Amcenestrant (SAR439859) Plus Palbociclib as First Line Therapy for Patients With ER (+) HER2(-) Advanced Breast Cancer

Phase 3

Terminated

Conditions: Breast Cancer

Interventions: Drug: Amcenestrant-matching placebo
Drug: SAR439859
Drug: Palbociclib
Drug: Letrozole
Drug: Letrozole-matching placebo
Drug: Goserelin

Registration Number: NCT04478266

Lead Sponsor: Sanofi

Brief Summary: Primary Objective:

To determine whether Amcenestrant (SAR439859) in combination with palbociclib improves progression free survival (PFS) when compared with letrozole in combination with palbociclib in participants with estrogen receptor positive (ER+), human epidermal growth factor receptor 2 negative (HER2-) advanced breast cancer who have not received any prior systemic anticancer therapies for advanced disease.

Secondary Objective:

* To compare the overall survival in both treatment arms.

* To evaluate the objective response rate in both treatment arms.

* To evaluate the duration of response in both treatment arms.

* To evaluate the clinical benefit rate in both treatment arms.

* To evaluate progression-free survival on next line of therapy.

* To evaluate the pharmacokinetics of amcenestrant, and palbociclib.

* To evaluate health-related quality of life in both treatment arms.

* To evaluate the time to first chemotherapy in both treatment arms.

* To evaluate safety in both treatment arms.

Detailed Description: Study duration per participant was approximately 59 months, which includes a 33- month treatment period.

Recruitment & Eligibility

Status: TERMINATED

Sex: All

Target Recruitment: 1068

Inclusion Criteria

Not provided

Exclusion Criteria

Not provided

Study Type: INTERVENTIONAL

Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Amcenestrant + Palbociclib	Letrozole-matching placebo	Participants received amcenestrant 200 mg tablet along with letrozole-matching placebo once daily, continuously and palbociclib 125 mg PO, QD from Day 1 to Day 21 of each 28-day treatment cycle until disease progression, death, or study cut-off date, whichever comes first (maximum exposure: 109 weeks). Goserelin once every 4 weeks in pre/peri menopausal women and men.
Letrozole + Palbociclib	Amcenestrant-matching placebo	Participants received letrozole 2.5 milligrams (mg) capsule along with amcenestrant-matching placebo once daily, continuously and palbociclib 125 mg orally (PO), once daily (QD) from Day 1 to Day 21 of each 28-day treatment cycle until disease progression, death or study cut-off date, whichever comes first (maximum exposure: 112 weeks). Goserelin once every 4 weeks in pre/peri menopausal women and men.
Amcenestrant + Palbociclib	SAR439859	Participants received amcenestrant 200 mg tablet along with letrozole-matching placebo once daily, continuously and palbociclib 125 mg PO, QD from Day 1 to Day 21 of each 28-day treatment cycle until disease progression, death, or study cut-off date, whichever comes first (maximum exposure: 109 weeks). Goserelin once every 4 weeks in pre/peri menopausal women and men.
Letrozole + Palbociclib	Palbociclib	Participants received letrozole 2.5 milligrams (mg) capsule along with amcenestrant-matching placebo once daily, continuously and palbociclib 125 mg orally (PO), once daily (QD) from Day 1 to Day 21 of each 28-day treatment cycle until disease progression, death or study cut-off date, whichever comes first (maximum exposure: 112 weeks). Goserelin once every 4 weeks in pre/peri menopausal women and men.
Letrozole + Palbociclib	Letrozole	Participants received letrozole 2.5 milligrams (mg) capsule along with amcenestrant-matching placebo once daily, continuously and palbociclib 125 mg orally (PO), once daily (QD) from Day 1 to Day 21 of each 28-day treatment cycle until disease progression, death or study cut-off date, whichever comes first (maximum exposure: 112 weeks). Goserelin once every 4 weeks in pre/peri menopausal women and men.
Letrozole + Palbociclib	Goserelin	Participants received letrozole 2.5 milligrams (mg) capsule along with amcenestrant-matching placebo once daily, continuously and palbociclib 125 mg orally (PO), once daily (QD) from Day 1 to Day 21 of each 28-day treatment cycle until disease progression, death or study cut-off date, whichever comes first (maximum exposure: 112 weeks). Goserelin once every 4 weeks in pre/peri menopausal women and men.
Amcenestrant + Palbociclib	Palbociclib	Participants received amcenestrant 200 mg tablet along with letrozole-matching placebo once daily, continuously and palbociclib 125 mg PO, QD from Day 1 to Day 21 of each 28-day treatment cycle until disease progression, death, or study cut-off date, whichever comes first (maximum exposure: 109 weeks). Goserelin once every 4 weeks in pre/peri menopausal women and men.
Amcenestrant + Palbociclib	Goserelin	Participants received amcenestrant 200 mg tablet along with letrozole-matching placebo once daily, continuously and palbociclib 125 mg PO, QD from Day 1 to Day 21 of each 28-day treatment cycle until disease progression, death, or study cut-off date, whichever comes first (maximum exposure: 109 weeks). Goserelin once every 4 weeks in pre/peri menopausal women and men.

