Primary Myelofibrosis Clinical Trial
Official title:
Effects of Sympathicomimetic Agonists on the Disease Course and Mutant Allele Burden in Patients With JAK2-mutated Myeloproliferative Neoplasms. A Multicenter Phase II Trial.
The aim of this phase II study is to test a novel concept in the treatment of patients with myeloproliferative neoplasms (MPN), a disease of the bone marrow. With no current cure available, MPN are a group of chronic leukemias (blood cancers) in which patients produce too many blood cells. These increased blood cell numbers cause problems to the patient such as bleedings or thrombosis and some patients may progress to acute leukemia, a life threatening condition. Most MPN patients have a gene mutation called JAK2-V617F. The disease is maintained by mutant MPN stem cells that reside in the bone marrow in specialized locations called "niches". These niches need connections to the nervous system. New findings show that these connections are destroyed by the presence of the mutated MPN stem cells. Research teams found that some drugs (beta3-sympathicomimetics) can restore these damaged niches and at the same time reduce the MPN disease manifestation in a mouse model of MPN. Such sympathicomimetic drugs are already being used to treat patients with asthma or hyperactive bladder. These drugs have shown to have only few side effects. The study tests the effects of the beta-3-sympathicomimetic drug Mirabegron (Betmiga®) on MPN disease in 39 patients that carry a JAK2-V617F mutation. The hypothesis is that Mirabegron will have a beneficial effect on bone marrow niche cells and will thereby improve the disease manifestation in MPN patients. This study should provide a rapid answer whether targeting the nervous system of the niche cells could be useful for patients with MPN and warrants to be tested in larger and more long-term studies.
DISEASE BACKGROUND
Myeloproliferative neoplasms (MPN) are clonal stem cell disorders characterized by aberrant
proliferation of the erythroid, megakaryocytic and myeloid lineages. They are associated with
decreased survival, thromboembolic complications, hemorrhage and an inherent tendency towards
leukemic transformation. About 4-6 of 100'000 residents per year are diagnosed with MPN
Currently, MPN are subdivided into three disease entities: polycythemia vera (PV), essential
thrombocythemia (ET) and primary myelofibrosis (PMF). Three genes are frequently mutated in
MPN and are implicated to be the phenotypic driver mutations: more than 95% of PV patients
carry a somatic JAK2-V617F mutation, while about half of the remaining PV patients (2-3%)
display mutations in JAK2 exon 12. Thus, almost all patients with PV have somatic mutations
in the JAK2 gene. The mutational profiles of ET and PMF are more diverse: JAK2-V617F is found
in 50-60% of the patients, whereas the recently described mutations in calreticulin (CALR)
occur in 20-25% of the patients. Between 5-8% of the remaining ET and PMF patients carry
mutations in the thrombopoietin receptor (MPL) and in 10-15% of the patient the mutation
remains to be determined. Quantitative tests are now available to follow the mutant allele
burden of each of the JAK2, CALR and MPL mutant alleles.
THERAPY BACKGROUND
No curative treatment exists for MPN, possibly with the exception of allogeneic hematopoietic
stem cell transplantation (HSCT), which is applicable only in a minority of patients.
Currently, treatments for MPN are not very effective, or extremely costly. Hydroxyurea has
been the standard of care for many decades. A reduction in thrombotic complications can be
demonstrated in "high risk" MPN patients (age >60, presence of a previous thrombotic event),
but hydroxyurea has no effect on the course of disease (no remission or substantial reduction
of the mutant allele burden). Interferon alpha (IFNα) is a promising treatment for early
stage PV and is currently being tested in phase III studies. However, IFNα is not always well
tolerated and in phase II studies only a proportion of patients showed a substantial
response. Ruxolitinib, recently approved for PMF with splenomegaly, is effective in reducing
spleen size and improving quality of life, but has little effect on the JAK2-V617F mutant
allele burden and has so far not been reported to induce remissions. Allogeneic HSCT is
reserved for patients with PMF with a poor prognostic score. These including the recently
developed JAK2 inhibitors reduce the symptoms of the disease, but, with the exception of
pegylated interferon alpha (peg-IFNα), have little effect on the size of the neoplastic clone
and are unable to induce molecular remissions. Thus, the percentage of mutant allele burden
in hematopoietic cells does not change much even with successful treatment when considering
symptom reduction. It is generally expected that reduction in the size of the malignant
clone, as a surrogate marker of treatment success, will have the potential to reduce
morbidity and result in prolonged survival of patients.
NOVEL TREATMENT
The beta-3-sympathicomimetic drug Mirabegron is currently available as Betmiga® and indicated
to treat hyperactive bladder. It is available as a slow release tablet in a 25 mg and 50 mg
formulation. Sympathicomimetic drugs are known to relax the smooth muscle in several areas of
the human body and are therefore used for inhalation in patients with asthma or as described
for this drug to relax the smooth muscle of the bladder to treat urge incontinence.
β3-Adrenoceptors mediate a negative inotropic effect in human ventricular cardiomyocytes,
which is opposite to that of β1- and β2-adrenergic receptors. Unlike beta1/2-mimetics, that
have significant cardiovascular side effects (including hypertrophy), beta3-mimetics have
been reported to protect from hypertrophy and are only associated with some risk of
tachycardia and palpitations in some patients.
Sympathicomimetic agonists in patients with JAK2-mutated MPN
RATIONALE FOR PERFORMING THE TRIAL
MPN is initiated and maintained from a mutated hematopoietic stem cell (HSC). The interplay
between the MPN HSCs and the stem cell niche is increasingly recognized as crucial for the
biology of the disease. Dr. Simon Méndez-Ferrer et al, previously demonstrated that
nestin-positive mesenchymal stem cells (nestin+ MSCs) within the bone marrow niche are
innervated by sympathetic nerve fibers and are important in regulating normal HSCs. New
findings by Dr. Méndez-Ferrer's laboratory show that these nestin+ MSCs are strongly reduced
in bone marrow from patients with MPN.
Furthermore, in a mouse model of MPN expressing the human JAK2-V617F mutation, this effect
was found to be caused by early glial and sympathetic nerve damage and apoptosis of nestin+
MSCs triggered by the mutant HSCs. In vivo depletion of nestin+ cells accelerated MPN
progression. Conversely, MPN phenotype could be reversed by compensating for the sympathetic
neuropathy by the treatment with a beta-3-sympathicomimetic drug. Mice with JAK2-V617F driven
MPN treated with a beta-3-sympathicomimetic agonist not only restored nestin+ MSCs numbers,
but also showed correction of thrombocytosis, neutrophilia, and bone marrow fibrosis, and
efficiently reduced mutant hematopoietic progenitor numbers in bone marrow and peripheral
blood. Thus, treatments with a beta-3 sympathicomimetic agonist corrected the damage
inflicted by the MPN clone on the stem cell niche and led to a dramatic improvement of the
MPN phenotype. Therefore, beta-3 sympathicomimetic agonists represent a promising novel
therapeutic approach to MPN by targeting the stem cell niche rather than the MPN clone
itself.
Considering the widely used and established safety track record of beta-3-sympathicomimetic
drugs, a phase II study has been selected to test the concept of a beneficial effect of beta
sympathicomimetic activity on bone marrow niche cells and through this effect on the disease
manifestation in MPN patients.
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