A Study to Evaluate the Safety and Efficacy of Relugolix in Men With Advanced Prostate Cancer (HERO)

• ClinicalTrials.gov Identifier: NCT03085095
• Recruitment Status: Completed
• First Posted: March 21, 2017
• Results First Posted: March 25, 2021
• Last Update Posted: January 18, 2022
• Sponsor: Myovant Sciences GmbH
• Information provided by (Responsible Party): Myovant Sciences GmbH

Study Description

Brief Summary:

The purpose of this study is to determine the efficacy and safety of relugolix 120 milligrams (mg) orally once daily for 48 weeks on maintaining serum testosterone suppression to castrate levels (< 50 nanograms/deciliter [ng/dL]) in participants with androgen-sensitive advanced prostate cancer.

Condition or disease	Intervention/treatment	Phase
Prostate Cancer	Drug: Relugolix; Drug: Leuprolide Acetate	Phase 3

Detailed Description:

This is a phase 3, multinational, randomized, open-label, parallel group study to evaluate the efficacy and safety of oral daily relugolix 120 mg in participants with androgen-sensitive advanced prostate cancer who require at least 1 year of continuous androgen-deprivation therapy. Relugolix 120 mg orally once daily or leuprolide acetate depot suspension, 22.5 mg (or 11.25 mg in Japan and Taiwan based on local labels), every 3 months by subcutaneous injection will be administered to participants.

There are 2 analyses for this study, a primary analysis and a final analysis.

Primary Analysis:

The primary analysis of efficacy and safety has been completed (N=934). Participants were randomized 2:1 to receive relugolix or leuprolide for 48 weeks, followed by a 30-day safety follow-up visit or early termination 30-day safety follow-up.

Final Analysis:

The final analysis will occur after additional participants with metastatic disease (approximately 130) have been enrolled and randomized from any sites to the study, and have completed the 48-week treatment period. A cohort of participants enrolled in China and Taiwan will be analyzed separately once they have completed treatment to support registration in China.

Eligible participants were randomized 2:1 to relugolix or leuprolide arm and will attend visits monthly (every 4 weeks) where serum testosterone and prostate-specific antigen will be assessed. Safety will be assessed throughout the study by monitoring adverse events, vital signs, physical examinations, clinical laboratory tests, and 12-lead electrocardiograms.

Castration resistance-free survival will be assessed up to Week 49, Day 1 of the study and reported as part of the final analysis.

The study enrolled 1134 participants, including 139 participants with metastatic advanced prostate cancer to support the analysis of the secondary endpoint of castration resistance-free survival and 93 Chinese participants (enrolled in China and Taiwan) to support registration in China.

Study Design

• Study Type: Interventional (Clinical Trial)
• Actual Enrollment: 1134 participants
• Allocation: Randomized
• Intervention Model: Parallel Assignment
• Masking: None (Open Label)
• Primary Purpose: Treatment
• Official Title: HERO: A Multinational Phase 3 Randomized, Open-label, Parallel Group Study to Evaluate the Safety and Efficacy of Relugolix in Men With Advanced Prostate Cancer
• Actual Study Start Date: April 18, 2017
• Actual Primary Completion Date: October 25, 2019
• Actual Study Completion Date: November 26, 2021

Arms and Interventions

Arm	Intervention/treatment
Experimental: Relugolix; Relugolix for 48 weeks	Drug: Relugolix; Relugolix 120-mg tablet administered orally once daily following an oral loading dose of 360 mg (3 x 120-mg tablets) on Day 1; Other Names: TAK-385; MVT-601; RVT-601; T-1331285
Active Comparator: Leuprolide Acetate; Leuprolide acetate for 48 weeks	Drug: Leuprolide Acetate; Leuprolide acetate depot suspension, 22.5 mg (or 11.25 mg in Japan, Taiwan, and China), every 3 months by subcutaneous injection; Other Name: Leuprolide

Outcome Measures

Primary Outcome Measures :

1. Sustained Castration Rate [ Time Frame: From Week 5 Day 1 (Day 29) to Week 49 Day 1 (Day 337) ]

   Sustained castration rate defined as the cumulative probability of testosterone suppression to < 50 nanogram (ng)/deciliter (dL). The rate was estimated for each treatment group using the Kaplan-Meier method and reported as percentage of participants.

   The lower bound of the 95% confidence interval (CI) for the cumulative probability of sustained testosterone suppression in the relugolix treatment group must have been ≥ 90% to meet evaluation criteria for efficacy.

