Enfortumab Vedotin and Pembrolizumab vs. Chemotherapy Alone in Untreated Locally Advanced or Metastatic Urothelial Cancer
- Conditions
- Urothelial Cancer
- Interventions
- Registration Number
- NCT04223856
- Lead Sponsor
- Astellas Pharma Global Development, Inc.
- Brief Summary
This study is being done to see how well two drugs (enfortumab vedotin and pembrolizumab) work together to treat patients with urothelial cancer. The study will compare these drugs to other drugs that are usually used to treat this cancer (standard of care). The patients in this study will have cancer that has spread from their urinary system to other parts of their body.
- Detailed Description
Japan PMDA has approved enfortumab vedotin (Padcev) for the treatment of advanced urothelial cancer. The study will continue as a post marketing study in Japan.
This study is being conducted to evaluate the combination of enfortumab vedotin + pembrolizumab versus standard of care gemcitabine + platinum-containing chemotherapy, in subjects with previously untreated locally advanced or metastatic urothelial cancer.
Enfortumab vedotin may be administered for an unlimited number of cycles until a protocol defined reason for study discontinuation occurs. Pembrolizumab may be administered for a maximum of 35 cycles or a protocol-defined reason for study discontinuation occurs, whichever is first. Cisplatin or carboplatin plus gemcitabine may be administered for a maximum of 6 cycles or a protocol-defined reason for study discontinuation occurs, whichever is first.
Recruitment & Eligibility
- Status
- ACTIVE_NOT_RECRUITING
- Sex
- All
- Target Recruitment
- 1030
-
Histologically documented, unresectable locally advanced or metastatic urothelial carcinoma
-
Measurable disease by investigator assessment according to RECIST v1.1
- Participants with prior definitive radiation therapy must have measurable disease per RECIST v1.1 that is outside the radiation field or has demonstrated unequivocal progression since completion of radiation therapy
-
Participants must not have received prior systemic therapy for locally advanced or metastatic urothelial carcinoma with the following exceptions:
- Participants that received neoadjuvant chemotherapy with recurrence >12 months from completion of therapy are permitted
- Participants that received adjuvant chemotherapy following cystectomy with recurrence >12 months from completion of therapy are permitted
-
Must be considered eligible to receive cisplatin- or carboplatin-containing chemotherapy, in the investigator's judgment
-
Archival tumor tissue comprising muscle-invasive urothelial carcinoma or a biopsy of metastatic urothelial carcinoma must be provided for PD-L1 testing prior to randomization
-
Eastern Cooperative Oncology Group (ECOG) Performance Status score of 0, 1, or 2
-
Adequate hematologic and organ function
- Previously received enfortumab vedotin or other monomethyl auristatin E (MMAE)-based antibody-drug conjugate (ADCs)
- Received prior treatment with a programmed cell death ligand-1 (PD-(L)-1) inhibitor for any malignancy, including earlier stage urothelial cancer (UC), defined as a PD-1 inhibitor or PD-L1 inhibitor
- Received prior treatment with an agent directed to another stimulatory or co inhibitory T-cell receptor
- Received anti-cancer treatment with chemotherapy, biologics, or investigational agents not otherwise prohibited by exclusion criterion 1-3 that is not completed 4 weeks prior to first dose of study treatment
- Uncontrolled diabetes
- Estimated life expectancy of less than 12 weeks
- Active central nervous system (CNS) metastases
- Ongoing clinically significant toxicity associated with prior treatment that has not resolved to ≤ Grade 1 or returned to baseline
- Currently receiving systemic antimicrobial treatment for active infection (viral, bacterial, or fungal) at the time of randomization. Routine antimicrobial prophylaxis is permitted.
- Known active hepatitis B, active hepatitis C, or human immunodeficiency virus (HIV) infection.
