ Time Frame: Clinically and statistically significant change in measures taken at baseline and at the end of treatment will be compared. Patients will have approximately 6 third weekly treatments however this will vary depending on initial SF. ] [ Designated as safety issue: No ]Modified Fatigue Impact Scale (MFIS). The MFIS is a shortened version of the Fatigue Impact Scale. This 21-item scale can be self completed and measures the impact of fatigue on physical, cognitive and psychosocial functioning. Each item is scored from 0 (never) to 4 (almost always) resulting in a score from 0-84. In addition, physical (0-36), cognitive (0-40) and psychosocial (0-8) subscale scores can be derived.
- Change in markers of liver fibrosis [ Time Frame: Clinically and statistically significant change in measures taken at baseline and at the end of treatment will be compared. Patients will have on average 6 third weekly treatments (15 weeks). ] [ Designated as safety issue: Yes ]Liver fibrosis will be assessed using Hepascore and Fibrometer (blood tests) and transient elastography (ultrasound).
- Quality of life [ Time Frame: Clinically and statistically significant change in measures taken at baseline and at the end of treatment will be compared. Patients will have on average 6 third weekly treatments (15 weeks). ] [ Designated as safety issue: No ]Medical Outcomes Study 36-item short form (SF36). As there are no specific quality of life tools available for HH, we will use this very widely used generic tool that has been used in a number of HH studies. This tool covers eight dimensions of health and wellbeing. One study found that individuals seen in a HH clinic and who had no clinical symptoms had significantly lower scores on a number of dimensions of the SF36 compared to population norms.
- Depression and Anxiety [ Time Frame: Clinically and statistically significant change in measures taken at baseline and at the end of treatment will be compared. Patients will have on average 6 third weekly treatments (15 weeks). ] [ Designated as safety issue: No ]The Hospital Anxiety and Depression Scale (HADS) is a brief self-report measure designed to screen for anxiety symptoms and depression symptoms in a hospital setting. It is composed of two seven-item subscales, the Anxiety (HADS-A) and Depression (HADS-D) subscales, and a 14-item total scale (HADS-T). Participants use a four-point Likert-type scale to rate how they have felt in the past week. It has been found to be valid and reliable in various populations.
- Arthritis [ Time Frame: Clinically and statistically significant change in measures taken at baseline and at the end of treatment will be compared. Patients will have on average 6 third weekly treatments (15 weeks). ] [ Designated as safety issue: No ]The presence and impact of arthritis will be measured by the Arthritis Impact Measurement Scales 2 short form. This is a 24 item validated scale that assesses the impact of arthritis on the individual over the past four weeks. We will also ascertain the use of arthritis medication at baseline and end of erythrocytapheresis/sham erythrocytapheresis.
- Markers of oxidative stress [ Time Frame: Clinically and statistically significant change in measures taken at baseline and at the end of treatment will be compared. Patients will have on average 6 third weekly treatments (15 weeks). ] [ Designated as safety issue: Yes ]To assess oxidative stress, we will measure F2-isoprostanes, a validated marker of cellular lipid oxidative damage, in urine and blood.
| Estimated Enrollment: | 110 |
| Study Start Date: | June 2012 |
| Estimated Study Completion Date: | March 2015 |
| Estimated Primary Completion Date: | December 2014 (Final data collection date for primary outcome measure) |
| Arms | Assigned Interventions |
|---|---|
|
Active Comparator: Erythrocytapheresis
Erythrocytapheresis is a procedure whereby whole blood is drawn from an individual and all elements except erythrocytes are returned to the donor. An automated filtration process removes the erythrocytes. Those in arm 1 will have third weekly erythrocytapheresis until their SF is returned to the normal range. |
Procedure: Erythrocytapheresis
To achieve a blinded randomised trial, apheresis treatment will be used. Those in arm 1 will have erythrocytapheresis reducing iron levels and those in arm 2 will have plasmapheresis and their iron levels will not be reduced. An apheresis machine will be used to remove red blood cells only from the erythrocytapheresis group. Subjects will have third weekly treatments until SF levels are reduced to ~100 ug/L in accordance with current guidelines. Other Name: red blood cell removal, red blood cell apheresis
|
|
Sham Comparator: Plasmapheresis
In plasmapheresis, the plasma is removed by the automated filtration process whilst other blood elements including erythrocytes are returned to the subject. Those in arm 2 will have plasmapheresis with the approximate number of episodes of apheresis that would be required to reduce their SF to normal had they been randomised to the true treatment arm. |
Procedure: Plasmapheresis
An apheresis machine will be used to remove blood plasma only from the plasmapheresis group. Those in arm 2 will have the approximate number of episodes of apheresis that would be required to reduce their SF to normal had they been randomised to the true treatment arm. Those in the sham arm will be offered to have venesection at their choice of venue or to have their SF normalised by erythrocytapheresis after the initial blinded part of the study. This will be done because it will not be known for some time if there is benefit from normalisation of SF and therefore leaving people with elevated SF that may be harmful.