Secondary Outcome Measures :

1. Castration Rate At Week 1 Day 4 [ Time Frame: Week 1 Day 4 (Day 4) ]
   Castration rate was defined as the cumulative probability of testosterone suppression to < 50 ng/dL. The rate was estimated for each treatment group using the Kaplan-Meier method and reported as percentage of participants.
2. Castration Rate At Week 3 Day 1 [ Time Frame: Week 3 Day 1 (Day 15) ]
   Castration rate was defined as the cumulative probability of testosterone suppression to < 50 ng/dL. The rate was estimated for each treatment group using the Kaplan-Meier method and reported as percentage of participants.
3. Confirmed Prostate-specific Antigen (PSA) Response Rate [ Time Frame: Week 3 Day 1 (Day 15) and Week 5 Day 1 (Day 29) ]
   Confirmed PSA response defined as > 50% reduction in PSA from baseline at Week 3 Day 1 followed with confirmation at Week 5 Day 1.
4. Profound Castration Rate At Week 3 Day 1 (Day 15) [ Time Frame: Week 3 Day 1 (Day 15) ]
   Castration rate defined as the cumulative probability of testosterone suppression to < 20 ng/dL. The rate was estimated for each treatment group using the Kaplan-Meier method and reported as percentage of participants.
5. Follicle-stimulating Hormone (FSH) Level [ Time Frame: Week 25 Day 1 (Day 169) ]
   To evaluate the effect of relugolix and leuprolide acetate on FSH suppression.
6. PSA Response Rate At Week 3 Day 1 [ Time Frame: Week 3 Day 1 (Day 15) ]
   PSA response defined as > 50% reduction in PSA from baseline. The rate was estimated for each treatment group using the Kaplan-Meier method and reported as percentage of participants.
7. PSA Response Rate At Week 5 Day 1 [ Time Frame: Week 5 Day 1 (Day 29) ]
   PSA response defined as > 50% reduction in PSA from baseline. The rate was estimated for each treatment group using the Kaplan-Meier method and reported as percentage of participants.
8. Testosterone Recovery Rate [ Time Frame: Day 90 follow-up ]
   The cumulative probability of testosterone recovery back to > 280 ng/dL (lower limit of the normal range), back to ≥ 50 ng/dL (definition of castration), and back to > 280 ng/dL or baseline at 90 days after drug discontinuation was assessed. The rate was estimated for each treatment group using the Kaplan-Meier method and reported as percentage of participants.
9. Sustained Profound Castration Rate From Week 5 Day 1 Through Week 49 Day 1 [ Time Frame: Week 5 Day 1 (Day 29) through Week 49 Day 1 (Day 337) ]
   Sustained profound castration rate was defined as the cumulative probability of testosterone suppression to < 20 ng/dL. The rate was estimated by the Kaplan-Meier method and reported as percentage of participants.
10. Profound Castration Rate At Week 1 Day 4 (Day 4) [ Time Frame: At Week 1 Day 4 (Day 4) ]
    Castration rate defined as the cumulative probability of testosterone suppression to < 20 ng/dL. The rate was estimated for each treatment group using the Kaplan-Meier method and reported as percentage of participants.
11. Sustained Profound Castration Rate From Week 25 Day 1 Through Week 49 Day 1 [ Time Frame: Week 25 Day 1 (Day 169) through Week 49 Day 1 (Day 337) ]
    Sustained profound castration rate was defined as the cumulative probability of testosterone suppression to < 20 ng/dL. The rate was estimated by the Kaplan-Meier method and reported as percentage of participants.
12. Undetectable PSA Rate [ Time Frame: Week 25 Day 1 (Day 169) ]
    Defined as the proportion of participants with PSA concentration < 0.02 ng/milliliter (mL).The rate was estimated by the Kaplan-Meier method and reported as percentage of participants.
13. Rate Of PSA Progression-free Survival [ Time Frame: Week 49 Day 1 (Day 337) ]
    PSA progression was defined as the first increase in PSA of 25% or greater and 2 ng/mL or greater above the nadir with confirmation by a second consecutive PSA measurement at least 3 weeks later. For participants without declining PSA from baseline, a PSA increase of ≥ 25% and ≥ 2 ng/mL from baseline beyond 12 weeks was considered PSA progression. The rate of progression-free survival was estimated using the Kaplan-Meier method and reported as percentage of participants.
14. Change From Baseline In Quality Of Life (QoL) Total Score As Assessed By The Global Health Domain Of The European Organisation Of Research And Treatment Of Cancer (EORTC)-Quality Of Life Questionnaire (QLQ)-C30 [ Time Frame: Baseline, Week 49 Day 1 (Day 337) ]
    The EORTC QLQ-C30 core measurement was used to capture distal outcomes, including physical, social functioning, and overall health-related quality of life. The questionnaire incorporates 30 questions comprising nine multi-item scales: 5 functional scales (physical, role, cognitive, emotional, and social); 3 symptom scales (fatigue, pain, and nausea and vomiting); and a global health and quality of life scale. All raw domain scores are linearly transformed to a 0-100 scale. The global health and quality of life domain is presented. An increase in activity or functioning scores indicates improvement (higher/healthier level of functioning) and a decrease in symptom scores indicates improvement (lower level of symptoms/problems).