Primary Outcome Measures

Name	Time	Method
Progression-free Survival (PFS)	From randomization to the date of first documented tumor progression or death due to any cause or data cut-off date whichever comes first (maximum duration: 81 weeks)	PFS was defined as the time interval (in months) from the date of randomization to the date of first documented tumor progression as per Response Evaluation Criteria in Solid Tumors (RECIST 1.1) assessed by local radiologist or investigator, or death (due to any cause), whichever comes first. Progressive Disease (PD) as per RECIST 1.1: at least a 20 percent (%) increase in sum of diameters of target lesions, unequivocal progression of existing non-target lesions. Analysis was performed by Kaplan-Meier method.

Secondary Outcome Measures

Name	Time	Method
Change From Baseline in European Quality of Life Working Group Health Status Measure 5 Dimensions (5D), 5 Levels (5L) (EQ-5D-5L) Score: Visual Analog Scale (VAS) Score	Baseline, overall treatment duration (Cycle 1 up to Cycle 21 [i.e., 81 weeks])	EQ-5D-5L is a standardized measure of health status, provides a simple, generic measure of health for clinical and economic appraisal, and consists of 2 sections: the EQ-5D-5L health state utility index (descriptive system) and the EQ-5D-5L VAS. The Visual Analogue Scale is designed to rate the participant's current health state on a scale from 0 to 100, where 0 represents the worst imaginable health state and 100 represents the best imaginable health state. LS mean and SE are derived from MMRM model with change from Baseline values as response variable, treatment, time, treatment-by-time interaction, Baseline value and stratifications factors as fixed effect. Average of LS mean change from Baseline values of overall treatment (i.e., each cycle \[Cycle 1 up to Cycle 21\]) for VAS was reported in this outcome measure.
Overall Survival (OS)	From randomization to the death due to any cause or data cut-off date, whichever comes first (maximum duration: 81 weeks)	OS was defined as the interval (in months) from the date of randomization to the date of documented death (due to any cause). In the absence of observation of death, survival time was censored to last date the participant was known to be alive or at the cut-off date, whichever comes first. Analysis was performed by Kaplan-Meier method.
Percentage of Participants With Objective Response	From randomization to the date of first documented tumor progression, death due to any cause or data cut-off date whichever comes first (maximum duration: 81 weeks)	Objective response was defined as percentage of participants having a partial response (PR) or complete response (CR) according to the RECIST version 1.1 assessed by investigator. As per RECIST 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 less than (\<) 10 millimeters (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.
Change From Baseline in European Organization for Research and Treatment of Cancer Core Quality of Life Questionnaire (EORTC-QLQ-C30) Domain Scores	Baseline, overall treatment duration (Cycle 1 up to Cycle 21 [i.e., 81 weeks])	EORTC-QLQ-C30: cancer-specific instrument with 30 questions for evaluation of new chemotherapy \& assessment of participant reported outcome. These include 5 functional scales, 9 symptom scales, \& Global Health Status/quality of life scale (GHS/QoL). All 14 items/domains were scored on scale of 1 (not at all) to 4 (very much) \& GHS/QoL, scored on scale of 1 (very poor) to 7 (excellent). All scales are transformed from raw scores to linear scales ranging 0 to 100. Higher score for functional \& GHS/QoL=higher level of functioning, \& higher score for symptoms scales=higher symptom burden. Least Square (LS) mean and Standard Error (SE) were derived from MMRM model with change from Baseline values as response variable, treatment, time, treatment-by-time interaction, Baseline value and stratifications factors as fixed effect. Average of LS mean change from Baseline values of overall treatment (i.e., each cycle \[Cycle 1 up to Cycle 21\]) for each domain was reported in this outcome measure.
Pharmacokinetics: Plasma Concentrations of Palbociclib	Cycle 1 Day 1: 3 hr post-dose, Cycle 1 Day 15: pre-dose, Cycle 2 Day 1: pre-dose, 3 hr post-dose, Cycle 2 Day 15: pre-dose, Cycle 3 Day 1: pre-dose, Cycle 4 Day 1: pre-dose, Cycle 7 Day 1: pre-dose, Cycle 10 Day 1: pre-dose	Palbociclib plasma concentrations at specified time points were reported.
