Myelodysplastic Syndrome Clinical Trial
Official title:
A Phase 2, Open-Label, Multiple-Dose Study Investigating the Efficacy and Safety of Panhematin in Patients With Low or Intermediate-1 Risk Myelodysplastic Syndrome
This is a Phase II, open-label clinical trial examining the role of Panhematin® in patients
with MDS. The objective of this study is to evaluate the safety and efficacy of Panhematin®
(hematin for injection) in the treatment of adult patients (≥ 18 years of age) with low-risk
MDS.
The study will be conducted on an outpatient basis and will consist of the following:
- A Screening Period (within 28 days of the Day 1)
- Screening bone marrow aspiration and biopsy up to 60 days prior to receiving study
medication
- An 8-week Treatment Period (Days 1 through 4 of Week 1, and weekly visits during Weeks
2 through 8); partial and complete responders in any of the three cell lines may
continue treatment for an additional 4 weeks
- A 6-month Post treatment Follow-up Period (monthly clinic visits during Weeks 12 40)
The myelodysplastic syndromes (MDS), a diverse group of hematopoietic stem cell (HSC)
disorders, are characterized by ineffective hematopoiesis that manifest clinically as
anemia, neutropenia, and/or thrombocytopenia. MDS is most frequently observed in the elderly
population (median age between 60 and 70 years) and has a male predominance. The incidence
of MDS varies from 2.1 to 12.6 cases per 100,000 people per year, with an estimated
prevalence of up to 55,000 patients in the United States [Catenacci, 2005; Williamson, 1994;
Aul, 1998; Aul, 2001]. Patients with MDS most frequently present with symptoms of fatigue,
pallor, exertional dyspnea, infection, bleeding or bruising [Catenacci, 2005].
MDS can be divided into 2 major subtypes: indolent (or early) MDS, in which pro-apoptotic
forces predominate, and aggressive (or advanced) MDS, in which pro-proliferative factors are
more common.
The only curative therapy for MDS is allogeneic transplantation [Catenacci, 2005; Thompson,
2005]. Curative treatments are restricted to younger, healthier individuals with
histocompatible-matched donors or those able to undergo intensive chemotherapeutic regimens
[Catenacci, 2005]. Recently, the FDA approved 3 agents for the treatment of this disease,
Vidaza, Dacogen, and revlimid. The latter is approved for a subset of patients with MDS with
del 5q abnormality, the former two are more applicable to higher risk disease. Rhu-EPO is
currently available to patients with low risk MDS however, if they fail, their options are
limited to the agents mentioned above, all of which have significant myelotoxic effects.
Effective and less myelosuppressive treatments for low-risk MDS are needed.
We are proposing a novel approach for the treatment of patients with low-risk MDS using heme
supplementation with Panhematin® (hemin for injection). Panhematin® is an iron-containing
metalloporphyrin, indicated for the amelioration of recurrent attacks of acute intermittent
porphyria; it acts to limit the hepatic and/or marrow synthesis of porphyrin, presumably, as
a result of the inhibition of aminolevulinic acid synthetase (the enzyme which limits the
rate of porphyrin/heme biosynthetic pathway) [Panhematin® Product Prescribing Information].
There are pre-clinical and clinical data to suggest that heme supplementation with
Panhematin® (hematin for injection) has potential as a treatment option for patients with
MDS. Preliminary data indicate hemin administration has the potential to stimulate
progenitor cell growth, stimulate globin synthesis, and elevate overall hemoglobin levels.
Panhematin® has been proven to be well tolerated when used therapeutically in patients with
acute intermittent porphyria, and it is anticipated to be well tolerated in this patient
population. For this study, selected patients will have low or intermediate 1 risk disease
by IPSS, and the standard of care for MDS (supportive therapies) will be administered as
needed. Measurement of serum porphyrin levels and Hgb F will be done at baseline and at week
8.
;
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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