- History of another invasive malignancy within 3 years before the first dose of study drug, or any evidence of residual disease from a previously diagnosed malignancy
- Documented history of a cerebral vascular event (stroke or transient ischemic attack), unstable angina, myocardial infarction, or cardiac symptoms consistent with New York Heart Association (NYHA) Class IV within 6 months prior to randomization
- Receipt of radiotherapy within 2 weeks prior to randomization
- Received major surgery (defined as requiring general anesthesia and >24 hour inpatient hospitalization) within 4 weeks prior to randomization
- Known severe (≥ Grade 3) hypersensitivity to any enfortumab vedotin excipient contained in the drug formulation of enfortumab vedotin
- Active keratitis or corneal ulcerations
- History of autoimmune disease that has required systemic treatment in the past 2 years
- History of idiopathic pulmonary fibrosis, organizing pneumonia, drug induced pneumonitis, idiopathic pneumonitis, or evidence of active pneumonitis on screening chest computed tomography (CT) scan
- Prior allogeneic stem cell or solid organ transplant
- Received a live attenuated vaccine within 30 days prior to randomization
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- PARALLEL
- Arm && Interventions
Group Intervention Description Arm A Enfortumab vedotin Enfortumab vedotin + pembrolizumab Arm A Pembrolizumab Enfortumab vedotin + pembrolizumab Arm B Carboplatin Gemcitabine + cisplatin or carboplatin Arm B Gemcitabine Gemcitabine + cisplatin or carboplatin Arm B Cisplatin Gemcitabine + cisplatin or carboplatin
- Primary Outcome Measures
Name Time Method Progression-Free Survival (PFS) Per Response Evaluation Criteria in Solid Tumors (RECIST) Version (v) 1.1 by Blinded Independent Central Review (BICR) From the date of randomization to first documentation of PD or death due to any cause, whichever occurred first (maximum exposure to treatment was up to 39.2 months) PFS was defined as the time from date of randomization to first documentation of disease progression (PD), or to death due to any cause, whichever occurred first. PD: at least a 20 percent (%) increase in the sum of diameters of target lesions, taking as reference the smallest sum on study. In addition to the relative increase of 20%, the sum must also demonstrate an absolute increase of at least 5 millimeter (mm). PD could also be unequivocal progression of non-target lesions or the presence of unequivocal new lesions. Kaplan-Meier method was used for analysis.
Overall Survival (OS) From randomization to date of death due to any cause or censoring date, whichever occurred first (maximum exposure to treatment was up to 39.2 months) OS was defined as the time from the date of randomization to the date of death from any cause. In the absence of death, OS was censored at the date the participant was last known to be alive. Kaplan-Meier method was used for analysis.
- Secondary Outcome Measures
Name Time Method Percentage of Participants With Objective Response Rate (ORR) Per RECIST v1.1 by BICR From first dose till CR/PR or PD or death, whichever occurred first (maximum up to approximately 7.4 years) ORR as per RECIST v1.1 by BICR was defined as the percentage of participants with confirmed complete response (CR) or partial response (PR) CR was defined as disappearance of all lesions including non-target lesions (not just target lesions). Any pathological lymph nodes must have reduction in short axis to\<10 mm. PR was defined as at least 30 percent \[%\] decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters. For a response to be considered as confirmed, the subsequent response needs to be at least 4 weeks after the initial response.
Time to Pain Progression (TTPP) From the date of randomization to date of pain progression (maximum up to approximately 7.4 years) TTPP was defined as the time from the date of randomization to date of pain progression. Pain progression was defined as a participant reporting either of the following, whichever came first: 1) Increase of 2 or more points from baseline on Brief Pain Inventory - Short Form (BPI-SF) Question 3 (i.e., pain at its worst in the last 24 hours, score range 0 to 10 with higher scores associated with higher pain levels) maintained for at least two consecutive assessments. 2) Initiation of new opioid medication from baseline for pain with usage maintained for at least two consecutive assessments as recorded in BPI-SF Question 7 (i.e., What medications received for pain).
Change From Baseline in Worst Pain Using BPI-SF at Week 26 Baseline, Week 26 Brief Pain Inventory (BPI-SF) was defined as summary of the worst, least, and average pain experienced in the last 24 hours as well as pain right now and number of pain locations were provided for each treatment arm. BPI-sf worst pain measured the severity of pain based on the pain at its worst in the last 24 hours, score range 0 to 10 with higher scores associated with higher pain levels.