Number of Participants With Liver Function Abnormalities of Grade 3 and 4 During the Treatment Period	From first dose of study treatment up to 30 days after last dose of study treatment (maximum duration: 112 weeks)	Liver Function parameters assessed were aspartate aminotransferase increased, alanine aminotransferase increased, alkaline phosphatase increased, total bilirubin increased, gamma-glutamyl transferase increased. Parameters were assessed as per the NCI-CTCAE v 5.0, where Grade 1 = Mild; Grade 2 = Moderate; Grade 3 = Severe; Grade 4 = Potentially Life Threatening. Grade refers to the severity of the AEs. Treatment period was defined as the time from the first dose of study treatments up to 30 days after last dose of study treatment. Participants with Grade 3 and 4 liver function abnormalities were reported in this outcome measure.
12-month Progression-free Survival (PFS) Rate	Month 12	Percentage of participants who were disease progression-free at Month 12 after randomization were reported in this outcome measure. PFS was defined as the time interval (in months) from the date of randomization to the date of first documented tumor progression as per RECIST 1.1 assessed by local radiologist or investigator, or death (due to any cause), whichever comes first. PD as per RECIST 1.1: at least a 20% increase in sum of diameters of target lesions, unequivocal progression of existing non-target lesions. The PFS rate at Month 12 was estimated using the Kaplan-Meier method and provided an estimation of the percentage of participants who were disease progression-free at Month 12 after randomization.
Pharmacokinetics: Plasma Concentrations of Amcenestrant	Cycle 1 Day 1: 3 hours (hr) post-dose, Cycle 1 Day 15: pre-dose, Cycle 2 Day 1: pre-dose, 3 hr post-dose, Cycle 2 Day 15: pre-dose, Cycle 3 Day 1: pre-dose, Cycle 4 Day 1: pre-dose, Cycle 7 Day 1: pre-dose, Cycle 10 Day 1: pre-dose	Amcenestrant plasma concentrations at specified time points were reported. Data for this outcome measure was not planned to be collected and analyzed for Letrozole+Palbociclib arm as pre-specified in protocol.
Change From Baseline in European Organization for Research and Treatment of Cancer Quality of Life Breast Cancer Specific Module (EORTC QLQ-BR45) Domain Scores	Baseline, overall treatment duration (Cycle 1 up to Cycle 21 [i.e., 81 weeks])	EORTC QLQ-BR45: comprised of all 23 items from the QLQ-BR23 plus an additional 22 items assessing endocrine therapy symptoms (10 items), endocrine sexual symptoms (4 items), breast satisfaction (2 items), and skin mucosis symptoms (6 items). All items scored 1 (not at all) to 4 (very much). Scores of all scales transformed from raw scores to linear scales ranging 0 to 100. Higher score for functional scales = better outcome; higher score for symptoms scales = higher symptom burden. LS mean and SE are derived from Mixed Model Repeated Measures (MMRM) model with change from Baseline values as response variable, treatment, time, treatment-by-time interaction, Baseline value and stratifications factors as fixed effect. Average of LS mean change from Baseline values of overall treatment (i.e., each cycle \[Cycle 1 up to Cycle 21\]) for each domain (endocrine therapy symptoms, endocrine sexual symptoms, breast satisfaction and skin mucosis symptoms) was reported.
Duration of Response (DOR)	From the date of first response of CR or PR until disease progression or death, or start of any anti-cancer therapy or data cut-off date, whichever comes first (maximum duration: 81 weeks)	DOR was defined as time (in months) from first documented evidence of CR or PR until disease progression determined by investigator as per RECIST 1.1, or start of any anti-cancer therapy, or death from any cause, whichever occurs first. For participants with ongoing response at the time of the analysis, DOR was censored at the date of the last valid disease assessment not showing documented progression performed before the initiation of a new anticancer treatment (if any). As per RECIST 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: at least a 30% decrease in the sum of diameters of target lesions, taking as reference the Baseline sum diameters. PD: at least 20% increase in sum of diameters of target lesions, unequivocal progression of existing non-target lesions. Analysis was performed by Kaplan-Meier method.
Percentage of Participants With Clinical Benefit	From randomization until disease progression, or death, or data cut-off date, whichever comes first (maximum duration: 81 weeks)	Clinical Benefit was defined as the percentage of participants having a confirmed CR, PR, or stable disease (SD) for at least 24 weeks determined by investigator as per RECIST 1.1, from date of randomization until disease progression, or death, or data cut-off date, or initiation of post treatment anti-cancer therapy, whichever occurs first. As per RECIST 1.1; CR was defined as disappearance of all target, non-target lesions \& normalization of tumor marker level. Any pathological lymph nodes (whether target or non-target) must have reduction in short axis to \<10 mm. PR: at least a 30% decrease in sum of diameters of target lesions, taking as reference Baseline sum diameters. SD: neither sufficient shrinkage to qualify for PR nor sufficient increase to qualify for PD, taking as reference smallest sum diameters. PD: at least 20% increase in sum of diameters of target lesions, unequivocal progression of existing non-target lesions.
