Hematological Diseases Clinical Trial
Official title:
Pilot Study of Non-Invasive Assessment of Hepatic And Myocardial Iron Through T2* MRI In Patients With Iron Overload
Many hematological disorders are treated by giving red blood cells. Over a long period of
time iron from the red blood cell will accumulate in the tissues of the heart, liver, and
endocrine glands. This condition is referred to as iron overload and may become life
threatening due to the effects of the iron on these tissues. The normal method for
evaluation of iron overload is a liver biopsy. This procedure is invasive and has potential
risks, such as bleeding and infection.
It is very desirable to establish a method for assessing iron overload which is not
invasive. New magnet resonance imaging (MRI) relaxation techniques (T2*MRI) can be used to
indirectly assess the liver iron content and iron in the heart. Results of T2*MRIs show
excellent correlation with liver iron content and heart function. The use of this method of
assessment will minimize the risk and inconvenience of liver biopsy and possibly allow more
frequent evaluations for iron overload, thus better treatment for these patients.
Participants in this study will undergo both liver biopsy for liver iron content and T2* MRI
of the liver and the heart. Results from the procedures performed in this study will be
compared, with the end result being the possible elimination of invasive procedures to
diagnose iron overload.
Quantitative measurements of hepatic and cardiac iron by single-breath-hold MRI T2* will
allow us to determine the value of this technique as a non-invasive method of monitoring
liver and cardiac iron content. By obtaining T2 measurements, we will be able to compare two
different techniques for non-invasive iron assessment. With regard to the liver, we will
correlate T2* measurements with the gold standard, LIC on liver biopsy. Because it is not
feasible to perform cardiac biopsies to evaluate the degree of cardiac hemosiderosis, we
will evaluate the relationships between cardiac T2* values and left and right diastolic
function, left ventricular ejection fraction, left ventricular end-systolic volume and left
ventricular mass index obtained by echocardiography and MUGA scans that are performed as
part of the routine clinical care of these patients. In order to estimate whether cardiac
T2* values are clinically relevant, we will also investigate the relationship between T2*
values and the need for cardiac medication due to cardiac hemosiderosis. Cardiac and hepatic
T2* measurements will also be compared to their visual appearances on T2* MR images in order
to investigate the relationship between these two assessments. Cardiac and hepatic T2* and
their respective visual appearances on T2* MR images will be compared with serum ferritin to
evaluate the potential relationships among these measurements of iron overload.
Amen T2* and T2 phantoms are devices that allow calibration of the MR measurements for
absolute iron content. Phantoms are test tubes filled with aqueous solutions or gel
compounds of materials that mimic various tissue relaxation times (T1, T2 and T2*). Phantoms
are commonly used in MRI when quantification is desired. Our phantom will consist of a
multitude of small vials which will be visible in the imaging plane. The relaxation times
vary in the different vials of the phantom and are known very accurately, especially the T2
and T2* values, which vary over the physiological relevant range. This way the phantom can
be used to calibrate the T2* values obtained from the patients heart and liver and
eventually be correlated to absolute iron concentrations.
If accurate, the T2* MRI technique would ultimately allow a non-invasive method of
quantitatively assessing myocardial and liver iron accumulation, and could predict the
degree of morbidity due to iron overload. This new technique could greatly improve the care
of our iron overloaded patients by offering a practical and risk free method for evaluation
of body iron load. We plan to apply this preliminary information into future studies in this
area. Eventually we plan to use the T2* MRI measurements in longitudinal studies of patients
with iron overload, both to assess their degree of iron burden and monitor chelation therapy
treatments.
Amen Dark blood applications are state-of-the-art in cardiac MRI and commonly applied. There
is no risk associated with the dark blood preparation. Comparison of dark and bright blood
measurements will show whether both sequences yield similar results and whether one
technique is less susceptible to cardiac motion and associated artifacts, thereby offering a
higher accuracy and a smaller error in the calculation of T2* and iron concentration.
Information about the heart function can be obtained using MRI techniques, however this
information needs to be validated in different populations, such as patients with iron
overload. If MR data show a high correlation with echocardiography and MUGA functional data,
subsequent protocols could be conducted where the functional information can be gained with
an MR measurement, thereby avoid acquiring a MUGA scan and eliminating the exposure to
radiation as well as streamlining the protocol by just adding a few additional measurements
to an already scheduled MR iron scan. Performing cardiac measurement in a few patients using
the MRI technique will allow us to expand the use of this technique for future and larger
studies.
Pulmonary hypertension causes progressive right ventricular dysfunction and severe
respiratory symptoms (e.g., dyspnea, hypoxemia, poor exercise tolerance, etc.). The
association of myocardium iron deposition and its relationship with pulmonary hypertension
has not been investigated. Pulmonary hypertension is a prevalent complication among patients
with hematologic diseases, especially those with a hemolytic component to the anemia.
Because many of these patients are treated with blood transfusion and consequently develop
iron accumulation in the heart, the investigation of the association of myocardial
hemosiderosis and pulmonary hypertension is warranted.
Finally, because little is understood about iron loading and unloading at the cellular and
molecular level, we propose to perform tissue microarray analysis on liver biopsy samples
obtained from children with iron overload. This powerful tool will help identify over- and
under-expressed genes in the clinical scenario of iron loading, and later in the setting of
iron mobilization in these overloaded patients. This pilot study will allow us to
investigate differences in gene expression from patients with mild, moderate and severe iron
overload, as determined by quantitative LIC on liver biopsy. Our approach will allow
characterization of gene expression and analysis for patterns that reflect cellular
responses to different degrees of iron overload. This study will not obtain "normal liver"
controls from our population, since sickle cell patients without transfusional iron overload
have no clinical indication for liver biopsy. It is hoped, however, that subsequent
therapeutic protocols will also include microarray studies on liver biopsy samples. In this
way, the current microarray analysis will serve as a "baseline" and patients will serve as
their own controls for differences in gene expression. This will particularly be important
for those patients undergoing successful chelation therapy that should lower LIC. Overall,
an understanding of the genetic and biochemical events that regulate these iron loading and
unloading processes could greatly improve our ability to treat patients appropriately.
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