PFS Per RECIST v1.1 by Investigator Assessment From the date of randomization to first documentation of PD or death due to any cause, whichever occurred first (maximum up to approximately 7.4 years) PFS as per RECIST v1.1 by investigator was defined as the time from date of randomization to first documentation of PD, or to death due to any cause, whichever comes first. PD: at least a 20% increase in the sum of diameters of target lesions, taking as reference the smallest sum on study. In addition to the relative increase of 20%, the sum must also demonstrate an absolute increase of at least 5 mm. PD could also be unequivocal progression of non-target lesions or the presence of unequivocal new lesions.
ORR Per RECIST v1.1 by Investigator Assessment From first dose till CR/PR or PD or death, whichever occurred first (maximum up to approximately 7.4 years) ORR as per RECIST v1.1 by investigator was defined as the percentage of participants with confirmed CR or PR. CR was defined as disappearance of all lesions including non-target lesions (not just target lesions). Any pathological lymph nodes must have reduction in short axis to\<10 mm. PR was defined as at least 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters. For a response to be considered as confirmed, the subsequent response needs to be at least 4 weeks after the initial response.
Duration of Response (DOR) Per RECIST v1.1 by BICR From the date of first documented response of CR or PR to the first documented disease progression or to death from any cause, whichever occurred first (maximum up to approximately 7.4 years) DOR was defined as the time from the first objective response (CR or PR that is subsequently confirmed) to the first documented PD per RECIST v1.1 per BICR or death from any cause, whichever occurs first. DOR will only include subjects with a confirmed response (CR or PR per RECIST v1.1). CR was defined as disappearance of all target lesions. Any pathological lymph nodes must have reduction in short axis to\<10 mm. PR was defined as at least 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters. For a response to be considered as confirmed, the subsequent response needs to be at least 4 weeks after the initial response. PD: at least a 20% increase in the sum of diameters of target lesions, taking as reference the smallest sum on study. In addition to the relative increase of 20%, the sum must also demonstrate an absolute increase of at least 5 mm.
DOR Per RECIST v1.1 by Investigator Assessment From the date of first documented response of CR or PR to the first documented disease progression or to death from any cause, whichever occurred first (maximum up to approximately 7.4 years) DOR was defined as the time from the first objective response (CR or PR that is subsequently confirmed) to the first documented PD per RECIST v1.1 per investigator or death from any cause, whichever occurs first. DOR will only include subjects with a confirmed response (CR or PR per RECIST v1.1). CR was defined as disappearance of all target lesions. Any pathological lymph nodes must have reduction in short axis to\<10 mm. PR was defined as at least 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters. PD: at least a 20% increase in the sum of diameters of target lesions, taking as reference the smallest sum on study. In addition to the relative increase of 20%, the sum must also demonstrate an absolute increase of at least 5 mm. For a response to be considered as confirmed, the subsequent response needs to be at least 4 weeks after the initial response.
Disease Control Rate (DCR) Per RECIST v1.1 by BICR From the date of randomization to the date of PD or death from any cause or censoring date, whichever occurred first (maximum up to approximately 7.4 years) DCR by BICR was defined as the percentage of participants with confirmed response (CR or PR), or SD (or non-CR/non-PD), per RECIST v1.1. Subjects who have no post-baseline response assessments will be considered as non-responders for calculating the DCR. Only response assessments before the first documented PD or subsequent anticancer therapies were considered. CR was defined as disappearance of all target lesions. Any pathological lymph nodes must have reduction in short axis to\<10 mm. PR was defined as at least 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters. For a response to be considered as confirmed, the subsequent response needs to be at least 4 weeks after the initial response. SD was defined as a change in tumor size that is neither radiological response (\>30% shrinkage) nor progression (\>20% growth).
DCR Per RECIST v1.1 by Investigator Assessment From the date of randomization to the date of PD or death from any cause or censoring date, whichever occurred first (maximum up to approximately 7.4 years) DCR by BICR was defined as the percentage of participants with confirmed response (CR or PR), or SD (or non-CR/non-PD), per RECIST v1.1. Subjects who have no post-baseline response assessments will be considered as non-responders for calculating the DCR. Only response assessments before the first documented PD or subsequent anticancer therapies were considered. CR was defined as disappearance of all target lesions. Any pathological lymph nodes must have reduction in short axis to\<10 mm. PR was defined as at least 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters. For a response to be considered as confirmed, the subsequent response needs to be at least 4 weeks after the initial response. SD was defined as a change in tumor size that is neither radiological response (\>30% shrinkage) nor progression (\>20% growth).