Progression-free Survival on Next Line of Therapy (PFS2)	From randomization to date first documented disease progression on the next systemic anti-cancer therapy, or death due to any cause, or data cut-off date, whichever comes first (maximum duration: 81 weeks)	PFS2 was defined as the time interval (in months) from the date of randomization to the date of first documentation of PD on the next systemic anti-cancer therapy according to investigator, or death due to any cause in the absence of documented PD on the next systemic anti-cancer therapy, whichever occurs first. PD was defined as at least 20% increase in sum of diameters of target lesions, unequivocal progression of existing non-target lesions. Analysis was performed by Kaplan-Meier method.
Change From Baseline in European Organization for Research and Treatment of Cancer Quality of Life Breast Cancer Specific Module (EORTC-QLQ-BR23) Domain Scores	Baseline, overall treatment duration (Cycle 1 up to Cycle 21 [i.e., 81 weeks])	QLQ-BR23: disease-specific Health-related QOL assesses breast cancer impact \& side effects of treatment. EORTCQLQ- BR23 contains 23 items: multi-item scales \& single-item measures. 4 functional scales (body image, sexual functioning, sexual enjoyment, future perspective) \& 4 scales related to symptoms of disease or treatment (arm symptoms, breast symptoms, systemic therapy side effects, \& upset by hair loss). All items scored 1 (not at all) to 4 (very much). Scores of all scales transformed from raw scores to linear scales ranging 0-100. Higher score for functional scales=better outcome; higher score for symptoms scales=higher symptom burden. LS mean \& SE were derived from MMRM model with change from Baseline values as response variable, treatment, time, treatment-by-time interaction, Baseline value \& stratifications factors as fixed effect. Average of LS mean change from Baseline values of overall treatment (i.e., each cycle \[Cycle 1 up to Cycle 21\]) for each domain was reported.
Change From Baseline in European Quality of Life Working Group Health Status Measure 5 Dimensions (5D), 5 Levels (5L) (EQ-5D-5L) Score: Health Utility Index Value Score	Baseline, overall treatment duration (Cycle 1 up to Cycle 21 [i.e., 81 weeks])	EQ-5D-5L: consists of 2 sections: EQ-5D-5L health state utility index (descriptive system) \& VAS. The EQ-5D descriptive system consists of 5 dimensions: mobility, self-care, usual activities, pain/discomfort \& anxiety/depression. Each dimension has 5 levels: no problems, slight problems, moderate problems, severe problems, \& extreme problems. Response options are measured with 5-point Likert scale (for 5L version). The EQ-5D-5L responses are converted into single index utility score between 0 to 1, where higher score indicates better health state \& lower score indicate worse health state. LS mean and SE were derived from MMRM model with change from Baseline values as response variable, treatment, time, treatment-by-time interaction, Baseline value and stratifications factors as fixed effect. Average of LS mean change from Baseline values overall treatment (i.e., each cycle \[Cycle 1 up to Cycle 21\]) for health utility index value score was reported in this outcome measure.
Time to First Chemotherapy	From randomization to the start date of the first chemotherapy (maximum duration: 81 weeks)	Time to chemotherapy was defined as the time interval (in months) from the date of randomization to the start date of the first chemotherapy after disease progression.
Number of Participants With Hematological Abnormalities During the Treatment Period	From first dose of study treatment up to 30 days after last dose of study treatment (maximum duration: 112 weeks)	Hematological parameters assessed were anemia, lymphocyte count decreased, neutrophil count decreased, white blood cell decreased, platelet count decreased. Parameters were assessed as per the National Cancer Institute Common Terminology Criteria for Adverse Experience version 5.0 (NCI-CTCAE v 5.0), where Grade 1 = Mild; Grade 2 = Moderate; Grade 3 = Severe; Grade 4 = Potentially Life Threatening. Grade refers to the severity of the AEs. Treatment period was defined as the time from the first dose of study treatments up to 30 days after last dose of study treatment.

