Scleroderma Clinical Trial
Official title:
A Proof of Concept Trial of Gleevec (Imatinib) in Active Diffuse Scleroderma
The purpose of this study is to investigate the effectiveness and safety of the drug Gleevec
(imatinib) as a new treatment for patients with active diffuse scleroderma. This drug has
not been used previously to treat scleroderma, but it has been found to advance the
treatment and life span of patients with a type of leukemia called chronic myeloid leukemia
or CML. Gleevec acts on chemical signals in the cells that may decrease fibrosis (the
hardening of the skin that occurs in scleroderma). It works by interfering in the process
that activates many molecules that cause fibrosis, including TGFbeta (which may be a key
part of disease activity in scleroderma).
This study proposes to treat patients that have significant diffuse scleroderma with Gleevec
for 6 months and investigate several measures of scleroderma disease activity before, during
and at the end of treatment (0, 3 months and 6 months). This is a randomized, double blind,
placebo-controlled trial: 20 patients will be divided into two groups in a 4:1 ratio, with
16 patients taking 400mg of Gleevec per day and 4 taking a placebo. The differences between
the groups that will be measured include safety, Modified Rodnan skin score (mRSS), Health
Assessment Questionnaire (HAQ), global assessments (100mm VAS) and changes in biomarkers in
blood and skin biopsies.
Purpose:
Scleroderma is a connective tissue disease that is prototypical for fibrosis with
autoantibodies and vascular abnormalities including vasomotor instability (Raynaud's) at one
end and blood vessel obliteration at the other (1,2). Scleroderma occurs in > 2/10,000 (with
thousands of Canadians affected) and has no proven therapy to modify the disease overall
(3). The purpose of this study is to investigate the potential of Gleevec to be used as a
novel therapy in the treatment of scleroderma.
Background:
There are two subtypes of systemic scleroderma: diffuse and limited (2). Limited skin
involvement includes skin involvement distal to the elbows and knees and may include the
neck and face, but spares the trunk and proximal extremities. Diffuse scleroderma has more
extensive skin involvement including trunk or proximal extremities and is associated with
more internal organ involvement and increased mortality (4). For instance, significant
interstitial lung disease, cardiomyopathy and scleroderma renal crisis are more common in
diffuse scleroderma than limited. The extent of organ involvement in these areas may
correlate with the extent of skin involvement and worsening skin involvement is associated
with increased mortality and worse overall health function as measured by the Health
Assessment Questionnaire (HAQ) (5).
Formulation of Objective:
Various signals that could be therapeutically down regulated in scleroderma such as PDGF,
VEGF, endothelin, and TGFβ are potential therapeutic targets. The inhibition of tyrosine
kinase can decrease cell growth and could be a key signal modifier in scleroderma (6).
Signal transduction modification with selected targets has been very successful in the
treatment of some cancers, such as using Gleevec in chronic myelocytic leukemia (7).
Gleevec (imatinib) is an oral tyrosine kinase inhibitor. It is used in the treatment of CML
and some GI stromal tumors, with a reduction in mortality in CML. Tyrosine kinase activates
PDGF and TGFbeta, which are key signals in scleroderma so a proof of concept study is needed
to determine if there is a biological signal to proceed in a disease of fibrosis such as
scleroderma. PDGF regulation is important in fibrotic diseases by stimulating replication
and migration of myofibroblasts (8).
Protocol:
Subjects with active diffuse scleroderma will be enrolled after consenting and will receive
Gleevec 400mg/od or placebo. Serum and skin biopsies will be collected for biomarkers. Serum
samples will be taken at baseline, 3 and 6 months and analyzed by ELISA/multiplexing for
changes in profibrotic cytokines including PDGF, VEGF, endothelin, and TGFβ. Skin biopsies
will be taken prior to the first dose and at 6 months. Modified Rodnan Skin Score (MRSS),
Health Assessment Questionnaire (HAQ), MD and patient global assessments will also be done
at times 0, 3, and 6 months. SF36 and Health Transition Score will be done at 0 and 6
months. Biochemistry for safety and inflammation will be done once a month for the duration
of the trial.
Gleevec at 400 mg/od or placebo will be given orally with food and a large glass of water
for 6 months. As this is a proof of concept and Phase IIa trial they will be randomized into
active vs. placebo groups in a 4:1 ratio, where n=20. Therefore, 16 patients will receive
active drug and 4 will receive placebo.
Specific Aims:
1. Primary outcome measurement: changes in cytokine expression in skin biopsies and serum
samples for profibrotic cytokines.
2. To determine the between groups differences from baseline to final skin score on
Gleevec and placebo at 6 months using the Modified Rodnan Skin Score (MRSS).
3. To compare the AEs (adverse events) and SAEs (serious adverse events) between the
groups.
4. Secondary objectives will be:
Comparing secondary outcome measurements such as: MD global, patient global, HAQ, SF36,
Health Transition, ESR, CRP.
Randomization and Blinding:
The randomization will be stratified by current use of methotrexate. It is anticipated that
the majority of patients in this trial will not be taking methotrexate at time of
randomization, but stratification should balance the groups if there is a heterogenous
response. The randomization will be done in balanced blocks of 5, after stratification by
methotrexate use. The pharmacy will be called and will provide the medication and will have
the randomization code. The trial is blinded where the patient, the research nurse
performing study procedures including dispensing the study drug, and the physician doing the
outcome assessments will all be unaware of treatment allocation.
