Prostatic Neoplasms Clinical Trial
— PSMAforeOfficial title:
PSMAfore: A Phase III, Open-label, Multi-Center, Randomized Study Comparing 177Lu-PSMA-617 vs. a Change of Androgen Receptor-directed Therapy in the Treatment of Taxane Naïve Men With Progressive Metastatic Castrate Resistant Prostate Cancer
Verified date | March 2024 |
Source | Novartis |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
The purpose of this study is to determine whether 177Lu-PSMA-617 improves the rPFS or death compared to a change in ARDT in mCRPC participants that were previously treated with an alternate ARDT and not exposed to a taxane-containing regimen in the CRPC or mHSPC settings. Approximately 450 participants will be randomized (225 per treatment group).
Status | Active, not recruiting |
Enrollment | 469 |
Est. completion date | September 30, 2025 |
Est. primary completion date | October 3, 2022 |
Accepts healthy volunteers | No |
Gender | Male |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: 1. Signed informed consent must be obtained prior to participation in the study. 2. Participants must be adults >= 18 years of age. 3. Participants must have an ECOG performance status of 0 to 1. 4. Participants must have histological pathological, and/or cytological confirmation of adenocarcinoma of the prostate. 5. Participants must be 68Ga-PSMA-11 PET/CT scan positive, and eligible as determined by the sponsor's central reader. 6. Participants must have a castrate level of serum/plasma testosterone (< 50 ng/dL or < 1.7 nmol/L). 7a. Participants must have progressed only once on prior second generation ARDT (abiraterone, enzalutamide, darolutamide, or apalutamide). - First generation androgen receptor inhibitor therapy (e.g. bicalutamide) is allowed but not considered as prior ARDT therapy. - Second generation ARDT must be the most recent therapy received. 8. Participants must have progressive mCRPC. Documented progressive mCRPC will be based on at least 1 of the following criteria: - Serum/plasma PSA progression defined as 2 increases in PSA measured at least 1 week apart. The minimal start value is 2.0 ng/mL; 1.0 ng/mL is the minimal starting value if confirmed rise in PSA is the only indication of progression. - Soft-tissue progression defined [PCWG3-modified RECIST v1.1 (Eisenhauer et al 2009, Scher et al 2016)]. - Progression of bone disease: two new lesions; only positivity on the bone scan defines metastatic disease to bone (PCWG3 criteria (Scher et al 2016)). 9a. Participants must have >= 1 metastatic lesion that is present on baseline CT, MRI, or bone scan imaging obtained prior to randomization. 10. Participants must have recovered to =< Grade 2 from all clinically significant toxicities related to prior therapies (i.e. prior chemotherapy, radiation, etc.) except alopecia. 11. Participants must have adequate organ function: - Bone marrow reserve: - ANC >= 1.5 x 109/L - Platelets >= 100 x 109/L - Hemoglobin >= 9 g/dL - Hepatic: - Total bilirubin < 2 x the institutional upper limit of normal (ULN). For participants with known Gilbert's Syndrome =< 3 x ULN is permitted. - ALT or AST =< 3.0 x ULN OR =< 5.0 x ULN for participants with liver metastases. - Renal: - eGFR >= 50 mL/min/1.73m2 using the Modification of Diet in Renal Disease (MDRD) equation. 12. Albumin >= 2.5 g/dL. 13a. Candidates for change in ARDT as assessed by the treating physician: - Participants cannot have previously progressed nor had intolerable toxicity to both enzalutamide and abiraterone. Exclusion Criteria: 1. Previous treatment with any of the following within 6 months of randomization: Strontium-89, Samarium-153, Rhenium-186, Rhenium-188, Radium-223, hemi-body irradiation. 2. Previous PSMA-targeted radioligand therapy. 3a. Prior treatment with cytotoxic chemotherapy for castration resistant or castrate sensitive prostate cancer (e.g., taxanes, platinum, estramustine, vincristine, methotrexate, etc.), immunotherapy or biological therapy [including monoclonal antibodies]. [Note: Taxane exposure (maximum 6 cycles) in the adjuvant or neoadjuvant setting is allowed if 12 months have elapsed since completion of this adjuvant or neoadjuvant therapy. Prior treatment with sipuleucel-T is allowed]. 4. Any investigational agents within 28 days prior to day of randomization. 5. Known hypersensitivity to any of the study treatments or its excipients or to drugs of similar classes. 6a. Concurrent cytotoxic chemotherapy, immunotherapy, radioligand therapy, PARP inhibitor, biological therapy, or investigational therapy. 7. Transfusion or use of bone marrow stimulating agents for the sole purpose of making a participant eligible for study inclusion. 8a. Participants with a history of CNS metastases who are neurologically unstable, symptomatic, or receiving corticosteroids for the purpose of maintaining neurologic integrity. Participants with CNS metastases are eligible if received therapy (surgery, radiotherapy, gamma knife), asymptomatic and neurologically stable without corticosteroids. Participants with epidural disease, canal disease and prior cord involvement are eligible if those areas have been treated, are stable, and not neurologically impaired. 