Trial Locations

Locations (249): Investigational Site Number :8400029
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Santa Monica, California, United States
Investigational Site Number :8400038
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Fullerton, California, United States
Investigational Site Number :8400013
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Westwood, Kansas, United States
Investigational Site Number :8400028
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Scarborough, Maine, United States
Investigational Site Number :8400039
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Chicago, Illinois, United States
Investigational Site Number :8400001
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Pittsburgh, Pennsylvania, United States
Investigational Site Number :8400017
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Boston, Massachusetts, United States
Investigational Site Number :8400061
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Houston, Texas, United States
Investigational Site Number :8400058
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Las Vegas, Nevada, United States
Investigational Site Number :8400068
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Houston, Texas, United States
Investigational Site Number :0760008
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São Paulo, Brazil
Investigational Site Number :2030002
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Praha 2, Czechia
Investigational Site Number :8400067
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Tigard, Oregon, United States
Investigational Site Number :8400085
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Blacksburg, Virginia, United States
Investigational Site Number :1000001
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Sofia, Bulgaria
Investigational Site Number :1240004
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Kingston, Ontario, Canada
Investigational Site Number :8400016
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Atlanta, Georgia, United States
Investigational Site Number :8400008
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Fort Wayne, Indiana, United States
Investigational Site Number :1560036
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Changchun, China
Investigational Site Number :1560006
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Hangzhou, China
Investigational Site Number :1560005
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Hangzhou, China
Investigational Site Number :1560011
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Harbin, China
Investigational Site Number :1560055
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Luoyang, China
Investigational Site Number :5280006
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Arnhem, Netherlands
Investigational Site Number :0760005
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Porto Alegre, Rio Grande Do Sul, Brazil
Investigational Site Number :1520009
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Talca, Maule, Chile
Investigational Site Number :0360001
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Nedlands, Western Australia, Australia
Investigational Site Number :3800005
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Prato, Italy
Investigational Site Number :6430003
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Moscow, Russian Federation
Investigational Site Number :0320001
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Caba, Buenos Aires, Argentina
Investigational Site Number :0320006
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Pergamino, Buenos Aires, Argentina
Investigational Site Number :0320009
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Mar del Plata, Argentina
Investigational Site Number :0560004
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Charleroi, Belgium
Investigational Site Number :0320002
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Rosario, Santa Fe, Argentina
Investigational Site Number :8400015
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New Brunswick, New Jersey, United States
Investigational Site Number :8400083
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Glendale, Arizona, United States
Investigational Site Number :0320005
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Caba, Buenos Aires, Argentina
Investigational Site Number :0320004
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Buenos Aires, Argentina
Investigational Site Number :0400001
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Graz, Austria
Investigational Site Number :0320010
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Cordoba, Córdoba, Argentina
Investigational Site Number :0320003
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La Rioja, Argentina
Investigational Site Number :0360002
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Richmond, Victoria, Australia
Investigational Site Number :0320008
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Capital Federal, Buenos Aires, Argentina
Investigational Site Number :0320007
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Salta, Argentina
Investigational Site Number :8400066
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Tucson, Arizona, United States
Investigational Site Number :8400024
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Paramus, New Jersey, United States
Investigational Site Number :0560001
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Leuven, Belgium
Investigational Site Number :0560002
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Namur, Belgium
Investigational Site Number :1520006
