Prostate Cancer Clinical Trial
— FIRSTANAOfficial title:
Randomized, Open Label, Multi-Center Study Comparing Cabazitaxel at 25 mg/m^2 and at 20 mg/m^2 in Combination With Prednisone Every 3 Weeks to Docetaxel in Combination With Prednisone in Patients With Metastatic Castration Resistant Prostate Cancer Not Pretreated With Chemotherapy
| Verified date | May 2019 |
| Source | Sanofi |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
Primary Objective:
- To demonstrate the superiority of cabazitaxel plus prednisone at 25 mg/m^2 (Arm A) or 20
mg/m^2 (Arm B) versus docetaxel plus prednisone (Arm C) in term of overall survival (OS)
in participants with metastatic castration resistant prostate cancer (mCRPC) and not
previously treated with chemotherapy.
Secondary Objectives:
- To evaluate safety in the 3 treatment arms.
- To compare efficacy of cabazitaxel at 20 mg/m^2 and 25 mg/m^2 to docetaxel for:
- Progression Free Survival (PFS) (RECIST 1.1)
- Tumor progression free survival (RECIST 1.1)
- Tumor response in participants with measurable disease (RECIST 1.1),
- PSA response
- PSA-Progression free survival (PSA-PFS).
- Pain response in participants with stable pain at baseline
- Pain progression free survival
- Time to occurrence of any skeletal related events (SRE)
- To compare Health-Related Quality of Life (HRQL).
- To assess the pharmacokinetics and pharmacogenomics of cabazitaxel.
| Status | Completed |
| Enrollment | 1168 |
| Est. completion date | May 2018 |
| Est. primary completion date | September 2015 |
| Accepts healthy volunteers | No |
| Gender | Male |
| Age group | 18 Years and older |
| Eligibility |
Inclusion criteria : - I 01. Histologically- or cytologically-confirmed prostate adenocarcinoma. - I 02. Metastatic disease. - I 03. Progressive disease while receiving hormonal therapy or after surgical castration. - I 04. Effective castration (serum testosterone levels =0.50 ng/mL) by orchiectomy and/or luteinizing hormone-releasing hormone (LHRH) agonists or antagonist with or without anti-androgens. Exclusion criteria: - E 01. Prior chemotherapy for prostate cancer, - E 02. Less than 28 days elapsed from prior treatment with estramustine, radiotherapy or surgery to the time of randomization. Participants on biphosphonates prior to study entry. - E 03. Prior isotope therapy, whole pelvic radiotherapy, or radiotherapy to >30% of bone marrow. - E 04. Adverse events (excluding alopecia and those listed in the specific exclusion criteria) from any prior anticancer therapy of grade >1(National Cancer Institute Common Terminology Criteria [NCI CTCAE] v4.03) at the time of randomization. - E 05. Less than 18 years (or country's legal age of majority if the legal age is >18 years). - E 06. Eastern Cooperative Oncology Group (ECOG) performance status >2. - E 07. History of brain metastases, uncontrolled spinal cord compression, or carcinomatous meningitis or new evidence of brain or leptomeningeal disease. - E 08. Prior malignancy. - E 09. Participation in another clinical trial and any concurrent treatment with any investigational drug within 30 days prior to randomization. - E 10. Any of the following within 6 months prior to study enrollment: myocardial infarction, severe/unstable angina pectoris, coronary/peripheral artery bypass graft, New York Heart Association (NYHA) class III or IV congestive heart failure, stroke or transient ischemic attack. - E 11. Any of the following within 3 months prior to randomization: treatment resistant peptic ulcer disease, erosive esophagitis or gastritis, infectious or inflammatory bowel disease, diverticulitis, pulmonary embolism, or other uncontrolled thromboembolic event. - E 12. Acquired immunodeficiency syndrome (AIDS-related illnesses) or known HIV disease requiring antiretroviral treatment. - E 13. Any severe acute or chronic medical condition which could impair the ability of the participant to participate to the study or interfere with interpretation of study results, or participants unable to comply with the study procedures. - E 14. Absence of signed and dated Institutional