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| ID | Type | Description | Link |
|---|---|---|---|
| 2022-502623-22-00 | Registry Identifier | CTIS (EU) |
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Researchers are looking for a better way to treat people who have advanced metastatic castration-resistant prostate cancer (mCRPC). In participants with metastatic castration-resistant prostate cancer (mCRPC), the cancer of the prostate has spread to other parts of the body (metastatic) and does not respond to the lowering of testosterone levels in the body (castration resistant). The cancer is 'advanced' and is unlikely to be cured or controlled with currently available treatments. Despite new treatment options for participant(s) with prostate cancer in recent years, the cancer often returns and worsens.
The study treatment actinium-225-macropa-pelgifatamab (also called 225Ac-pelgi or BAY3546828) is a new type of treatment under development for participants with mCRPC who have already received available treatments or have few treatment options available. It works by binding to a protein on the surface of the cancer cells called prostate specific membrane antigen (PSMA). As it gives off a type of radioactivity that travels a very short distance, it kills the nearby (cancer) cells that express PSMA.
The main purpose of this first-in-human study in participants with mCRPC is to learn:
To answer this, the researchers will look at:
Doctors keep track of all medical problems (also called adverse events) that participants have during the study, even if they do not think that they might be related to the study treatment.
Anticancer activity is measured using cancer imaging techniques and change in blood level of a protein called PSA. PSA is made by normal and by cancerous cells in the body. The PSA level is taken as a marker for prostate cancer development and is usually elevated in participants with mCRPC.
In addition, researchers want to find out how 225Ac-pelgi moves into, through and out of the body.
The study will have two parts. The first part, called dose escalation, is done to find the most appropriate dose and schedule that can be given in the second part of the study. For this, each participant will receive one of the predefined increasing doses of 225Ac-pelgi as an infusion into the vein. All participants in part 2, called dose expansion, will receive the most appropriate dose and schedule identified from the first part of the study. More than one dose level or schedule from part 1 may be tested. Both the participants and the study team know what treatment the participants will take.
Participants in this study will take the study treatment 225Ac-pelgi once in a period of 6 weeks called a cycle. Each participant will have 4 of these treatment cycles, if the participant benefits from the treatment.
Each participant will be in the study for up to nearly six years, including a first test (screening) phase of a maximum of 30 days, up to 12 months of treatment depending on the participant's benefit, and a follow-up phase of 60 months after the end of treatment. The following visits to the study site are planned: 2 during the screening phase, 8 in the first treatment cycle, 7 in subsequent cycles, and a visit 6 to 12 weeks after the last dose. In the following 12 months, visits are planned every 6 weeks and during the next 48 months phone calls or clinic visits are planned approximately every 12 weeks.
In addition, a sub study during the dose escalation part will gather information on the distribution of the study treatment in the body, the proportion that binds to the cancer cells, and the resulting radiation at the tumor site.