9. Symptomatic cord compression, or clinical or radiologic findings indicative of impending cord compression. 10. History or current diagnosis of the following ECG abnormalities indicating significant risk of safety for study participants: - Concomitant clinically significant cardiac arrhythmias, e.g. sustained ventricular tachycardia, complete left bundle branch block, high-grade AV block (e.g., bifascicular block, Mobitz type II and third degree AV block). - History of familial long QT syndrome or known family history of Torsades de Pointe. - Cardiac or cardiac repolarization abnormality, including any of the following: History of myocardial infarction (MI), angina pectoris, or CABG within 6 months prior to starting study treatment. 11a. Concurrent serious (as determined by the Principal Investigator) medical conditions, including, but not limited to New York Heart Association class III or IV congestive heart failure, history of congenital prolonged QT syndrome, uncontrolled infection, known active hepatitis B or C or other significant co-morbid conditions that in the opinion of the investigator would impair study participation or cooperation. - HIV-infected participants who are at a low risk of AIDS-related outcomes may participate in this trial. - Participants with an active documented COVID-19 infection (any grade of disease severity) at time of informed consent may be included only when completely recovered (in accordance with local guidance). 12a. Diagnosed with other malignancies that are expected to alter life expectancy or may interfere with disease assessment. However, participants with a prior history of malignancy that has been adequately treated and who have been disease free and treatment free for more than 3 years prior to randomization, are eligible, as are participants with adequately treated non-melanoma skin cancer and superficial bladder cancer. 13a. Sexually active males unwilling to use a condom during intercourse while taking study treatment and for 14 weeks after stopping study treatment. A condom is required for all sexually active male participants to prevent them from fathering a child AND to prevent delivery of study treatment via seminal fluid to their partner. In addition, male participants must not donate sperm for the time period specified above. If local regulations deviate from the contraception methods listed above to prevent pregnancy, local regulations apply and will be described in the ICF. 14a. Unmanageable concurrent bladder outflow obstruction or urinary incontinence. Note: Participant with bladder outflow obstruction or urinary incontinence, which is manageable and controlled with best available standard of care (incl. pads, drainage) are allowed. 15. History of somatic or psychiatric disease/condition that may interfere with the objectives and assessments of the study. 16. Any condition that precludes raised arms position. 17a. Eligible for treatment(s) other than ARDT based on presence of any mutations or biomarkers that are known as predictors of better response (e.g., AR-V7 or BRCA). 18. Not able to understand and to comply with study instructions and requirements. |
Country | Name | City | State |
---|---|---|---|
Austria | Novartis Investigative Site | Innsbruck | Tyrol |
Austria | Novartis Investigative Site | Linz | |
Austria | Novartis Investigative Site | Wien | |
Belgium | Novartis Investigative Site | Bruxelles | |
Belgium | Novartis Investigative Site | Gent | |
Belgium | Novartis Investigative Site | Liege | |
Belgium | Novartis Investigative Site | Roeselare | |
Canada | Novartis Investigative Site | Montreal | Quebec |
Canada | Novartis Investigative Site | Montreal | Quebec |
Canada | Novartis Investigative Site | Vancouver | British Columbia |
Czechia | Novartis Investigative Site | Olomouc | CZE |
France | Novartis Investigative Site | Angers 02 | |
France | Novartis Investigative Site | Bordeaux | |
France | Novartis Investigative Site | Clermont-Ferrand | |
France | Novartis Investigative Site | Lyon | |
France | Novartis Investigative Site | Paris | |
France | Novartis Investigative Site | Villejuif | |
Germany | Novartis Investigative Site | Essen | |
Germany | Novartis Investigative Site | Muenchen | |
Netherlands | Novartis Investigative Site | Maastricht | |
Netherlands | Novartis Investigative Site | Nijmegen | Netherland |
Netherlands | Novartis Investigative Site | Utrecht | |
Poland | Novartis Investigative Site | Gliwice | Slaskie |
Slovakia | Novartis Investigative Site | Bratislava | Slovak Republic |
Spain | Novartis Investigative Site | Barcelona | Catalunya |
Spain | Novartis Investigative Site | Barcelona | Catalunya |
Spain | Novartis Investigative Site | Barcelona | |
Spain | Novartis Investigative Site | El Palmar | Murcia |
Spain | Novartis Investigative Site | Hospitalet de LLobregat | Catalunya |
Spain | Novartis Investigative Site | Madrid | |
Spain | Novartis Investigative Site | Madrid | |
Spain | Novartis Investigative Site | Madrid | |
Spain | Novartis Investigative Site | Madrid | |
Spain | Novartis Investigative Site | Malaga | Andalucia |