Mean Scores in Patient Reported Outcome (PRO) Assessment Measured by the EuroQOL Five Dimensions Questionnaire 5L (EQ-5D-5L) End of study (approximately up to 7.4 years) The EQ-5D-5L is a 5-item self-reported measure of functioning and well-being, which assesses 5 dimensions of health, including mobility, self-care, usual activities, pain/discomfort, and anxiety/depression (EQ-5D-5L User Guide, 2019). Each dimension comprises 5 levels (no problems, slight problems, moderate problems, severe problems, and extreme problems).
Change From Baseline in PRO Assessment Measured by the EQ-5D-5L Baseline, End of study (approximately up to 7.4 years) The EQ-5D-5L is a 5-item self-reported measure of functioning and well-being, which assesses 5 dimensions of health, including mobility, self-care, usual activities, pain/discomfort, and anxiety/depression (EQ-5D-5L User Guide, 2019). Each dimension comprises 5 levels (no problems, slight problems, moderate problems, severe problems, and extreme problems).
Mean Scores in PRO Assessment Measured by European Organisation for Research and Treatment of Cancer (EORTC) Quality of Life Questionnaire Core 30 (QLQ-C30) End of study (approximately up to 7.4 years) EORTC QLQ-C30: included functional scales (physical, role, cognitive, emotional, and social), global health status (GHS), symptom scales (fatigue, pain, nausea/vomiting), and single items (dyspnoea, appetite loss, insomnia, constipation/diarrhea, and financial difficulties). Most questions used 4- point scale (1 'Not at All' to 4 'Very Much'); 2 questions used 7-point scale (1 'Very Poor' to 7 'Excellent'). Scores averaged, transformed to 0- 100 scale; higher score=better level of functioning or greater degree of symptoms.
Change From Baseline in PRO Assessment Measured by EORTC QLQ-C30 Baseline, End of study (approximately up to 7.4 years) EORTC QLQ-C30: included functional scales (physical, role, cognitive, emotional, and social), global health status (GHS), symptom scales (fatigue, pain, nausea/vomiting), and single items (dyspnoea, appetite loss, insomnia, constipation/diarrhea, and financial difficulties). Most questions used 4- point scale (1 'Not at All' to 4 'Very Much'); 2 questions used 7-point scale (1 'Very Poor' to 7 'Excellent'). Scores averaged, transformed to 0- 100 scale; higher score=better level of functioning or greater degree of symptoms. Change from baseline=Cycle/Day score minus baseline score.
Number of Participants With Treatment Emergent Adverse Events Adverse Events (AEs) From start of treatment up to 37 days after last dose of study drug (approximately up to 7.4 years) An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. Treatment-emergent are events between first dose of study drug and up to 37 days after last dose that were absent before treatment or that worsened relative to pretreatment state.
Number of Participants With Serious TEAE From start of treatment up to 37 days after last dose of study drug (approximately up to 7.4 years) SAE was an AE resulting in any of the following outcomes or deemed significant for any other reason: death; initial or prolonged inpatient hospitalization; life-threatening experience (immediate risk of dying); persistent or significant disability/ incapacity; congenital anomaly. Treatment-emergent are events between first dose of study drug and up to 37 days after last dose that were absent before treatment or that worsened relative to pretreatment state.
Number of Participants With Grade 3-5 TEAE From start of treatment up to 37 days after last dose of study drug (approximately up to 7.4 years) AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. As per common terminology criteria for adverse events (CTCAE) version 4, Grade 3= severe AE; Grade 4= life-threatening or disabling AE; Grade 5= death related to an AE.
Number of Participants Related to Treatment AEs From start of treatment up to 37 days after last dose of study drug (approximately up to 7.4 years) An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. Treatment relatedness was assessed by the investigator.
Number of Participants With Laboratory Abnormalities From start of treatment up to 37 days after last dose of study drug (approximately up to 7.4 years) Laboratory abnormalities included Hematology and Serum Chemistry. In Hematology (increased : hemoglobin, lymphocytes, leukocytes, and decreased : hemoglobin, lymphocytes, neutrophils, platelets and leukocytes) and In serum chemistry (increased in : alkaline phosphatase, alanine aminotransferase, aspartate aminotransferase, bilirubin, calcium corrected for albumin, creatinine, glucose (non-fasting), potassium, sodium, and decreased in albumin, calcium corrected for albumin, glucose (non-fasting), potassium, phosphate and sodium).
