Kancera is developing two fractalkine blocking candidate drugs, KAND567 and KAND145, both in clinical stage: KAND567, primarily developed for cardiovascular diseases caused by hyperinflammation, is the lead candidate in the fractalkine program and is currently being studied in two ongoing clinical studies, FRACTAL and KANDOVA. KAND145, the company?s second generation fractalkine blocker primarily intended for treatment of cancer, is currently being studied in a recently initiated phase I first-in-human study in healthy subjects. FRACTAL: FRACTAL is a phase IIa study of KAND567 in myocardial infarction patients undergoing percutaneous coronary intervention that is being conducted in collaboration with the Newcastle Hospitals NHS Foundation Trust (NHS).

All patients have been enrolled and gone through all treatment steps. All laboratory analyses of data related to the primary and secondary endpoints have been completed and the study database has been validated and locked. As previously has been reported, Kancera?s presentation of the top line results are delayed due to lack of statistical resources within the NHS.

Kancera now expects that top line results will be presented by the end of December this year. NHS is currently conducting the statistical analysis, which is the final remaining activity before the data can be unblinded, provided to Kancera and presented externally. KANDOVA: KANDOVA is a two-part clinical study of KAND567 in ovarian cancer patients aiming to increase the efficacy of carboplatin in relapsed disease.

The first part is a phase Ib study with the objective to define the maximum safe and tolerable dose of KAND567. This dose will then been used in the second part, a phase IIa study, with the objective to evaluate KAND567?s treatment efficacy. As of today, five Nordic hospitals are activated in the study.

In the second part of the study, Kancera intends to activate two additional sites. Depending on what maximum dose level will be tolerable, Kancera expects that approximately 6-12 patients will be required to finalize the phase Ib part of the study. With the objective to study 30 patients in total, 18-24 patients will be enrolled to the phase IIa part of the study.

As of November 17, two patients have been enrolled to the study. In collaboration with the primary investigator, Kancera has analyzed the key root causes for screening failure and identified opportunities to increase recruitment by making certain protocol adjustments. These modifications to the study protocol are now submited to the applicable regulatory authorities.

Approval of the amended study protocol is expected during the first quarter 2024. Kancera expects that the amended protocol will increase the recruitment of patients and the goal to roll over to phase IIa during the second quarter next year thereby remains. The goal to present the top line results before year end 2024 also remains, as Kancera expects that the seven hospitals that will be active in phase IIa will be capable of recruiting approximately 2-4 patients each.

Phase I study of KAND145: Kancera has previously reported that the company?s application to conduct a phase I first-in-human study of KAND145 has received regulatory approval. The study, that is being conducted at two sites in Finland, has now started and the first subjects have been enrolled and dosed with KAND145. Kancera expects to present top line results from the study in Second Quarter 2024, in line with the overall development plan for KAND145 in cancer.

Strategic review of preclinical project portfolio: Ever since the acquisition of the fractalkine program Kancera?s primary focus has been to develop the two candidate drugs KAND567 and KAND145. Kancera?s resources have mainly been allocated to these two candidate drugs and other preclinical projects in the portfolio have been managed primarily through academic collaborations at lower pace. Kancera?s management has conducted a strategic review of the company?s project portfolio.

When considering the expected lead times and costs for remaining development and the remaining patent term, management has concluded that the preclinical projects KAN571 (ROR1 inhibitor) and KAN757 (PFKFB3 inhibitor) are no longer commercially viable for Kancera. The company has therefore decided to discontinue the projects. The decision is made on strict commercial grounds, i.e. there is a lack of a sound business case and outlicensing is not believed to be feasible.

The discontinuation of these preclinical projects will allow Kancera to even further focus its resources and efforts on the clinical development of KAND567 and KAND145. Going forward, the company?s preclinical activities will be focused on fields closely related to the clinical development of these two candidate drugs. The preclinical data that has been generated in the ROR1 project still supports the rationale for ROR1 as a suitable target for treatment of various cancers, e.g. B-cell malignancies.

In order to enable continued research in the field, Kancera will make all data generated in the ROR1 project available for the research units at Karolinska Institute that have been involved in the project up until now.