During the study, the study team will:
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Dose escalation of BAY3546828 | Experimental | Participants with advanced metastatic castration-resistant prostate cancer (mCRPC) will receive 225Ac-pelgi dose in a stepwise fashion, according to a predefined dose escalation scheme |
|
| Dose expansion group A of BAY3546828 | Experimental | Participants with advanced mCRPC with at least 1 but no more than 2 prior taxane regimens. No prior radionuclide therapy |
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| Dose expansion group B of BAY3546828 | Experimental | Participants with advanced mCRPC who have not received taxane chemotherapy since becoming castration-resistant. No prior radionuclide therapy. |
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| Dose expansion group C of BAY3546828 | Experimental | Participants with advanced mCRPC after prior Lutetium-177 labeled PSMA ligand (177Lu-PSMA) treatment. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| BAY3546828 | Drug | Intravenous (IV) infusion on Day 1 of each cycle. |
|
| Measure | Description | Time Frame |
|---|---|---|
| Dose escalation & Dose expansion: The Incidence of treatment-emergent adverse events (TEAEs) including treatment-emergent serious adverse events (TESAEs) | After first administration of study treatment up to 42 days after the last dose of study treatment | |
| Dose escalation & Dose expansion: The Severity of TEAEs including TESAEs | After first administration of study treatment up to 42 days after the last dose of study treatment | |
| Dose escalation: Incidence of dose limiting toxicities (DLTs) at each 225Ac dose level during the DLT observation period | DLTs will be summarized by MedDRA system organ class, preferred term and worst CTCAE grade. | Up to Cycle 3 (each cycle is 42 days) |
| Dose escalation: Objective response rate (ORR) at each 225Ac dose level during the DLT observation period | ORR is defined as the proportion of participants who have a confirmed complete response (CR) or partial response (PR) per PCWG3 guidelines, as assessed by the Investigator. | Up to Cycle 3 (each cycle is 42 days) |
| Dose escalation: ≥50% decline in Prostate-specific antigen value from baseline (Cycle 1, Day 1) (PSA50) response at each 225Ac dose level during the DLT observation period | PSA partial response is defined as a ≥50% decline in PSA value from Cycle 1 Day 1 (baseline). This PSA decline must be confirmed to be sustained by a second PSA value obtained 3 to 4 or more weeks later. | Up to Cycle 3 (each cycle is 42 days) |
| Dose expansion: Objective response rate (ORR) by Prostate Cancer Working Group 3 (PCWG3) guidelines based on investigator review | Up to 12 months after End of treatment |
| Measure | Description | Time Frame |
|---|---|---|
| Dose escalation & Dose expansion: Radiologic progression-free survival (rPFS ) by PCWG3 based on investigator review | rPFS is defined as the time from the start of study treatment to the date of first observed disease progression (Investigator's radiological assessment by PCWG3) or death due to any cause, if death occurs before progression is documented. | Up to 12 months after end of treatment |
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Inclusion Criteria:
mCRPC with pathological confirmation of adenocarcinoma without small-cell or neuroendocrine features.
Previous treatment with at least 1 Novel androgen axis drug (NAAD) (e.g., enzalutamide, apalutamide, darolutamide and/or abiraterone).
Prior orchiectomy and/or ongoing androgen deprivation therapy and a castrate level of serum testosterone (<50 ng/dL or <1.7 nmol/L).
Prior taxane treatment:
Prior treatment with an established 177Lu-PSMA therapy (i.e., dose activity and cycles comparable to approved treatments) is required for participants in Dose Expansion Group C only. More specifically, to qualify for this expansion group, participants must not have discontinued 177Lu-PSMA tratment due to intolerance.
Eastern Cooperative Oncology Group performance status (ECOG PS) of 0 or 1.
Adequate bone marrow, hepatic, and renal function, as assessed by the following laboratory requirements within 30 days before start of study intervention:
Participants must have at least one Prostate-specific membrane antigen (PSMA)-positive distant metastatic lesion on the screening PSMA PET/CT scan using the study-designated PSMA PET tracers, as determined by the site Investigator. For eligibility purposes, a PSMA-positive lesion must have activity greater than the liver by visual assessment of the screening PSMA PET/CT. A PSMA-positive metastatic lesion should not correspond to a normal tissue structure or benign lesion.
Documented progressive mCRPC per PCWG3, defined as meeting at least one of the following criteria:
Exclusion Criteria:
Participants who have any of the following tumor lesions which are PSMA negative AND meet the size criteria below are excluded as determined by the site investigator. A PSMA-negative lesion for eligibility purposes must have activity equal to or less than the liver by visual assessment of the screening PSMA PET/CT scan using the study-designated PSMA PET/CT tracers. A PSMA-negative metastatic lesion should not correspond to a normal tissue structure or benign lesion.
Prior systemic anticancer therapy including chemotherapy, NAAD, biologic therapy, immunotherapy, or investigational therapies within 4 weeks of the start of study intervention, except luteinizing hormone-releasing hormone (LHRH) or gonadotropin-releasing hormone (GnRH). Start of study intervention is allowed in shorter timeframes if 5 half-lives of the prior drug(s) have elapsed.