Number of Participants With Treatment Discontinuation Rate Due to AEs During study (approximately up to 7.4 years)
Trial Locations
- Locations (260)
Hillman Cancer Center / University of Pittsburgh Medical Center
🇺🇸Pittsburgh, Pennsylvania, United States
Site JP81006
🇯🇵Kawasaki-shi, Japan
Site CN86025
🇨🇳Hefei, China
Site CN86030
🇨🇳Xicheng District, China
Site CN86026
🇨🇳Xuzhou, China
Site JP81017
🇯🇵Kyoto, Japan
Site CN86004
🇨🇳Beijing, China
Louisiana State University/ East Jefferson General Hospital
🇺🇸Metairie, Louisiana, United States
UT Health East Texas Hope Cancer Center
🇺🇸Tyler, Texas, United States
Site AR54008
🇦🇷Buenos Aire, Argentina
Site AR54001
🇦🇷Rosario, Argentina
Site AR54002
🇦🇷San Miguel, Argentina
Site AR54012
🇦🇷Tucuman, Argentina
Site AU61003
🇦🇺Box Hill, Australia
Site AUS61001
🇦🇺Douglas, Australia
Site AUS61004
🇦🇺Heidelberg, Australia
Site AUS61002
🇦🇺Macquarie Park, Australia
Site AUS61006
🇦🇺South Australia, Australia
Site BE32003
🇧🇪Brussels, Belgium
Site AU61005
🇦🇺South Brisbane, Australia
Site BE32007
🇧🇪Lueven, Belgium
Site CA11004
🇨🇦Calgary, Alberta, Canada
Site CA11003
🇨🇦Edmonton, Alberta, Canada
Site CA11006
🇨🇦Vancouver, British Columbia, Canada
Site CA11005
🇨🇦Toronto, Ontario, Canada
Site CA11001
🇨🇦Montreal, Quebec, Canada
Site CA11008
🇨🇦Quebec, Canada
Site CN86001
🇨🇳Beijing, China
Site CN86009
🇨🇳Beijing City, China
Site CN86015
🇨🇳Bengbu, China
Site CN86005
🇨🇳Beijing, China
Site CN86003
🇨🇳Changchun, China
Site CN86006
🇨🇳Changsha, China
Site CN86016
🇨🇳Changsha, China
Site CN86010
🇨🇳Chengdu, China
Site CN86007
🇨🇳Chongqing, China
Site CN86024
🇨🇳Chongqing, China
Site CN86002
🇨🇳Guangzhou, China
Site CN86020
🇨🇳Gunagzhou, China
Site CN86028
🇨🇳Fuzhou, China
Site CN86018
🇨🇳Hangzhou, China
Site CN86013
🇨🇳Hangzhou, China
Site CN86022
🇨🇳Hangzhou, China
Site CN86027
🇨🇳Jinan, China
Site CN86017
🇨🇳Nanjing, China
Site CN86021
🇨🇳Ningbo, China
Site CN86012
🇨🇳Nanjing, China
Site CN86011
🇨🇳Shenyang City, China
Site CN86014
🇨🇳Shanghai, China
Site CN86023
🇨🇳Tianjin, China
Site CN86019
🇨🇳Tianjin, China
Site CN86029
🇨🇳Wenzhou, China
Site CN86008
🇨🇳Wuhan City, China
Site CZ42006
🇨🇿Brno, Czechia
Site CZ42001
🇨🇿Hradec Kralove, Czechia
Site FR33003
🇫🇷Nice Cedex 2, France
Site DK45003
🇩🇰Aarhus N, Denmark
Site CZ42004
🇨🇿Olomouc, Czechia
Site CZ42005
🇨🇿Praha 4-Krc, Czechia
Site FR33020
🇫🇷Pierre-Bénite, France
Site FR33013
🇫🇷Strasbourg, France
Site FR33017
🇫🇷TOURS Cedex 09, France
Site DE49003
🇩🇪Berlin, Germany
Site DE49013
🇩🇪Bielefeld, Germany
Site DE49016
🇩🇪Düsseldorf, Germany
Site DE49011
🇩🇪Essen, Germany
Site DE49007
🇩🇪Frankfurt am Main, Germany
Site DE49009
🇩🇪Herne, Germany
Site DE49015
🇩🇪Gottingen, Germany
