Hereditary Anemias Clinical Trial
Official title:
Utility of Transient Elastography (Fibroscan) in Estimating Hepatic Iron Concentration in Comparison to MRI in Patients With Transfusion Dependent Hemoglobinopathies
In patients with hereditary anemias (e.g. thalassemias), defective red blood cells are
produced due to an error in the genes, or DNA, that provide the instructions for their
synthesis. As a result, hereditary anemias are characterized by chronically low hemoglobin,
which is contained inside red blood cells and carries oxygen throughout the body. In more
severe cases, patients are dependent on frequent blood transfusions to replenish the
hemoglobin.
The body has limited ability to get rid of excess iron. However, with repeated blood
transfusions, the iron level in the body builds up because the red blood cells contain iron
as heme. Over time, the high level of iron accumulates in organs such as the heart, liver,
and pancreas causing heart problems, liver failure, and diabetes. As a result, patients who
receive multiple blood transfusions need to be monitored for iron overload, and be started
on medical therapy in a timely fashion to prevent organ damage.
Liver is usually the first and the most affected organ by iron accumulation, so knowledge of
its iron concentration provides estimate of total body iron load. Liver biopsy is the gold
standard in measuring the iron concentration in the liver, but it is invasive and cannot be
performed on routine basis. MRI is another option that can assess liver iron concentration
non-invasively, and is currently recommended for monitoring iron load on a yearly basis.
However, MRI has a high cost and is not easily accessible in Canada. The investigators aim
to determine if transient elastography (Fibroscan), which is a form of ultrasound that
measures liver stiffness, can accurately assess liver iron concentration.
Hypothesis:
Fibroscan reading correlates with MRI and serum ferritin in estimating hepatic iron
concentration.
Inclusion criteria: All adult patients (age 19 or greater) with hereditary anemias requiring
chronic blood transfusion at St. Paul's Hospital will be invited to participate in this
study. The majority of patients will be β-Thalassemia Major. They will be given a pamphlet
containing the details of the study and can contact the research assistant or clinic nurse
for more information should they be interested.
Exclusion criteria: Patients with known Hepatitis B positive, known Hepatitis C positive,
known HIV positive, known liver cirrhosis, known primary liver disease such as Wilson's
disease and hereditary hemochromatosis are excluded from the study.
Written consent will be obtained from all participants by the clinic nurse/research
assistant prior to enrollment.
Study procedures:
Data to be collected retrospectively from patient charts (St. Paul's Hospital's EMR/Sunrise
Clinical Manager and paper chart) include: baseline demographic data (age, gender,
hematological condition), medical comorbidities and complications related to iron overload
(Diabetes, hypothyroidism, cardiomyopathy/arrhythmia and congestive heart failure,
hypogonadotropic hypogonadism, osteopenia and osteoporosis syndrome..etc), current
medications including use of iron chelators such as desferrioxamine, deferasirox,
deferiprone or combination therapy, viral hepatitis status (B and C) and date of test, liver
cirrhosis status (stage), liver biopsy result (iron concentration) and date of procedure.
Patients with chronic transfusion requirement usually undergo annual MRI at the beginning of
the year to estimate hepatic iron concentration as per standard practice. This year (2013),
R2 MRI (FerriScan) will also be available for the first time to all patients in BC as part
of routine monitoring for iron overload. Details/results from both techniques (i.e. same
images collected in one scan, but analyzed differently using R2 and T2* algorithms) will be
collected.
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Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Diagnostic
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