Review Board (IRB)-approved participant informed consent form prior to enrollment into the study. - E 15. Participants with reproductive potential who did not agree to use accepted and effective method of contraception during the study treatment period. - E 16. History of hypersensitivity to docetaxel, or polysorbate 80. - E 17. Inadequate organ and bone marrow function - E 18. Contraindications to the use of corticosteroid treatment. - E 19. Symptomatic peripheral neuropathy grade >2 (National Cancer Institute Common Terminology Criteria [NCI CTCAE] v.4.03). The above information was not intended to contain all considerations relevant to a participant's potential participation in a clinical trial. |
| Country | Name | City | State |
|---|---|---|---|
| Australia | Investigational Site Number 036016 | Bankstown | |
| Australia | Investigational Site Number 036008 | Camperdown | |
| Australia | Investigational Site Number 036015 | Coffs Harbour | |
| Australia | Investigational Site Number 036001 | Concord | |
| Australia | Investigational Site Number 036017 | Fitzroy | |
| Australia | Investigational Site Number 036003 | Herston | |
| Australia | Investigational Site Number 036010 | Hornsby | |
| Australia | Investigational Site Number 036012 | Kurralta Park | |
| Australia | Investigational Site Number 036002 | Parkville | |
| Australia | Investigational Site Number 036009 | South Brisbane | |
| Australia | Investigational Site Number 036011 | Subiaco | |
| Australia | Investigational Site Number 036013 | Wodonga | |
| Belarus | Investigational Site Number 112001 | Minsk | |
| Belarus | Investigational Site Number 112002 | Minsk | |
| Belarus | Investigational Site Number 112004 | Vitebsk | |
| Brazil | Investigational Site Number 076006 | Passo Fundo | |
| Brazil | Investigational Site Number 076001 | Porto Alegre | |
| Brazil | Investigational Site Number 076002 | Porto Alegre | |
| Brazil | Investigational Site Number 076004 | Rio De Janeiro | |
| Brazil | Investigational Site Number 076009 | Sao Jose Do Rio Preto | |
| Brazil | Investigational Site Number 076005 | Sao Paulo | |
| Brazil | Investigational Site Number 076003 | Uberlandia | |
| Canada | Investigational Site Number 124002 | London | |
| Canada | Investigational Site Number 124007 | Mississauga | |
| Canada | Investigational Site Number 124005 | Moncton | |
| Canada | Investigational Site Number 124003 | Montreal | |
| Canada | Investigational Site Number 124004 | Quebec | |
| Canada | Investigational Site Number 124006 | Toronto | |
| China | Investigational Site Number 156005 | Beijing | |
| China | Investigational Site Number 156002 | Shanghai | |
| China | Investigational Site Number 156003 | Shanghai | |
| China | Investigational Site Number 156004 | Shanghai | |
| Czechia | Investigational Site Number 203002 | Brno | |
| Czechia | Investigational Site Number 203003 | Novy Jicin | |
| Czechia | Investigational Site Number 203001 | Olomouc | |
| Czechia | Investigational Site Number 203004 | Praha 2 | |
| Denmark | Investigational Site Number 208004 | Ålborg | |
| Denmark | Investigational Site Number 208002 | Herlev | |
| Denmark | Investigational Site Number 208001 | København Ø | |
| Denmark | Investigational Site Number 208003 | Odense C | |
| Finland | Investigational Site Number 246002 | Helsinki | |
| Finland | Investigational Site Number 246001 | Kuopio | |
| Finland | Investigational Site Number 246003 | Turku | |
| France | Investigational Site Number 250010 | Besancon Cedex | |
| France | Investigational Site Number 250002 | Bordeaux Cedex | |
| France | Investigational Site Number 250006 | Caen Cedex 05 | |
| France | Investigational Site Number 250005 | Lyon | |
| France | Investigational Site Number 250003 | Paris Cedex 05 | |
| France | Investigational Site Number 250004 | Paris Cedex 10 | |
| France | Investigational Site Number 250001 | Paris Cedex 15 | |
| France | Investigational Site Number 250007 | Poitiers Cedex | |
| France | Investigational Site Number 250008 | Suresnes | |
| France | Investigational Site Number 250009 | Villejuif | |