15. Change From Baseline In QoL Total Score For Remaining Domain Scores As Assessed By The EORTC-QLQ-C30 [ Time Frame: Baseline, Week 49 Day 1 (Day 337) ]
    The EORTC QLQ-C30 core measurement was used to capture distal outcomes, including physical, social functioning, and overall health-related quality of life. The questionnaire incorporates 30 questions comprising nine multi-item scales: 5 functional scales (physical, role, cognitive, emotional, and social); 3 symptom scales (fatigue, pain, and nausea and vomiting); and a global health and quality of life scale. All raw domain scores are linearly transformed to a 0-100 scale. All domains except for the global health and quality are presented. An increase in activity or functioning scores indicates improvement (higher/healthier level of functioning) and a decrease in symptom scores indicates improvement (lower level of symptoms/problems).
16. Change From Baseline In QoL Total Score As Assessed By The EORTC-QLQ-PR25 Sexual Activity And Functioning And Hormonal-Treatment-Related Symptom Subdomains [ Time Frame: Baseline, Week 49 Day 1 (Day 337) ]
    Subscales for assessment of hormonal treatment-related symptoms (6 items) and sexual activity and function (6 items) from the EORTC-QLQ-PR25 25-item prostate cancer module of the EORTC are presented. Questions used 4 point scale (1 'Not at all' to 4 'Very much'). All raw domain scores are linearly transformed to a 0-100 scale. An increase in activity or functioning scores indicates improvement (higher/healthier level of functioning) and a decrease in symptom scores indicates improvement (lower level of symptoms/problems).
17. Change From Baseline In QoL Total Score For Urinary And Bowel Symptoms Domains As Assessed By The EORTC-QLQ-PR25 [ Time Frame: Baseline, Week 49 Day 1 (Day 337) ]
    Subscale assessments of urinary symptoms (9 items) and bowel symptoms (4 items) from the EORTC-QLQ-PR25 25-item prostate cancer module of the EORTC are presented. Questions used 4 point scale (1 'Not at all' to 4 'Very much'). All raw domain scores are linearly transformed to a 0-100 scale. A decrease in symptom scores indicates improvement (lower level of symptoms/problems).
18. Change From Baseline In QoL Total Score As Assessed By The European Quality Of Life 5-Dimension 5-Level Questionnaire (EuroQoL EQ-5D-5L) [ Time Frame: Baseline, Week 49 Day 1 (Day 337) ]
    The EuroQoL EQ-5D-5L comprises 5 dimensions (mobility, self-care, usual activities, pain/discomfort, and anxiety/depression). Each dimension has 5 levels: no problems (1 as numerical score), slight problems (2 as numerical score), moderate problems (3 as numerical score), severe problems (4 as numerical score), and extreme problems (5 as numerical score). The total score ranges from 0 to 100. A decrease in score indicates improvement.
19. Percent Change From Baseline In Serum Concentrations Of Luteinizing Hormone [ Time Frame: Week 1 Day 4 (Day 4), Week 5 Day 1 (Day 29), Week 25 Day 1 (Day 169), and Week 49 Day 1 (Day 337) ]
    Blood samples were collected from participants for hormonal measurements.
20. Percent Change From Baseline In Serum Concentrations Of FSH [ Time Frame: Week 1 Day 4 (Day 4), Week 5 Day 1 (Day 29), Week 25 Day 1 (Day 169), and Week 49 Day 1 (Day 337) ]
    Blood samples were collected from participants for hormonal measurements.
21. Percent Change From Baseline In Serum Concentrations Of Dihydrotestosterone [ Time Frame: Week 5 Day 1 (Day 29), Week 25 Day 1 (Day 169), and Week 49 Day 1 (Day 337) ]
    Blood samples were collected from participants for hormonal measurements.
22. Percent Change From Baseline In Serum Concentrations Of Sex Hormone-Binding Globulin [ Time Frame: Week 5 Day 1 (Day 29), Week 25 Day 1 (Day 169), and Week 49 Day 1 (Day 337) ]
    Blood samples were collected from participants for hormonal measurements.
23. Maximum Observed Plasma Concentration (Cmax) Of Relugolix [ Time Frame: Predose and 0.5, 1, 2, 4, 6, 8, 12, and 24 hours postdose on Day 1 and Week 2 ]
    The Cmax of relugolix was determined for single and repeat doses in subsets of participants from Japan. Single dose pharmacokinetics (PK) was assessed on Day 1 following an initial 360 mg dose of relugolix. Repeat dose PK was assessed following repeat dosing of relugolix 120 mg once daily for 2 weeks.
24. Area Under The Concentration-Time Curve (AUC0-τ) Of Relugolix [ Time Frame: Predose and 0.5, 1, 2, 4, 6, 8, 12, and 24 hours postdose on Day 1 and Week 2 ]
    The AUC0-τ of relugolix was determined for single and repeat doses in subsets of participants from Japan. Single dose PK was assessed on Day 1 following an initial 360 mg dose of relugolix. Repeat dose PK was assessed following repeat dosing of relugolix 120 mg once daily for 2 weeks.
25. Time To Maximum Observed Plasma Concentration (Tmax) Of Relugolix [ Time Frame: Predose and 0.5, 1, 2, 4, 6, 8, 12, and 24 hours postdose on Day 1 and Week 2 ]
    The Tmax of relugolix was determined for single and repeat doses in subsets of participants from Japan. Single dose PK was assessed on Day 1 following an initial 360 mg dose of relugolix. Repeat dose PK was assessed following repeat dosing of relugolix 120 mg once daily for 2 weeks.

