Kancera AB (publ) reports the top line results from the FRACTAL study, a double-blinded placebo-controlled, explorative phase IIa study of Kancera?s fractalkine blocker KAND567 in high-risk ST-elevation myocardial infarction (STEMI) patients undergoing acute percutaneous coronary intervention (PCI). The study met the primary objective to confirm the favourable safety and tolerability profile of KAND567 in myocardial infarction patients. In addition, the secondary objective to demonstrate signals of clinically relevant cardio-protective effects was met.

FRACTAL is an explorative phase IIa, randomized, two-armed parallel-group, placebo-controlled, double-blind, multi-centre trial with the primary objective to evaluate safety and tolerability and the secondary objective to evaluate cardio-protective effects after intravenous and oral administration of KAND567 in STEMI patients undergoing percutaneous coronary intervention. The study has been conducted in collaboration with the Newcastle upon Tyne Hospitals NHS Foundation Trust (NHS), also sponsor of the study and who has compiled the data and provided an end of study report. In total, 71 patients were recruited to the study and 61 patients completed the required steps to be considered fully evaluable.

The selected dosage of KAND567 resulted in an adequate plasma concentration of the drug candidate and expected effect on the fractalkine axis. The analysis of the primary endpoints based on NHS?s end of study report shows. that KAND567 and placebo had similar safety profiles.

Accordingly, the trial oversight committee at NHS concluded that KAND567 met the primary endpoint for safety and tolerability in myocardial infarction patients. The analysis of the secondary endpoints shows signals of heart-protective effects: reduction of intramyocardial hemorrhage incidence (38% in the KAND567 group vs 57% in the placebo group). The level in the placebo group is in line with prior studies in high-risk STEMI and hence the reduction in the KAND567 group is perceived to be clinically relevant as IM hemorrhage is strongly correlated with an increased risk of developing heart failure.

reduction of left ventricular (LV) thrombosis incidence (3% in the KAND567 group vs 15% in the placebo group). The level in the placebo group is in line with prior studies in high-risk STEMI and hence the reduction in the KAND567 group is perceived to be clinically relevant as LV thrombosis is strongly correlated with an increased risk of cardioembolic stroke or systemic embolism. all other markers of cardiac function and integrity were similar between patients receiving KAND567 or placebo, respectively, but all were numerically in favor of the KAND567 group when comparing change Day 3 and Day 90.

Kancera will now conduct detailed analyses of the full study data set and report any potential further significant findings as soon as they become available. Kancera views the top line results in this explorative phase IIa study as very positive, providing clear signals of cardio-protective effects. In addition to confirming the favourable safety profile, the results support the hypothesis that KAND567 is a ?first in class?

drug candidate with potential to protect against reperfusion injury by reducing intramyocardial hemorrhage as well as LV thrombus formation. Both factors are strongly related to increased cardiovascular events and mortality risk. The reduced incidence of LV thrombosis was achieved on top of an intensive anticoagulant and antiplatelet therapy.

If this overall effect profile can be confirmed in larger pivotal studies, KAND567 has the potential to meet a significant medical need for improved protection of vital organ function in patients undergoing reperfusion treatment such as STEMI or large vessel occlusion stroke. Kancera now takes action to continue the development of KAND567 for treatment of cardiovascular diseases and has exercised its option according to the clinical trial agreement with NHS to obtain exclusive commercial rights to all study data and results. Kancera will intensify its business development activities with the objective to enter into a partnership for the continued development of KAND567 for treatment of cardiovascular diseases.

The FRACTAL study is an explorative clinical phase IIa study of Kancera?s fractalkine-blocking drug candidate KAND567 when added to standard of care in STEMI patients undergoing acute primary percutaneous coronary intervention (PCI), including heparin, glycoprotein IIb/IIIa inhibitors and dual antiplatelet inhibitors. The study, a two-arm, double-blinded and placebo-controlled study, was conducted at the two hospitals: the Freeman Hospital in Newcastle and the James Cook University Hospital in Middlesbrough. Chief Investigator of the study was Professor Ioakim Spyridopoulos, Professor of Cardiology and Cardiovascular Gerontology, Newcastle University and sponsor was the Newcastle upon Tyne Hospitals NHS Foundation Trust.

Participants were randomized (1:1) to receive intravenous infusion of KAND567 for 6 hours, followed by a bridging dose of up to 200mg KAND567 orally after the infusion (bridging dose dependent on the time of primary PCI procedure, followed by 8 doses of 200mg of KAND567, 8 hours apart, or, a matched placebo). All participants who received any dose of KAND567 or placebo, and for whom any post-dose data were available were included in the safety analysis set. Any participant receiving any dose of KAND567 was treated as if they were allocated to the active arm.

Of the 71 patients recruited in total, 35 and 36 patients were randomized to the KAND567 group and placebo group, respectively. The primary objective was to evaluate safety and tolerability of KAND567, assessed on Adverse Events, Severe Adverse Events and Suspected Unexpected Serious Adverse Reactions, cumulatively for each arm from baseline up to day 90 and on safety laboratory parameters. The secondary objective was to evaluate signs of cardio-protective effects, which has been assessed through a range of inflammatory biomarkers and magnetic resonance imaging (MRI) markers.