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Santiago, Reg Metropolitana De Santiago, Chile
Investigational Site Number :2680004
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Tbilisi, Georgia
Investigational Site Number :6430005
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Moscow, Russian Federation
Investigational Site Number :1520005
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La Serena, Coquimbo, Chile
Investigational Site Number :3920015
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Meguro-ku, Tokyo, Japan
Investigational Site Number :6430010
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Saint Petersburg, Russian Federation
Investigational Site Number :1240005
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Montreal, Quebec, Canada
Investigational Site Number :6430001
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Saint -Petersburg, Russian Federation
Investigational Site Number :8400075
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Daphne, Alabama, United States
Investigational Site Number :8400056
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Los Alamitos, California, United States
Investigational Site Number :8400055
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Athens, Georgia, United States
Investigational Site Number :8400081
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Palm Bay, Florida, United States
Investigational Site Number :8400059
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Lakeland, Florida, United States
Investigational Site Number :8400034
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Savannah, Georgia, United States
Investigational Site Number :8400035
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Thomasville, Georgia, United States
Investigational Site Number :8400006
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Iowa City, Iowa, United States
Investigational Site Number :8400076
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Danvers, Massachusetts, United States
Investigational Site Number :8400077
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Newton, Massachusetts, United States
Investigational Site Number :8400004
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Saint Louis, Missouri, United States
Investigational Site Number :8400023
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Stony Brook, New York, United States
Investigational Site Number :8400010
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New York, New York, United States
Investigational Site Number :8400070
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Dallas, Texas, United States
Investigational Site Number :1560051
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Jining, China
Investigational Site Number :8400072
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Dallas, Texas, United States
Investigational Site Number :8400080
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Denton, Texas, United States
Investigational Site Number :8400086
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The Woodlands, Texas, United States
Investigational Site Number :8400084
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Plano, Texas, United States
Investigational Site Number :8400078
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Waco, Texas, United States
Investigational Site Number :8400082
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Webster, Texas, United States
Investigational Site Number :8400069
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Winchester, Virginia, United States
Investigational Site Number :0360004
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Macquarie Park, New South Wales, Australia
Investigational Site Number :0360005
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Randwick, New South Wales, Australia
Investigational Site Number :0360003
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Wahroonga, New South Wales, Australia
Investigational Site Number :0560003
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Bruxelles, Belgium
Investigational Site Number :0760007
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Sao Paulo, São Paulo, Brazil
Investigational Site Number :0760003
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Sao Paulo, São Paulo, Brazil
Investigational Site Number :0760006
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Porto Alegre, Rio Grande Do Sul, Brazil
Investigational Site Number :0760004
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Rio De Janeiro, Brazil
Investigational Site Number :1000004
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Burgas, Bulgaria
Investigational Site Number :1000005
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Dobrich, Bulgaria
Investigational Site Number :1000008
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Russe, Bulgaria
Investigational Site Number :1240002
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Toronto, Ontario, Canada
Investigational Site Number :1240014
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Montreal, Quebec, Canada
Investigational Site Number :1240007
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Greenfield Park, Quebec, Canada
Investigational Site Number :1520004
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Temuco, La Araucanía, Chile
Investigational Site Number :1520011
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Santaigo, Reg Metropolitana De Santiago, Chile
Investigational Site Number :1520001
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Viña del Mar, Valparaíso, Chile
Investigational Site Number :1520002
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Santiago, Reg Metropolitana De Santiago, Chile