Spain | Novartis Investigative Site | Pamplona | Navarra |
Spain | Novartis Investigative Site | Santiago De Compostela | Galicia |
Spain | Novartis Investigative Site | Sevilla | Andalucia |
Spain | Novartis Investigative Site | Valencia | Comunidad Valenciana |
Spain | Novartis Investigative Site | Valencia | |
Sweden | Novartis Investigative Site | Goteborg | |
Sweden | Novartis Investigative Site | Lund | |
Sweden | Novartis Investigative Site | Stockholm | |
Switzerland | Novartis Investigative Site | Baden | |
Switzerland | Novartis Investigative Site | Lausanne | |
Switzerland | Novartis Investigative Site | Zuerich | |
United Kingdom | Novartis Investigative Site | Coventry | |
United Kingdom | Novartis Investigative Site | Guildford | Surrey |
United Kingdom | Novartis Investigative Site | London | |
United Kingdom | Novartis Investigative Site | London | |
United Kingdom | Novartis Investigative Site | London | |
United Kingdom | Novartis Investigative Site | Middlesbrough | Yorkshire |
United Kingdom | Novartis Investigative Site | Sutton | Surrey |
United States | Beth Israel Deaconess Med Ctr Dept. of BIDMC | Boston | Massachusetts |
United States | Dana Farber Cancer Institute Dana-Farber Cancer Institute_ | Boston | Massachusetts |
United States | The Ohio State University Comprehensive Cancer Center PulmonaryClinicalTrialsOffice | Columbus | Ohio |
United States | Duke Univ Medical Center Morris Building | Durham | North Carolina |
United States | Univ of Florida College of Medicine x | Gainesville | Florida |
United States | Uni of TX MD Anderson Cancer Cntr | Houston | Texas |
United States | Rocky Mountain Cancer Centers RMCC - Aurora | Longmont | Colorado |
United States | Medical College of Wisconsin . | Milwaukee | Wisconsin |
United States | Sarah Cannon Research Institute . | Nashville | Tennessee |
United States | Tulane Uni Health Sciences Center . | New Orleans | Louisiana |
United States | Memorial Sloan Kettering Cancer Ctr Memorial Sloan Kettering CC | New York | New York |
United States | Mount Sinai Hosp School of Med Tisch Cancer Institute | New York | New York |
United States | NYU Laura and Isaac Perlmutter Cancer Center NYU Langone Medical Center | New York | New York |
United States | Virginia Oncology Associates VOA - Lake Wright | Norfolk | Virginia |
United States | Nebraska Cancer Specialists Oncology Hematology West | Omaha | Nebraska |
United States | Urology Cancer Center PC | Omaha | Nebraska |
United States | Onco Hemato Asso of SE Virginia Roanoke Loc | Roanoke | Virginia |
United States | Washington Uni School of Med Siteman Cancer Center | Saint Louis | Missouri |
United States | Utah Cancer Specialists UT Cancer Cnt | Salt Lake City | Utah |
United States | Seattle Cancer Care Alliance . | Seattle | Washington |
Lead Sponsor | Collaborator |
---|---|
Novartis Pharmaceuticals |
United States, Austria, Belgium, Canada, Czechia, France, Germany, Netherlands, Poland, Slovakia, Spain, Sweden, Switzerland, United Kingdom,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Radiographic Progression Free Survival (rPFS) | rPFS is defined as the time to radiographic progression by PCWG3-modified RECIST v1.1 (as assessed by Blinded independent central review) or death. | From date of randomization until date of radiographic progression or date of death from any cause, whichever comes first, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Overall survival (OS) | OS is defined as time to death for any cause | From date of randomization until date of death from any cause, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Radiographic Progression Free Survival 2 (rPFS2) | rPFS2 is defined as time from the date of crossover (ARDT to 177Lu-PSMA-617) to the date of radiographic disease progression by BICR or death from any cause | Only for participants that crossover from ARDT arm to Lu-PSMA treatment. From date of crossover until second radiographic progression or death, whichever comes first, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Progression Free survival (PFS) by investigator's assessment | PFS is defined as time from date of randomization to the first documented progression by investigator's assessment (radiographic, clinical, or PSA progression) or death from any cause, whichever occurs first | From date of randomization until date of progression or date of death from any cause, whichever comes first, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Second Progression Free Survival (PFS2) by investigator's assessment | PFS2 defined as time from date of randomization to the first documented progression by investigator's assessment (radiographic progression, clinical progression, PSA progression) or death from any cause, whichever occurs first, on next-line of therapy | From date of randomization until date of second progression or date of death from any cause, whichever comes first, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Biochemical response | PSA50 defined as proportion of participants who achieved a = 50% decrease from baseline that is confirmed by a second PSA measurement = 4 weeks.