Prior radiopharmaceutical treatment using actinium-225.
Other prior radiopharmaceutical treatments:
Note: Participants who have discontinued 177Lu-PSMA treatment due to intolerance are excluded from Group C.
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| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| City of Hope - Duarte Cancer Center | Duarte | California | 91010 | United States | ||
| M Health Fairview Masonic Cancer Clinic - Clinics and Surgery Center |
| PubMed Identifier | Type | Citation | Retractions |
|---|---|---|---|
| 38593212 | Derived | Schatz CA, Zitzmann-Kolbe S, Moen I, Klotz M, Nair S, Stargard S, Bjerke RM, Wickstrom Biseth K, Feng YZ, Indrevoll B, Cruciani V, Karlsson J, Haendler B, Nielsen CH, Alfsen MZ, Hammer S, Hennekes H, Cuthbertson A, Hagemann UB, Larsen A. Preclinical Efficacy of a PSMA-Targeted Actinium-225 Conjugate (225Ac-Macropa-Pelgifatamab): A Targeted Alpha Therapy for Prostate Cancer. Clin Cancer Res. 2024 Jun 3;30(11):2531-2544. doi: 10.1158/1078-0432.CCR-23-3746. |
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Availability of this study's data will later be determined according to Bayer's commitment to the EFPIA/PhRMA "Principles for responsible clinical trial data sharing". This pertains to scope, timepoint and process of data access. As such, Bayer commits to sharing upon request from qualified researchers patient-level clinical trial data, study-level clinical trial data, and protocols from clinical trials in patients for medicines and indications approved in the US and EU as necessary for conducting legitimate research. This applies to data on new medicines and indications that have been approved by the EU and US regulatory agencies on or after January 01, 2014.
Interested researchers can use www.vivli.org to request access to anonymized patient-level data and supporting documents from clinical studies to conduct research. Information on the Bayer criteria for listing studies and other relevant information is provided in the member section of the portal.
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| Dose expansion: ≥50% decline in Prostate-specific antigen value from baseline (Cycle 1, Day 1) (PSA50) response at 12 weeks or later | At 12 weeks or later (up to 12 months after End of treatment) |
| Dose expansion: Best overall Prostate-specific antigen (PSA) response | Up to 12 months after End of treatment |
| Dose escalation & Dose expansion: Duration of PSA50 response | Duration of PSA50 response by PCWG3 is defined as the time from the first documented PSA partial response as defined above to PSA progression by PCWG3 or death (if death occurs before progression is documented). | Up to 12 months after end of treatment |
| Dose escalation & Dose expansion: Duration of response (DOR) by PCWG3 based on investigator review | DOR is defined as the time from the first documented objective response of PR or CR by PCWG3, whichever occurs earlier, to disease progression or death (if death occurs before progression is documented). | Up to 12 months after end of treatment |
| Dose escalation: Recommended dose level(s) of 225Ac-pelgi for dose expansion | Up to 4 cycles (each cycle is 42 days) |
| Dose escalation: Recommended dose schedule of 225Ac-pelgi for dose expansion | Up to 4 cycles (each cycle is 42 days) |
| Dose expansion: Recommended dose of 225Ac-pelgi for further clinical development | Up to 4 cycles (each cycle is 42 days) |
| Dose expansion: Recommended dose schedule of 225Ac-pelgi for further clinical development | Up to 4 cycles (each cycle is 42 days) |