Site DE49005
🇩🇪Heidelberg, Germany
Site DE49010
🇩🇪Ulm, Germany
Site DE49006
🇩🇪Jena, Germany
Site DE49004
🇩🇪Tübingen, Germany
Site DE49002
🇩🇪Munchen, Germany
Site HU36001
🇭🇺Nyiregyhaza, Hungary
Site HU36006
🇭🇺Debrecen, Hungary
Site HU36005
🇭🇺Szolnok, Hungary
Site IL97203
🇮🇱Beer Sheva, Israel
Site IL97201
🇮🇱Haifa, Israel
Site IL97206
🇮🇱Jerusalem, Israel
Site IL97210
🇮🇱Tel Aviv, Israel
Site IL97204
🇮🇱Tel Hashomer, Israel
Site IT39009
🇮🇹Cremona, Italy
Site IL97205
🇮🇱Zerifin, Israel
Site IT39006
🇮🇹Genova, Italy
Site IT39007
🇮🇹Milano, Italy
Site IT39014
🇮🇹Milano, Italy
Site JP81011
🇯🇵Hirosaki, Japan
Site JP81005
🇯🇵Okayama, Japan
Site JP81008
🇯🇵Osaka, Japan
Site JP81007
🇯🇵Sapporo, Japan
Site JP81014
🇯🇵Tokushima, Japan
Site JP81003
🇯🇵Toyama, Japan
Site KR82001
🇰🇷Daejeon, Korea, Republic of
Site NL31005
🇳🇱Amsterdam, Noord-Holland, Netherlands
Site NL31004
🇳🇱Nieuwegein, Netherlands
Site RU70016
🇷🇺Arkhangelsk, Russian Federation
Site RU70013
🇷🇺Barnaul, Russian Federation
Site RU70020
🇷🇺Ivanovo, Russian Federation
Site RU70006
🇷🇺Leningradskaya Oblast', Russian Federation
Site RU70003
🇷🇺Moscow, Russian Federation
Site RU70011
🇷🇺Moscow, Russian Federation
Site RU70009
🇷🇺Saransk, Russian Federation
Site RU70008
🇷🇺St. Petersburg, Russian Federation
Site RU70015
🇷🇺Tyumen, Russian Federation
Site RU70005
🇷🇺Ufa, Russian Federation
Site ES34017
🇪🇸Barcelona, Spain
Site ES34006
🇪🇸Barcelona, Spain
Site ES34010
🇪🇸Barcelona, Spain
Site ES34001
🇪🇸Barcelona, Spain
Site ES34008
🇪🇸Barcelona, Spain
Site ES34013
🇪🇸Cordoba, Spain
Site ES34003
🇪🇸Madrid, Spain
Site ES34018
🇪🇸Madrid, Spain
Site ES34002
🇪🇸Madrid, Spain
Site ES34021
🇪🇸Lugo, Spain
Site ES34015
🇪🇸Madrid, Spain
Site ES34004
🇪🇸Manresa, Spain
Site ES34020
🇪🇸Pamplona, Spain
Site ES34012
🇪🇸Santander, Spain
Site ES34016
🇪🇸Sabadell, Spain
Site ES34007
🇪🇸Sevilla, Spain
Site ES34009
🇪🇸Valencia, Spain
Site ES34019
🇪🇸Valencia, Spain
Site CH41004
🇨🇭Basel, Switzerland
Site CH41002
🇨🇭Bern, Switzerland
Site CH41003
🇨🇭Winterthur, Switzerland
Site TW88604
🇨🇳Tainan, Taiwan
Site TW88602
🇨🇳Kweishan, Taiwan
Site TW88601
🇨🇳Taipei, Taiwan
Site TH66004
🇹🇭Bangkok, Thailand
Site TH66003
🇹🇭Bangkok, Thailand
Site TH66001
🇹🇭Ratchathewi, Thailand
Site TR90007
🇹🇷Ankara, Turkey
Site TR90009
🇹🇷Ankara, Turkey
Site TR90005
🇹🇷Antalya, Turkey
Site TR90004
🇹🇷Edirne, Turkey
Site TR90002
🇹🇷Istanbul, Turkey
Site TR90001
🇹🇷Konya, Turkey
Site TR90006
🇹🇷Malatya, Turkey
Site UK44005
🇬🇧Glasgow, United Kingdom
Site UK44009
🇬🇧London, United Kingdom
Site UK44001
🇬🇧London, United Kingdom
Site UK44006
🇬🇧Oxford, United Kingdom
Site UK44010
🇬🇧Plymouth, United Kingdom
Site UK44002
🇬🇧Preston, United Kingdom
Site UK44003
🇬🇧Sheffield, United Kingdom