Investigational Site Number :1520003
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Santiago de Chile, Chile
Investigational Site Number :1520007
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Santiago, Chile
Investigational Site Number :1560008
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Beijing, China
Investigational Site Number :1560038
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Baoding, China
Investigational Site Number :1560003
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Changchun, China
Investigational Site Number :1560035
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Beijing, China
Investigational Site Number :1560013
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Chengdu, China
Investigational Site Number :1560019
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Chongqing, China
Investigational Site Number :1560031
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Dalian, China
Investigational Site Number :1560021
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Dalian, China
Investigational Site Number :1560043
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Fuzhou, China
Investigational Site Number :1560054
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Deyang, China
Investigational Site Number :1560025
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Guangzhou, China
Investigational Site Number :1560007
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Hangzhou, China
Investigational Site Number :1560002
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Hangzhou, China
Investigational Site Number :1560018
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Jinan, China
Investigational Site Number :1560041
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Hefei, China
Investigational Site Number :1560046
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Jinan, China
Investigational Site Number :1560017
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Linyi, China
Investigational Site Number :1560048
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Neijiang, China
Investigational Site Number :1560001
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Shanghai, China
Investigational Site Number :1560037
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Shaoguan, China
Investigational Site Number :1560028
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Tianjin, China
Investigational Site Number :1560033
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Wuhan, China
Investigational Site Number :1560024
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Wuhan, China
Investigational Site Number :1560044
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Xi'An, China
Investigational Site Number :1560049
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Yantai, China
Investigational Site Number :1560045
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Xi'an, China
Investigational Site Number :1560027
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Xuzhou, China
Investigational Site Number :2030001
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Brno, Czechia
Investigational Site Number :1560022
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Zhengzhou, China
Investigational Site Number :2460001
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Helsinki, Finland
Investigational Site Number :2500009
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Nice, France
Investigational Site Number :2460003
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Turku, Finland
Investigational Site Number :2460002
🇫🇮
Tampere, Finland
Investigational Site Number :2500001
🇫🇷
Paris, France
Investigational Site Number :2500003
🇫🇷
Paris, France
Investigational Site Number :2500007
🇫🇷
Saint Cloud, France
Investigational Site Number :2500006
🇫🇷
Poitiers, France
Investigational Site Number :2500010
🇫🇷
Strasbourg, France
Investigational Site Number :2500002
🇫🇷
Saint-Herblain, France
Investigational Site Number :2500005
🇫🇷
TOULOUSE Cedex 9, France
Investigational Site Number :2500004
🇫🇷
Villejuif, France
Investigational Site Number :2680006
🇬🇪
Kutaisi, Georgia
Investigational Site Number :2680001
🇬🇪
Tbilisi, Georgia
Investigational Site Number :2680005
🇬🇪
Batumi, Georgia
Investigational Site Number :2680002
🇬🇪
Tbilisi, Georgia
Investigational Site Number :2680007
🇬🇪
Tbilisi, Georgia
Investigational Site Number :2680003
🇬🇪
Tbilisi, Georgia
Investigational Site Number :2760006
🇩🇪
Bottrop, Germany
Investigational Site Number :2760003
🇩🇪
Münster, Germany
Investigational Site Number :2760001
🇩🇪
Ulm, Germany
Investigational Site Number :2760007
🇩🇪
Oldenburg in Holstein, Germany
Investigational Site Number :3480011
🇭🇺
Gyula, Hungary
Investigational Site Number :3480008
🇭🇺
Budapest, Hungary
Investigational Site Number :3480005
🇭🇺
Győr, Hungary
Investigational Site Number :3480001
🇭🇺
Nyíregyháza, Hungary
Investigational Site Number :3480003
🇭🇺
Kaposvár, Hungary
Investigational Site Number :3480009
🇭🇺
Kecskemét, Hungary
Investigational Site Number :3480010
🇭🇺
Miskolc, Hungary
Investigational Site Number :3800008
🇮🇹
Meldola (FC), Emilia-Romagna, Italy
Investigational Site Number :3800003
🇮🇹
Rozzano, Milano, Italy
Investigational Site Number :3800007
🇮🇹
Monza, Monza E Brianza, Italy
Investigational Site Number :3800010
🇮🇹
Bologna, Italy
Investigational Site Number :3800004
🇮🇹
Milano, Italy
Investigational Site Number :3800002
🇮🇹
Milano, Italy
Investigational Site Number :3800006
🇮🇹
Napoli, Italy
Investigational Site Number :3920016
🇯🇵
Nagoya-shi, Aichi, Japan
Investigational Site Number :3920007
🇯🇵
Nagoya-shi, Aichi, Japan
Investigational Site Number :3920002
🇯🇵
Kashiwa-shi, Chiba, Japan
Investigational Site Number :3920009
🇯🇵
Matsuyama-shi, Ehime, Japan