| Dose escalation & Dose expansion: Maximum observed concentration (Cmax) of actinium-225 | Cycle 1, cycle 2 (From Pre-dose up to Day 36 post-dose for each cycle) |
| Dose escalation & Dose expansion: Maximum observed concentration (Cmax) of total antibody | Cycle 1, cycle 2 (From Pre-dose up to Day 36 post-dose for each cycle) |
| Dose escalation & Dose expansion: Area under the curve (AUC) of actinium-225 | Cycle 1, cycle 2 (From Pre-dose up to Day 36 post-dose for each cycle) |
| Dose escalation & Dose expansion: Area under the curve (AUC) of total antibody | Cycle 1, cycle 2 (From Pre-dose up to Day 36 post-dose for each cycle) |
| Minneapolis |
| Minnesota |
| 55455 |
| United States |
| XCancer Omaha | Omaha | Nebraska | 68130 | United States |
| The University of Texas MD Anderson Cancer Center - Texas Medical Center | Houston | Texas | 77030 | United States |
| Utah Cancer Specialists Cancer Center - Medical Oncology | Salt Lake City | Utah | 84106 | United States |
| Centre Hospitalier de l'Universite de Montreal (CHUM) | Oncology | Montreal | Quebec | H2X 0C1 | Canada |
| Research Institute of the McGill University Health Centre | McConnell Centre for Innovative Medicine | Montreal | Quebec | H4A 3J1 | Canada |
| Centre hospitalier universitaire de Sherbrooke (CHUS) | Oncology | Sherbrooke | Quebec | J1H 5N4 | Canada |
| Kuopio University Hospital, Kuopion yliopistollinen sairaala (KYS) - Syövänhoitokeskus | Kuopio | Northern Savonia | 70210 | Finland |
| Tampere University Hospital, Tampereen yliopistollinen sairaala (TAYS) - Syöpäkeskus | Tampere | Pirkanmaa | 33520 | Finland |
| CRST Oy - Clinical Research Services Turku | Turku | Southwest Finland | 20520 | Finland |
| HUS-Yhtymä, Helsingin yliopistollinen sairaala (HUS) - Syöpäkeskus | Helsinki | Uusimaa | 00029 | Finland |
| Docrates Mehiläinen Syöpäsairaala | Helsinki | Uusimaa | 00180 | Finland |
| Istituto Europeo di Oncologia s.r.l - Medicina Nucleare | Milan | 20141 | Italy |
| IRCCS Istituto Nazionale Tumori Fondazione Pascale - S. C. Medicina Nucleare e Terapia Metabolica | Naples | 80131 | Italy |
| Erasmus Medisch Centrum | Rotterdam | South Holland | 3015 CE | Netherlands |
| Universitair Medisch Centrum Groningen | Groningen | 9713 GZ | Netherlands |
| Skånes Universitetssjukhus - Lund - Onkologens kliniska forskningsenhet | Lund | Skåne County | 221 85 | Sweden |
| Karolinska Universitetssjukhuset - Solna - Fas I-enheten Solna CKC | Stockholm | Stockholm County | 171 76 | Sweden |
| Akademiska sjukhuset i Uppsala - Fas 1-enheten | Uppsala | Uppsala County | 751 85 | Sweden |
| Sahlgrenska Universitetssjukhuset - Sahlgrenska Sjukhuset - Klinisk prövningsenhet Fas I/FIH | Gothenburg | Västra Götaland County | 413 46 | Sweden |
| Kantonsspital Baden | Baden | Canton of Aargau | 5404 | Switzerland |
| Universitätsspital Basel | Basel | Canton of Basel-City | 4056 | Switzerland |
| UniversitätsSpital Zürich (USZ) - Klinik für Medizinische Onkologie und Hämatologie | Zurich | 8091 | Switzerland |
| Cambridge University Hospitals NHS Foundation Trust | Addenbrookes Hospital - Clinical Research Centre | Cambridge | Cambridgeshire | CB2 0QQ | United Kingdom |
| University College London Hospitals NHS Foundation Trust | University College Hospital - NIHR UCLH Clinical Research Facility | London | Greater London | W1T 7HA | United Kingdom |
| The Royal Marsden NHS Foundation Trust | Sutton - Oak Foundation Drug Development Unit | Sutton | Surrey | SM2 5PT | United Kingdom |
| The Newcastle upon Tyne Hospitals NHS Foundation Trust | Freeman Hospital - Cancer Trials Research Centre | Newcastle upon Tyne | Tyne and Wear | NE7 7DN | United Kingdom |