Site UK44008
🇬🇧Southampton, United Kingdom
Site AR54006
🇦🇷La Rioja, Argentina
Site AR54003
🇦🇷Viedma, Argentina
Site KR82004
🇰🇷Seongnam-si, Korea, Republic of
Site RU70002
🇷🇺Omsk, Russian Federation
Site SG65001
🇸🇬Singapore, Singapore
Site KR82008
🇰🇷Hwasun, Korea, Republic of
Site NL31001
🇳🇱Amsterdam, Netherlands
Site NL31007
🇳🇱Leeuwarden, Netherlands
Site JP81010
🇯🇵Ube, Japan
Site TW88605
🇨🇳Taipei, Taiwan
Huntsman Cancer Institute
🇺🇸Salt Lake City, Utah, United States
Site AR54005
🇦🇷Cordoba, Argentina
Arizona Oncology Associates PD - HOPE
🇺🇸Tucson, Arizona, United States
Maine Health Cancer Care
🇺🇸Biddeford, Maine, United States
Johns Hopkins Medical Center
🇺🇸Baltimore, Maryland, United States
Lombardi Cancer Center / Georgetown University Medical Center
🇺🇸Washington, District of Columbia, United States
Site AR54004
🇦🇷Mendoza, Argentina
Site BE32002
🇧🇪Ghent, Belgium
Site BE32001
🇧🇪Liege, Belgium
Ironwood Cancer & Research Centers - Chandler
🇺🇸Chandler, Arizona, United States
Eastern CT Hematology and Oncology Associates
🇺🇸Norwich, Connecticut, United States
Site DE49001
🇩🇪Lubeck, Germany
Site CA11012
🇨🇦Toronto, Ontario, Canada
Comprehensive Cancer Centers of Nevada
🇺🇸Las Vegas, Nevada, United States
Site CA11002
🇨🇦Hamilton, Ontario, Canada
Site AR54011
🇦🇷Caba, Argentina
Site DE49014
🇩🇪Erlangen, Germany
Site DE49008
🇩🇪Magdeburg, Germany
Site JP81004
🇯🇵Tsukuba, Japan
Site NL31002
🇳🇱Amsterdam, Netherlands
Site NL31003
🇳🇱Rotterdam, Netherlands
Site PL48002
🇵🇱Warszawa, Poland
Site RU70014
🇷🇺Krasnoyarsk, Russian Federation
Site RU70019
🇷🇺Pyatigorsk, Russian Federation
Site TW88603
🇨🇳Kaohsiung, Taiwan
Site TH66005
🇹🇭Chiang Mai, Thailand
Saint Francis Hospital / Bon Secours - South Carolina
🇺🇸Greenville, South Carolina, United States
Site CA11009
🇨🇦London, Ontario, Canada
West Cancer Center & Research Institute
🇺🇸Germantown, Tennessee, United States
Site HU36002
🇭🇺Budapest, Hungary
Site RU70004
🇷🇺Moscow, Russian Federation
Site BE32006
🇧🇪Roeselare, Belgium
Site KR82002
🇰🇷Goyang-si, Korea, Republic of
Site IT39008
🇮🇹Candiolo, Italy
Site IT39003
🇮🇹Meldola, Italy
Site JP81002
🇯🇵Bunkyo City, Japan
Site JP81013
🇯🇵Fukuoka, Japan
Site JP81020
🇯🇵Fukuoka, Japan
Site JP81015
🇯🇵Niigata, Japan
Site RU70007
🇷🇺Saint Petersburg, Russian Federation
Site KR82003
🇰🇷Seoul, Korea, Republic of
Site IL97211
🇮🇱Rehovot, Israel
Site IT39004
🇮🇹Pisa, Italy
Site JP81009
🇯🇵Chiba, Japan
Site JP81018
🇯🇵Chiba, Japan
Site JP81019
🇯🇵Tokyo, Japan
Site CH41001
🇨🇭Chur, Switzerland
Site TW88606
🇨🇳Taichung, Taiwan
Site FR33016
🇫🇷Lyon, France
Site CA11010
🇨🇦Montreal, Quebec, Canada
Site FR33014
🇫🇷Bordeaux, France
Site FR33011