Investigational Site Number :3920019
🇯🇵
Kurume-shi, Fukuoka, Japan
Investigational Site Number :3920014
🇯🇵
Yokohama-shi, Kanagawa, Japan
Investigational Site Number :3920017
🇯🇵
Takasaki-shi, Gunma, Japan
Investigational Site Number :3920010
🇯🇵
Hiroshima-shi, Hiroshima, Japan
Investigational Site Number :3920012
🇯🇵
Kagoshima-shi, Kagoshima, Japan
Investigational Site Number :3920001
🇯🇵
Sapporo-shi, Hokkaido, Japan
Investigational Site Number :3920006
🇯🇵
Yokohama-shi, Kanagawa, Japan
Investigational Site Number :3920022
🇯🇵
Miyazaki-shi, Miyazaki, Japan
Investigational Site Number :3920020
🇯🇵
Sendai-shi, Miyagi, Japan
Investigational Site Number :3920008
🇯🇵
Osaka-shi, Osaka, Japan
Investigational Site Number :3920018
🇯🇵
Osaka-shi, Osaka, Japan
Investigational Site Number :3920013
🇯🇵
Hidaka-shi, Saitama, Japan
Investigational Site Number :3920021
🇯🇵
Shizuoka-shi, Shizuoka, Japan
Investigational Site Number :3920003
🇯🇵
Koto-ku, Tokyo, Japan
Investigational Site Number :3920005
🇯🇵
Shinagawa-ku, Tokyo, Japan
Investigational Site Number :4100005
🇰🇷
Seongnam, Gyeonggi-do, Korea, Republic of
Investigational Site Number :4100007
🇰🇷
Seoul, Seoul-teukbyeolsi, Korea, Republic of
Investigational Site Number :4100006
🇰🇷
Goyang-si, Gyeonggi-do, Korea, Republic of
Investigational Site Number :4100002
🇰🇷
Seoul, Seoul-teukbyeolsi, Korea, Republic of
Investigational Site Number :4100004
🇰🇷
Seoul, Seoul-teukbyeolsi, Korea, Republic of
Investigational Site Number :4100003
🇰🇷
Seoul, Seoul-teukbyeolsi, Korea, Republic of
Investigational Site Number :5280005
🇳🇱
Delft, Netherlands
Investigational Site Number :4100009
🇰🇷
Seochogu, Korea, Republic of
Investigational Site Number :4100001
🇰🇷
Seoul, Seoul-teukbyeolsi, Korea, Republic of
Investigational Site Number :4100008
🇰🇷
Seongnam-si, Gyeonggi-do, Korea, Republic of
Investigational Site Number :5280001
🇳🇱
Maastricht, Netherlands
Investigational Site Number :6160007
🇵🇱
Poznan, Wielkopolskie, Poland
Investigational Site Number :6160002
🇵🇱
Tomaszow Mazowiecki, Lódzkie, Poland
Investigational Site Number :6200005
🇵🇹
Almada, Portugal
Investigational Site Number :6200002
🇵🇹
Porto, Portugal
Investigational Site Number :6200001
🇵🇹
Lisboa, Portugal
Investigational Site Number :7020004
🇸🇬
Singapore, Singapore
Investigational Site Number :6430007
🇷🇺
Arkhangelsk, Russian Federation
Investigational Site Number :6430004
🇷🇺
Krasnogorskiy District, Russian Federation
Investigational Site Number :6430009
🇷🇺
Moscow Region, Russian Federation
Investigational Site Number :6430008
🇷🇺
Moscow, Russian Federation
Investigational Site Number :6430006
🇷🇺
Moscow, Russian Federation
Investigational Site Number :7020002
🇸🇬
Singapore, Singapore
Investigational Site Number :7020001
🇸🇬
Singapore, Singapore
Investigational Site Number :7100004
🇿🇦
Cape Town, South Africa
Investigational Site Number :7100006
🇿🇦
Johannesburg, South Africa
Investigational Site Number :7240011
🇪🇸
Barcelona, Barcelona [Barcelona], Spain
Investigational Site Number :7240008
🇪🇸
Barcelona / Sabadell, Castilla Y León, Spain
Investigational Site Number :7240006
🇪🇸
Madrid / Madrid, Madrid, Comunidad De, Spain
Investigational Site Number :7240002
🇪🇸
Madrid / Madrid, Madrid, Comunidad De, Spain
Investigational Site Number :7240003
🇪🇸
Santiago de Compostela, Galicia [Galicia], Spain
Investigational Site Number :7240004
🇪🇸
Madrid, Madrid, Comunidad De, Spain
Investigational Site Number :7240005
🇪🇸
Valencia, Valenciana, Comunidad, Spain
Investigational Site Number :7240001
🇪🇸
Madrid, Spain
Investigational Site Number :7240007
🇪🇸
Málaga, Spain
Investigational Site Number :7240009
🇪🇸
Valencia, Spain
Investigational Site Number :1580001
🇨🇳
Taipei, Taiwan
Investigational Site Number :1580007
🇨🇳
Kaohsiung, Taiwan
Investigational Site Number :1580002
🇨🇳
Tainan, Taiwan
Investigational Site Number :1580003
🇨🇳
Taipei, Taiwan
Investigational Site Number :7920006
🇹🇷
Adana, Turkey
Investigational Site Number :7920005
🇹🇷
Bornova, Turkey
Investigational Site Number :7920003
🇹🇷
Edirne, Turkey
Investigational Site Number :7920007
🇹🇷
Antalya, Turkey
Investigational Site Number :7920008
🇹🇷
Ankara, Turkey
Investigational Site Number :7920009
🇹🇷
Ankara, Turkey
Investigational Site Number :7920011
🇹🇷
Istanbul, Turkey
Investigational Site Number :7920013
🇹🇷
Diyarbakır, Turkey
Investigational Site Number :7920001
🇹🇷
Istanbul, Turkey
Investigational Site Number :7920004
🇹🇷
Istanbul, Turkey
Investigational Site Number :7920012
🇹🇷
İzmir, Turkey
Investigational Site Number :7920010
🇹🇷
Kocaeli, Turkey
Investigational Site Number :7920002
🇹🇷
Malatya, Turkey
Investigational Site Number :8040004
🇺🇦
Kharkiv, Ukraine
Investigational Site Number :8040001
🇺🇦
Kryvyi Rih, Ukraine
Investigational Site Number :8040010
🇺🇦
Kharkiv, Ukraine
Investigational Site Number :8040002
🇺🇦
Odesa, Ukraine
Investigational Site Number :8040007
🇺🇦
Vinnytsia, Ukraine
Investigational Site Number :8260001
🇬🇧
Glasgow, Central Bedfordshire, United Kingdom
Investigational Site Number :8260005
🇬🇧
Blackburn, Lancashire, United Kingdom
Investigational Site Number :8260002
🇬🇧
Edinburgh, Edinburgh, City Of, United Kingdom
Investigational Site Number :8400025
🇺🇸
Denver, Colorado, United States
Investigational Site Number :8400053
🇺🇸
Orlando, Florida, United States
Investigational Site Number :8400002
🇺🇸
Ann Arbor, Michigan, United States
Investigational Site Number :8400005
🇺🇸
Kansas City, Missouri, United States
Investigational Site Number :8400009
🇺🇸
Winston-Salem, North Carolina, United States
Investigational Site Number :8400073
🇺🇸
Austin, Texas, United States

Amcenestrant (SAR439859) Plus Palbociclib as First Line Therapy for Patients With ER (+) HER2(-) Advanced Breast Cancer

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