Other Outcome Measures:

1. Percentage of Participants Who Experienced Major Adverse Cardiovascular Events (MACE) [ Time Frame: From Week 5 Day 1 (Day 29) to Week 49 Day 1 (Day 337) ]
   MACE were defined as nonfatal myocardial infarction, nonfatal stroke, and death from any cause.

Eligibility Criteria

• Ages Eligible for Study: 18 Years and older (Adult, Older Adult)
• Sexes Eligible for Study: Male
• Accepts Healthy Volunteers: No

Criteria

Key Inclusion Criteria:

1. Has histologically or cytologically confirmed diagnosis of adenocarcinoma of the prostate.

2. Is a candidate for, in the opinion of the investigator, at least 1 year of continuous androgen deprivation therapy for the management of androgen-sensitive advanced prostate cancer with 1 of the following clinical disease state presentations:

   1. Evidence of biochemical (PSA) or clinical relapse following local primary intervention with curative intent, such as surgery, radiation therapy, cryotherapy, or high-frequency ultrasound and not a candidate for salvage treatment by surgery; or
   2. Newly diagnosed androgen-sensitive metastatic disease; or
   3. Advanced localized disease unlikely to be cured by local primary intervention with either surgery or radiation with curative intent.
3. Has a serum testosterone at the Screening visit of ≥ 150 ng/dL (5.2 nanomoles [nmol]/liter [L]).
4. Has a serum PSA concentration at the Screening visit of > 2.0 ng/milliliter (mL) (2.0 microgram [μg]/L), or, when applicable, post radical prostatectomy of > 0.2 ng/mL (0.2 μg/L) or post radiotherapy, cryotherapy, or high frequency ultrasound > 2.0 ng/mL (2.0 μg/L) above the post interventional nadir.
5. Has an Eastern Cooperative Oncology Group performance status of 0 or 1 at initial screening and at baseline.

Key Exclusion Criteria:

1. In the investigator's opinion, is likely to require chemotherapy or surgical therapy for symptomatic disease management within 2 months of initiating androgen deprivation therapy.
2. Previously received gonadotropin-releasing hormone analog or other form of androgen deprivation therapy (estrogen or antiandrogen) for > 18 months total duration. If androgen deprivation therapy was received for ≤ 18 months total duration, then that therapy must have been completed at least 3 months prior to baseline. If the dosing interval of the depot is longer than 3 months, then the prior androgen deprivation therapy must have been completed at least as long as the dosing interval of the depot.
3. Previous systemic cytotoxic treatment for prostate cancer (for example, taxane-based regimen).
4. Metastases to brain per prior clinical evaluation.
5. Participants with myocardial infarction, unstable symptomatic ischemic heart disease, cerebrovascular events, or any significant cardiac condition within the prior 6 months.
6. Active conduction system abnormalities.
7. Uncontrolled hypertension.