| Germany | Investigational Site Number 276003 | Aachen | |
| Germany | Investigational Site Number 276005 | Berlin | |
| Germany | Investigational Site Number 276001 | Düsseldorf | |
| Germany | Investigational Site Number 276004 | Erlangen | |
| Germany | Investigational Site Number 276002 | Homburg | |
| Germany | Investigational Site Number 276006 | München | |
| Israel | Investigational Site Number 376004 | Kfar Saba | |
| Israel | Investigational Site Number 376003 | Petah-Tikva | |
| Israel | Investigational Site Number 376002 | Tel Aviv | |
| Italy | Investigational Site Number 380001 | Arezzo | |
| Italy | Investigational Site Number 380004 | Bari | |
| Italy | Investigational Site Number 380003 | Orbassano | |
| Italy | Investigational Site Number 380005 | Roma | |
| Italy | Investigational Site Number 380002 | Trento | |
| Japan | Investigational Site Number 392001 | Bunkyo-Ku | |
| Japan | Investigational Site Number 392003 | Chiba-Shi | |
| Japan | Investigational Site Number 392006 | Kashiwa-Shi | |
| Japan | Investigational Site Number 392005 | Koto-Ku | |
| Japan | Investigational Site Number 392002 | Osaka Sayama-Shi | |
| Japan | Investigational Site Number 392004 | Osaka-Shi | |
| Mexico | Investigational Site Number 484007 | Acapulco | |
| Mexico | Investigational Site Number 484008 | Aguascalientes | |
| Mexico | Investigational Site Number 484003 | D.f. | |
| Mexico | Investigational Site Number 484004 | Guadalajara | |
| Mexico | Investigational Site Number 484009 | Merida | |
| Mexico | Investigational Site Number 484005 | Queretaro | |
| Mexico | Investigational Site Number 484002 | San Luis Potosi | |
| Mexico | Investigational Site Number 484006 | Zapopan | |
| Peru | Investigational Site Number 604001 | Lima | |
| Peru | Investigational Site Number 604002 | Lima | |
| Peru | Investigational Site Number 604005 | Lima | |
| Peru | Investigational Site Number 604006 | Lima | |
| Poland | Investigational Site Number 616002 | Bydgoszcz | |
| Poland | Investigational Site Number 616001 | Gdansk | |
| Poland | Investigational Site Number 616003 | Koscierzyna | |
| Poland | Investigational Site Number 616005 | Lodz | |
| Poland | Investigational Site Number 616004 | Poznan | |
| Portugal | Investigational Site Number 620003 | Coimbra | |
| Portugal | Investigational Site Number 620004 | Lisboa | |
| Portugal | Investigational Site Number 620005 | Lisboa | |
| Portugal | Investigational Site Number 620001 | Porto | |
| Portugal | Investigational Site Number 620002 | Porto | |
| Romania | Investigational Site Number 642004 | Baia Mare | |
| Romania | Investigational Site Number 642008 | Bucharest | |
| Romania | Investigational Site Number 642005 | Bucuresti | |
| Romania | Investigational Site Number 642002 | Cluj Napoca | |
| Romania | Investigational Site Number 642003 | Cluj Napoca | |
| Romania | Investigational Site Number 642007 | Hunedoara | |
| Russian Federation | Investigational Site Number 643004 | Ekaterinburg | |
| Russian Federation | Investigational Site Number 643008 | Moscow | |
| Russian Federation | Investigational Site Number 643003 | Omsk | |
| Russian Federation | Investigational Site Number 643002 | Pyatigorsk | |
| Russian Federation | Investigational Site Number 643007 | Ryazan | |
| Russian Federation | Investigational Site Number 643005 | St-Petersburg | |
| Russian Federation | Investigational Site Number 643001 | Tomsk | |
| Russian Federation | Investigational Site Number 643006 | Yaroslavl | |
| Spain | Investigational Site Number 724001 | Barcelona | |
| Spain | Investigational Site Number 724002 | Barcelona | |
| Spain | Investigational Site Number 724007 | Barcelona | |
| Spain | Investigational Site Number 724003 | Hospitalet De Llobregat | |
| Spain | Investigational Site Number 724004 | Madrid | |
| Spain | Investigational Site Number 724005 | Madrid | |
| Spain | Investigational Site Number 724006 | Santiago De Compostela | |
| Sweden | Investigational Site Number 752003 | Malmö | |
| Sweden | Investigational Site Number 752002 | Stockholm | |
| Sweden | Investigational Site Number 752001 | Uppsala | |