Other Name: plasma removal, sham erythrocytapheresis
|
Detailed Description:
There is mounting evidence that treatment of moderate iron overload in HFE related hereditary haemochromatosis (HH) is not necessary. This project aims to undertake a randomised patient-blinded trial of erythrocytapheresis compared to sham erythrocytapheresis (using plasmapheresis) in individuals who have serum ferritin (SF) above the upper limit of the normal range but < 1000ug/L (defined here as moderate iron overload) due to HFE mutations and to compare the prevalence of symptoms and objective markers of disease in the two treatment arms.
Eligibility| Ages Eligible for Study: | 18 Years to 70 Years |
| Genders Eligible for Study: | Both |
| Accepts Healthy Volunteers: | Yes |
Inclusion Criteria:
- HFE C282Y homozygous.
- Aged 18 - 70 years .
- SF above the upper limit of the normal range of 300µg/L but less than 1000µg/L with a currently or previously raised TS (> 50% for males and > 45% for females).
Exclusion Criteria:
- HH due to genotypes other than HFE C282Y homozygosity.
- Normal SF, SF > 1000µg/L.
- Other major risk factor(s) for liver toxicity or other significant co-morbidities including positivity for hepatitis B or C, excess alcohol consumption (> 30g/day in males and 20g/day in females) or body mass index > 35.
- Has had venesection therapy for HH in the last two years.
Contacts and Locations| Contact: Martin B Delatycki | +61 3 9496 4355 | martin.delatycki@ghsv.org.au |
| Australia, Queensland | |
| Royal Brisbane and Woman's Hospital | Not yet recruiting |
| Brisbane, Queensland, Australia, 4072 | |
| Contact: Lawrie Powell, Prof | |
| Principal Investigator: Lawrie Powell, Prof | |
| Australia, Victoria | |
| Austin Health | Recruiting |
| Melbourne, Victoria, Australia, 3081 | |
| Contact: Martin B Delatycki, Prof +61 3 9496 4355 martin.delatycki@ghsv.org.au | |
| Principal Investigator: Martin B Delatycki, Prof | |
| Royal Melbourne Hospital | Not yet recruiting |
| Melbourne, Victoria, Australia | |
| Contact: Amanda Nicoll, A/Prof | |
| Principal Investigator: Amanda Nicoll, A / Prof | |
| Australia, Western Australia | |
| Fremantle Hospital and Health Service | Not yet recruiting |
| Perth, Western Australia, Australia, 6009 | |
| Contact: John Olynyk | |
| Principal Investigator: John Olynyk, Prof | |
| Principal Investigator: | Martin B Delatycki | Austin Health/Murdoch Childrens Research Institute |
More Information
Additional Information:
No publications provided
| Responsible Party: | Martin Delatycki, Professor, Murdoch Childrens Research Institute |
| ClinicalTrials.gov Identifier: | NCT01631708 History of Changes |
| Other Study ID Numbers: | 04609 |
| Study First Received: | June 24, 2012 |
| Last Updated: | June 27, 2012 |
| Health Authority: | Australia: Human Research Ethics Committee |
Keywords provided by Murdoch Childrens Research Institute:
|
Hereditary haemochromatosis Moderate iron overload Serum ferritin Treatment |
Additional relevant MeSH terms:
|
Hemochromatosis Iron Overload Metal Metabolism, Inborn Errors Metabolism, Inborn Errors Genetic Diseases, Inborn Iron Metabolism Disorders Metabolic Diseases |
Iron Trace Elements Micronutrients Growth Substances Physiological Effects of Drugs Pharmacologic Actions |
ClinicalTrials.gov processed this record on May 21, 2013