Concomitant Medications:
Stable dose concomitant methotrexate of up to 25 mg/week if tolerated (po or sc) can be
continued throughout the study. In addition, if necessary, folate can be added or increased
to decrease side effects.
All standard of care is allowed except for the medications listed above. Thus treatment for
GERD, Raynaud's, digital ulcers, HTN, delayed GI emptying, small bowel overgrowth, Sjogren's
symptoms, arthritis (using NSAIDs or low dose prednisone) is allowed. Severe PAH and severe
ILD is excluded as there could be expectations that this comorbidity may interfere with the
current 24-week treatment protocol. Steroids can be increased in the rare chance that a
patient develops a complication or co-morbidity that requires higher doses of steroids as
part of standard care. Regular need for antibiotics for small bowel overgrowth is allowed.
Good clinical practice will be followed and other appropriate treatment will not be denied.
This is an 'add-on' treatment to standard care. Concomitant medications will be assumed to
be held stable throughout the study. Patients taking any medications that may interact with
Gleevec (eg. SSRIs, TCA, trazadone, benzodiazepines, betablockers, etc.) will be monitored
cautiously.
Since Gleevec has been postulated (by a case report) to improve pulmonary arterial
hypertension (PAH) annual echocardiograms that are done as part of standard care may be
compared between the groups determining the estimated PAP on echocardiogram (9).
AEs and SAEs:
The University of Western Ontario Ethics Committee will approve the protocol and any
amendments and will be informed of any SAEs as per usual research conduct. The patients are
free to withdraw consent or drop out at any time with no adverse effect on their future
care. As per any trial, AEs and SAEs will be collected. SAEs will be reported in an
expedited way to the UWO Ethics Committee and Novartis.
Pregnancies:
Pregnancy or fathering of a child, although not itself a serious adverse event, should also
be reported on a serious adverse event form or pregnancy form and be followed up to
determine outcome, including spontaneous or voluntary termination, details of birth, and the
presence or absence of any birth defects or congenital abnormalities. In addition to any
pregnancy or fathering of a child within 84 days (12 weeks or 3 months) after the last
Gleevec intake has to be reported and recorded as an SAE.
Any pregnancy that occurs during study participation should be reported using a Clinical
Trial Pregnancy Form. To ensure patient safety each pregnancy must also be reported to
Novartis within 24 hours of learning of its occurrence. The pregnancy should be followed up
to determine outcome, including spontaneous or voluntary termination, details of birth, and
the presence or absence of any birth defects or congenital abnormalities or maternal and
newborn complications.
Patients will be informed of the risks involved in becoming pregnant while taking Gleevec in
the Letter of Information and female partners of male study participants will be required to
read and sign a "Pregnant Partner Data Release Form" acknowledging that they have been
informed of these risks as well.
Discontinuation of Treatment:
The patients are free to drop out at any time. A severe allergic reaction will necessitate
withdrawal. If there are sustained cytopenias (WBC <2.0, Hbg < 8.0 or Plt < 50,000) for 2
infusions in a row then the patient will be withdrawn. If there is a WBC < 1.0 or Hbg < 7.5
or Plt < 10,000 at any time, the patient will be withdrawn. If there are sustained
elevations of AST/ALT twice in a row, of twice the upper limit of normal, then the
methotrexate will be decreased by 5 mg/week. If the elevation persists for 2 more tests, the
methotrexate will be held for two weeks and the liver enzymes repeated. If still elevated,
the methotrexate will be cut in half and if still elevated and no other concomitant meds are
thought to be causing the elevation, then the patient will be withdrawn.
Sample Size:
This study is a pilot and is not anticipated to have enough power to have a statistically
significant between groups difference on skin score. However, the effects on fibrosis and
other mediators in serum and tissue specimens may help to determine if a larger trial should
be a 'go' or 'no go'.
Analysis:
This will be a modified intent to treat analysis, where any patient receiving at least one
dose of the study drug will be analyzed, and for dropouts the last observation will be
carried forward (LOCF). The primary outcome measurement will be changes in profibrotic
cytokine expression in serum and urine samples and skin biopsies. Multiplexing will be used
to measure up to 30 analytes of interest in one 50ul sample of any biological fluid.
Statistics will include the between groups (active and placebo) difference at 24 weeks (6
months) in the MRSS. There will be a between groups assessment of HAQ, ESR and CRP for
placebo compared to Gleevec. The SF36 and Health Transition Scores will be compared using
paired tests. AEs and SAEs will be quantified and compared between placebo and active
treatment. PK and PD data will only be analyzed if there is a thought of continuing drug
development in this area. If the data appear to demonstrate some benefit, then a repeated
measures ANOVA will be done to determine if there are between groups differences at various
time points.
Data Safety Monitoring Board:
All SAEs will be reported to the Ethics Committee and to Novartis. An independent safety
board blinded to treatment allocation will meet at 3 months to monitor study progress and
SAEs. There will be no interim analysis, as the study is not powered to do one. Safety
events will be collected up until one month after discontinuing study drug in all cases
wherever possible.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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