| Taiwan | Investigational Site Number 158004 | Kaohsiung | |
| Taiwan | Investigational Site Number 158002 | Taichung | |
| Taiwan | Investigational Site Number 158001 | Taipei | |
| Taiwan | Investigational Site Number 158003 | Tao-Yuan | |
| Turkey | Investigational Site Number 792002 | Ankara | |
| Turkey | Investigational Site Number 792001 | Istanbul | |
| Ukraine | Investigational Site Number 804009 | Cherkasy | |
| Ukraine | Investigational Site Number 804004 | Dnipropetrovsk | |
| Ukraine | Investigational Site Number 804010 | Donetsk | |
| Ukraine | Investigational Site Number 804006 | Ivano-Frankivsk | |
| Ukraine | Investigational Site Number 804003 | Kharkov | |
| Ukraine | Investigational Site Number 804001 | Kyiv | |
| Ukraine | Investigational Site Number 804002 | Kyiv | |
| Ukraine | Investigational Site Number 804007 | Lutsk | |
| Ukraine | Investigational Site Number 804005 | Uzhgorod | |
| Ukraine | Investigational Site Number 804008 | Zaporizhzhya | |
| United States | Investigational Site Number 840026 | Akron | Ohio |
| United States | Investigational Site Number 840033 | Albuquerque | New Mexico |
| United States | Investigational Site Number 840009 | Anaheim | California |
| United States | Investigational Site Number 840014 | Bakersfield | California |
| United States | Investigational Site Number 840013 | Boca Raton | Florida |
| United States | Investigational Site Number 840138 | Boston | Massachusetts |
| United States | Investigational Site Number 840238 | Boston | Massachusetts |
| United States | Investigational Site Number 840038 | Brookline | Massachusetts |
| United States | Investigational Site Number 840028 | Chattanooga | Tennessee |
| United States | Investigational Site Number 840023 | Cleveland | Ohio |
| United States | Investigational Site Number 840015 | Decatur | Illinois |
| United States | Investigational Site Number 840019 | Denver | Colorado |
| United States | Investigational Site Number 840005 | Detroit | Michigan |
| United States | Investigational Site Number 840032 | Dunmore | Pennsylvania |
| United States | Investigational Site Number 840017 | East Orange | New Jersey |
| United States | Investigational Site Number 840035 | Jacksonville | Florida |
| United States | Investigational Site Number 840016 | Kansas City | Missouri |
| United States | Investigational Site Number 840020 | Lincoln | Nebraska |
| United States | Investigational Site Number 840004 | Muscle Shoals | Alabama |
| United States | Investigational Site Number 840037 | Myrtle Beach | South Carolina |
| United States | Investigational Site Number 840008 | New Orleans | Louisiana |
| United States | Investigational Site Number 840010 | Paducah | Kentucky |
| United States | Investigational Site Number 840007 | Pawtucket | Rhode Island |
| United States | Investigational Site Number 840001 | Port Saint Lucie | Florida |
| United States | Investigational Site Number 840036 | Raleigh | North Carolina |
| United States | Investigational Site Number 840006 | Rockville | Maryland |
| United States | Investigational Site Number 840030 | Sacramento | California |
| United States | Investigational Site Number 840021 | Saint Louis Park | Minnesota |
| United States | Investigational Site Number 840003 | San Bernardino | California |
| United States | Investigational Site Number 840012 | San Francisco | California |
| United States | Investigational Site Number 840011 | Washington | North Carolina |
| United States | Investigational Site Number 840018 | Wichita | Kansas |
| Lead Sponsor | Collaborator |
|---|---|
| Sanofi |
United States, Australia, Belarus, Brazil, Canada, China, Czechia, Denmark, Finland, France, Germany, Israel, Italy, Japan, Mexico, Peru, Poland, Portugal, Romania, Russian Federation, Spain, Sweden, Taiwan, Turkey, Ukraine,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Overall Survival (OS) | OS was defined as the time interval from the date of randomization to the date of death due to any cause. In the absence of confirmation of death, survival time was censored at the last date participant was known to be alive, or at the cut-off date if the participant's last contact was after the cut-off date. The study cut-off date for the final analysis of OS was the date when the 774th death had been observed. Analysis was performed by Kaplan-Meier method. | Baseline up to death or study cut-off date, whichever was earlier (maximum duration: 51 months ) | |