PSA50 will be evaluated at 3, 6 and 12 months. |
From date of randomization till 30 day safety follow-up, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Time to First Symptomatic Skeletal Event (TTSE) | Time to SSE (TTSSE) defined as date of randomization to the date of first new symptomatic pathological bone fracture, spinal cord compression, tumor-related orthopedic surgical intervention, requirement for radiation therapy to relieve bone pain or death from any cause, whichever occurs first | From date of randomization till EOT or death, whichever happens first, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Time to radiographic soft tissue progression (TTSTP) | TTSTP defined as time from randomization to radiographic soft tissue progression per PCWG3-modified RECIST v1.1 (Soft Tissue Rules of Prostate Cancer Working Group modified Response Evaluation Criteria in Solid Tumors Version 1.1) as Assessed by Blinded Independent Central Review (BICR) | From date of randomization until date of soft tissue radiographic progression or date of death from any cause, whichever comes first, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Time to chemotherapy (TTCT) | TTCT defined as time from randomization to initiation of the first subsequent chemotherapy or death, whichever occurs first | From date of randomization until date of subsequent chemotherapy or date of death from any cause, whichever comes first, assessed up to 43 months (estimated final OS analysis) | |
Secondary | European Quality of Life (EuroQol) - 5 Domain 5 Level scale (EQ-5D- 5L) | EQ-5D-5L is a standardized participant completed questionnaire that measures health-related quality of life and translates that score into an index value or utility score. EQ-5D-5L consists of two components: a health state profile and an optional visual analogue scale (VAS). EQ-5D health state profile is comprised of 5 dimensions: mobility, self-care, usual activities, pain/discomfort and anxiety/depression. Each dimension has 5 levels: 1= no problems, 2= slight problems, 3= moderate problems, 4= severe problems, and 5= extreme problems. Higher scores indicated greater levels of problems across each of the five dimensions. | From randomization up till 30 day safety Follow-up or week 48 of long term Follow-up for patients prematurely discontinued, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Functional Assessment of Cancer Therapy - Prostate (FACT-P) Questionnaire | FACT-P assesses symptoms/problems related to prostate carcinoma and its treatment. It is a combination of the FACT- General + the Prostate Cancer Subscale (PCS). The FACTGeneral (FACT-G) is a 27 item Quality of Life (QoL) measure that provides a total score as well as subscale scores: Physical (0-28), Functional (0-28), Social (0-28), and Emotional Well-being (0-24). The total score range is between 1-108, higher scores indicates better for total score and subscale scores. PCS is a 12-item prostate cancer subscale that asks about symptoms and problems specific to prostate cancer (Range 0-48, higher scores better). The FACT-P total score is the sum of all 5 subscale scores of the FACT-P questionnaire and ranges from 0-156. Higher scores indicate higher degree of functioning and better quality of life. | From randomization up till 30 day safety Follow-up or week 48 of long term Follow-up for patients prematurely discontinued, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Brief Pain Inventory - Short Form (BPI-SF) Questionnaire | The BPI-SF is a publicly available instrument to assess the pain and includes severity and interference scores. BPI-SF is an 11-item selfreport questionnaire that is designed to assess the severity and impact of pain on daily functions of a participant. Pain severity score is a mean value for BPI-SF questions 3, 4, 5 and 6 (questions inquiring about the extent of pain, where the extent is ranked from 0 [no pain] to 10 [pain as bad as you can imagine]). Pain severity progression is defined as an increase in score of 30% or greater from baseline without decrease in analgesic use. | From screening up till 30 day safety Follow-up or week 48 of long term Follow-up for patients prematurely discontinued, assessed up to 43 months (estimated final OS analysis) | |
Secondary | Number of Participants with Treatment Emergent Adverse Events | The distribution of adverse events will be done via the analysis of frequencies for treatment emergent Adverse Event (TEAEs), Serious Adverse Event (TESAEs) and Deaths due to AEs, through the monitoring of relevant clinical and laboratory safety parameters. Treatment emergent adverse events falling into the category of myelosuppression, renal toxicity or second malignancy will be recorded beyond 30 day safety observation period. | From randomization till 30 day safety follow-up, assessed up to 43 months (estimated final OS analysis). |
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