🇫🇷Villejuif-Cedex-France, France
Site DE49012
🇩🇪Mannheim, Germany
Site IL97202
🇮🇱Kfar Saba, Israel
Site IL97208
🇮🇱Petach Tikva, Israel
Site IT39001
🇮🇹Verona, Italy
Site JP81001
🇯🇵Koto-ku, Japan
Site RU70017
🇷🇺Nizhniy Novgorod, Russian Federation
Site RU70010
🇷🇺Saint Petersburg, Russian Federation
Site SG65003
🇸🇬Singapore, Singapore
Site CA11011
🇨🇦Oshawa, Ontario, Canada
Site KR82007
🇰🇷Seoul, Korea, Republic of
Site IL97209
🇮🇱Holon, Israel
Site IT39002
🇮🇹Terni, Italy
Site IT39011
🇮🇹Torrette, Italy
Site JP81016
🇯🇵Osakasayama-Shi, Japan
Site JP81012
🇯🇵Sendai-city, Japan
Site NL31006
🇳🇱Utrecht, Netherlands
Site RU70012
🇷🇺Saint-Petersburg, Russian Federation
Site SG65002
🇸🇬Singapore, Singapore
Site TH66002
🇹🇭HatYai, Thailand
Site TR90003
🇹🇷Istanbul, Turkey
Site HU36003
🇭🇺Budapest, Hungary
Site KR82005
🇰🇷Seoul, Korea, Republic of
Site KR82006
🇰🇷Seoul, Korea, Republic of
Site TW88607
🇨🇳Taichung, Taiwan
Site TH66006
🇹🇭Krung Thep Maha Nakhon, Thailand
Site TH66007
🇹🇭Muang, Thailand
Site TR90008
🇹🇷Istanbul, Turkey
Providence St Joseph Medical Center
🇺🇸Burbank, California, United States
University of California Los Angeles Medical Center
🇺🇸Los Angeles, California, United States
City of Hope National Medical Center
🇺🇸Duarte, California, United States
New Mexico Cancer Center
🇺🇸Albuquerque, New Mexico, United States
Georgia Cancer Specialists / Northside Hospital Cancer Institute
🇺🇸Marietta, Georgia, United States
University of California Irvine - Newport
🇺🇸Orange, California, United States
Winship Cancer Institute / Emory University School of Medicine
🇺🇸Atlanta, Georgia, United States
New York University (NYU) Cancer Institute
🇺🇸New York, New York, United States
Vidant Medical Center
🇺🇸Greenville, North Carolina, United States
University of Texas Southwestern Medical Center
🇺🇸Dallas, Texas, United States
The Cleveland Clinic
🇺🇸Cleveland, Ohio, United States
Mount Sinai Medical Center
🇺🇸New York, New York, United States
Toledo Clinic Cancer Center
🇺🇸Toledo, Ohio, United States
Memorial Sloan Kettering Cancer Center
🇺🇸New York, New York, United States
Seattle Cancer Care Alliance / University of Washington
🇺🇸Seattle, Washington, United States
University of Virginia
🇺🇸Charlottesville, Virginia, United States
Site DK45001
🇩🇰Aalborg, Denmark
Site IT39005
🇮🇹Areezo, Italy
Cancer Centers of Colorado - Denver
🇺🇸Denver, Colorado, United States
Rocky Mountain Cancer Centers - Aurora
🇺🇸Aurora, Colorado, United States
University of Colorado Hospital / University of Colorado
🇺🇸Aurora, Colorado, United States
Yale Cancer Center
🇺🇸New Haven, Connecticut, United States
H. Lee Moffitt Cancer Center and Research Institute
🇺🇸Tampa, Florida, United States