| Secondary | Progression Free Survival (PFS) | PFS: time interval between date of randomization to date of first occurrence of any of following events: tumor progression according to Response Evaluation Criteria In Solid Tumors (RECIST) version 1.1; Prostate Specific Antigen (PSA) progression; pain progression or death due to any cause. Analysis was performed by Kaplan-Meier method. | Baseline up to tumor progression, PSA progression, pain progression or death (maximum duration: 51 months) | |
| Secondary | Time to Tumor Progression Free Survival | Time to tumor progression free survival was defined as the time interval between randomization and the date of first occurrence of tumor progression (assessed using RECIST version 1.1) or death, whichever was earlier. Analysis was performed by Kaplan-Meier method. | Baseline up to tumor progression or death due to any cause or study cut-off date, whichever was earlier (maximum duration: 51 months) | |
| Secondary | Percentage of Participants With Overall Objective Tumor Response | Overall objective tumor response was defined as having a partial response (PR) or complete response (CR) according to the RECIST version 1.1. CR was defined as disappearance of all target and non-target lesions and normalization of tumor marker level. Any pathological lymph nodes (whether target or non-target) must have reduction in short axis to <10 mm. PR was defined as at least a 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters. | Baseline up to DP or death due to any cause or study cut-off date, whichever was earlier (maximum duration: 51 months) | |
| Secondary | Time to Prostate Serum Antigen Progression Free Survival (PSA-PFS) | Time to PSA-PFS: time interval between date of randomization & first occurrence of PSA progression/ death, whichever was earlier. PSA progression:1) In PSA responders(=50% decline from baseline PSA of =10 ng/mL):increase of =25%(at least 2 ng/mL)over nadir value, confirmed by second PSA value at least 3 weeks later;2)In PSA non-responders(not achieved =50% decline from baseline PSA =10 ng/mL):increase of =25% (at least 2 ng/mL) over baseline value, confirmed by second PSA value at least 3 weeks later;3)In participants not eligible for PSA response(baseline PSA <10 ng/mL):(a)in participants with baseline PSA>0 ng/mL&<10 ng/mL: increase in PSA by 25% (at least 2 ng/mL) above baseline level, confirmed by second PSA value at least 3weeks apart;(b)in participants with baseline value=0ng/mL: a post baseline PSA value =2ng/mL.Early rise in PSA only indicated progression if it was associated with another sign of DP or if it continued beyond 12 weeks. Analysis performed by Kaplan-Meier method. | Baseline up to PSA progression or death due to any cause or study cut-off date, whichever was earlier (maximum duration: 51 months) | |
| Secondary | Percentage of Participants With PSA Response | PSA response was defined as =50% decrease from baseline in serum PSA levels, confirmed by a second PSA value at least 3 weeks later in participants with baseline PSA value =10 ng/mL. | Baseline up to PSA progression or death due to any cause or study cut-off date, whichever was earlier (maximum duration: 51 months) | |
