Polycythemia Vera Clinical Trial
Official title:
A Randomized, Open-label, Multicenter, Controlled, Parallel Arm, Phase III Study Assessing the Efficacy and Safety of AOP2014 vs. Hydroxyurea in Patients With Polycythemia Vera
Phase III study to compare the efficacy and safety of the novel monopegylated interferon alpha 2b AOP2014 versus Hydroxyurea (the current licensed therapy for this disease). One year treatment of patients with polycythemia vera. Objective is to demonstrate non-inferiority of AOP2014 vs. HU in terms of disease response rate in both HU naïve and currently treated patients, diagnosed with Polycythemia Vera. Response is measured as normalisation of key lab parameters as well as normalized spleen size.
Hydroxyurea is an established first-line treatment option currently approved in several
European countries for Polycythemia Vera (PV) patients requiring a cytoreductive therapy
(Barbui et al, 2011). Clinical trials have shown that HU is an effective drug for preventing
thrombosis in PV compared to phlebotomy (Michiels et al, 1999).
The main concern of a long term treatment with HU is its potential leukaemogenicity: based
on the mechanism of action, HU can potentially accelerate the accumulation of mutations in
DNA and increase the risk of leukaemic transformation (Dingli et Tefferi, 2006). However,
there is currently no clear clinical data to confirm leukaemogenicity of HU in patients with
PV (Tefferi, 2012).
Even though IFN-alpha has shown its activity in PV in the 1980s, it is still considered as
an experimental treatment in Europe due to pending approval in this indication (Barbui et
al, 2011). It induces major or complete molecular remissions in patients with PV accompanied
by a reduction in the risk of thrombosis and bleeding - the major determinants of morbidity
in this indication (Hasselbalch, 2011). However, only low doses are tolerated and
significant adverse effects from long-term use may limit its usefulness.
Pegylated interferons are better tolerated and are the preferred options of treatment in PV
patients (Kiladjian et al, 2008) despite the lack of evidences based on well-designed
randomized controlled clinical studies.
AOP2014 is a next generation pegylated interferon (Peg-P-IFN-alpha-2b), with the addition of
proline in the N-terminal end.
AOP2014 like all interferon suppresses the malignant clone causing PV and subsequently is
expected to possibly defer the onset of or avoid long term sequelae of PV. In addition, a
reduction in the frequency of phlebotomies should be achieved. The peg-P-IFN-alpha-2b might
potentially have a positive impact on reducing the drop-out rate compared to conventional
IFNs. It is expected that the reduced frequency of administration of AOP2014 will contribute
to higher compliance rates.
The maximum tolerated dose as well as the safety, efficacy and pharmacokinetics of AOP2014
were assessed in a phase I/II study in patients with PV. After 24 evaluable patients had
entered the Phase I dose finding part, the MTD was defined at the level of 540 µg
administered every two weeks. Another 27 patients were recruited in order to further
investigate the drug efficacy and safety in PV. Efficacy results of AOP2014 were promising.
By visit 18, 53.0% of the patients had reached complete response (12 evaluable patients).
Adverse events were manageable and rarely necessitated treatment discontinuation.
AOP2014 was shown to have a prolonged plasma half-life with a concomitant increase in AUC.
This is expected to enhance the therapeutic window of peg-IFN-alpha-2b.
The safety profile of type I interferons alpha is believed to be well characterized after
clinical experience for nearly 20 years. Since the dose is carefully titrated to the optimal
effective dose no additional risks for the patients are expected. HU, the IMP-comparator in
the study, is the standard reference treatment in PV.
This phase III study was designed to compare, for the first time, the efficacy and safety of
HU with a pegylated prolin-interferon alpha-2b (AOP2014) in patients with PV. Two
populations will be assessed: HU naïve patients and patients currently treated or
pre-treated with HU for less than 3 years, not responding to HU treatment (according to
criteria in this protocol).
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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