| Secondary | Time to Pain Progression Free Survival (Pain PFS) | Time to pain PFS was defined as the time interval between date of randomization and the date of the first occurrence of pain progression or death, whichever was earlier. Pain progression was defined as an increase of =1 point in the median present pain intensity (PPI) score from the nadir confirmed by a second assessment at least 3 weeks later or =25 % increase in the mean analgesic score from baseline, due to cancer related pain confirmed by a second assessment at least 3 weeks later or requirement for local palliative radiotherapy. PPI was rated by participant in a diary using a scale of 0=no pain, 1=mild, 2=discomforting, 3=distressing, 4=horrible 5=excruciating. Analgesic use was recorded by the participant in a diary. Analgesic score was calculated from the analgesic use data based on a table of analgesic medications, with non-narcotic medications assigned a value of 1 point and narcotic medications assigned a value of 4 points. Analysis was performed by Kaplan-Meier method. | Baseline until disease progression, death or study cut-off date (maximum duration: 51 months) | |
| Secondary | Percentage of Participants With Pain Response | Pain response was defined as either a =2-point decrease from baseline median PPI score without increase in analgesic score, or a =50% decrease in analgesic use from baseline mean analgesic score (only in participants with baseline mean analgesic score=10) without increase in the pain. Either criterion was maintained for 2 consecutive evaluations at least 3 weeks apart. PPI was rated by participant in a diary using a scale of 0=no pain, 1=mild, 2=discomforting, 3=distressing, 4=horrible 5=excruciating. Analgesic use was recorded by the participant in a diary. Analgesic score was calculated from the analgesic use data based on a table of analgesic medications, with non-narcotic medications assigned a value of 1 point and narcotic medications assigned a value of 4 points. | Baseline until pain progression, death or study cut-off date (maximum duration: 51 months) | |
| Secondary | Skeletal Related Events (SRE) Free Survival | SRE free survival was defined as the time interval between the date of randomization and the date of the occurrence of the first event defining a SRE or death due to any cause, whichever was earlier. SRE were assessed by clinical evaluation. Occurrence of SRE was defined as: pathological fracture(s) and/or spinal cord compression; need for bone irradiation, including radioisotopes or bone surgery; and change of antineoplastic therapy (including introduction of bisphosphonates or denosumab in the setting of increased pain) to treat bone pain. Analysis was performed by Kaplan-Meier method. | Baseline until occurrence of first SRE or death (maximum duration: 51 months) | |
| Secondary | Change From Baseline in Functional Assessment of Cancer Therapy-Prostate (FACT-P) Total Score as a Measure of Health Related Quality of Life (HRQoL) | FACT-P was a 39-item participant rated questionnaire that measures the concerns of participants with prostate cancer. It consisted of 5 sub-scales assessing physical well-being (7 items), social/family well-being (7 items), emotional well-being (6 items), functional well-being (7 items), and prostate-specific concerns (12 items). FACT-P total score was the sum of all 5 subscale scores. It ranged from 0 to156 with higher score indicated better quality of life with fewer symptoms. | Baseline, Day 1 of each cycle 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16 (each cycle 21-day); post-treatment follow up 1, 2, 3, 4, 5, 6 (each up to 12 weeks) | |
| Secondary | Change From Baseline in Functional Assessment of Cancer Therapy-Prostate (FACT-P):Trial Outcome Index (TOI) as a Measure of HRQoL | FACT-P was a 39-item participant rated questionnaire that measures the concerns of participants with prostate cancer. It consisted of 5 sub-scales assessing physical well-being (7 items), social/family well-being (7 items), emotional well-being (6 items), functional well-being (7 items), and prostate-specific concerns (12 items). Physical well being, functional well being, and prostate-specific concerns sub-scales of the FACT-P questionnaire were combined to calculate TOI. Total TOI score ranges from 0 to 104, with higher scores representing a better quality of life with fewer symptoms. | Baseline, Day 1 of each cycle 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16 (each cycle 21-day); post-treatment follow up 1, 2, 3, 4, 5, 6 (each up to 12 weeks) |
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