Contacts and Locations

Locations

United States, Arizona

Tucson

Tucson, Arizona, United States, 85741

United States, California

Orange

Orange, California, United States, 92868

United States, Colorado

Denver

Denver, Colorado, United States, 80211

United States, Florida

Pompano Beach

Pompano Beach, Florida, United States, 33060

United States, Indiana

Jeffersonville

Jeffersonville, Indiana, United States, 47130

United States, Iowa

Des Moines

Des Moines, Iowa, United States, 50266

United States, Kansas

Wichita

Wichita, Kansas, United States, 67226

United States, Maryland

Baltimore

Baltimore, Maryland, United States, 21204

United States, Michigan

Troy

Troy, Michigan, United States, 48084

United States, Nebraska

Omaha

Omaha, Nebraska, United States, 68130

United States, Nevada

Las Vegas

Las Vegas, Nevada, United States, 89135

United States, New Jersey

Brick

Brick, New Jersey, United States, 08724

United States, New Mexico

Albuquerque

Albuquerque, New Mexico, United States, 87109

United States, New York

Albany

Albany, New York, United States, 12208

Garden City

Garden City, New York, United States, 11530

Plainview

Plainview, New York, United States, 11803

Poughkeepsie

Poughkeepsie, New York, United States, 12601

Syracuse

Syracuse, New York, United States, 13210

United States, North Carolina

Durham

Durham, North Carolina, United States, 27710

Greensboro

Greensboro, North Carolina, United States, 27403

United States, Ohio

Cincinnati

Cincinnati, Ohio, United States, 45212

Middleburg Heights

Middleburg Heights, Ohio, United States, 44130

United States, Oklahoma

Oklahoma City

Oklahoma City, Oklahoma, United States, 73104

United States, Pennsylvania

Lancaster

Lancaster, Pennsylvania, United States, 17604

United States, South Carolina

Myrtle Beach

Myrtle Beach, South Carolina, United States, 29572

United States, Tennessee

Nashville

Nashville, Tennessee, United States, 37209

United States, Texas

San Antonio

San Antonio, Texas, United States, 78258

Australia, New South Wales

Camperdown

Camperdown, New South Wales, Australia, 2050

Tweed Heads

Tweed Heads, New South Wales, Australia, 2485

Wahroonga

Wahroonga, New South Wales, Australia, 2076

Australia, Queensland

Redcliffe

Redcliffe, Queensland, Australia, 4020

Southport

Southport, Queensland, Australia, 4215

Austria

Linz

Linz, Austria, 402

Belgium

Gent

Gent, Oost-Vlaanderen, Belgium, 9000

Brussels

Brussels, Belgium, 1200

Kortrijk

Kortrijk, Belgium, 8500

Brazil

Itabuna

Itabuna, Bahia, Brazil, 45602-650

Salvador

Salvador, Bahia, Brazil, 41253-190

Salvador

Salvador, Bahia, Brazil, 41820-021

Teresina

Teresina, Piauí, Brazil, 64001-280

Natal

Natal, Rio Grande Do Norte, Brazil, 59062-000

Ijuí

Ijuí, Rio Grande Do Sul, Brazil, 98700

Passo Fundo

Passo Fundo, Rio Grande Do Sul, Brazil, 99010-080

Porto Alegre

Porto Alegre, Rio Grande Do Sul, Brazil, 90110-270

Porto Alegre

Porto Alegre, Rio Grande Do Sul, Brazil, 90430-090

Joinville

Joinville, Santa Catarina, Brazil, 89201-260

São José Do Rio Preto

São José Do Rio Preto, Sao Paulo, Brazil, 15090-000

Curitiba

Curitiba, Brazil, 81520-060

Canada, Alberta

Calgary

Calgary, Alberta, Canada, T2V4R6

Canada, British Columbia

Vancouver

Vancouver, British Columbia, Canada, V5Z1M9

Canada, Nova Scotia

Halifax

Halifax, Nova Scotia, Canada, B3H2Y9

Canada, Ontario

Hamilton

Hamilton, Ontario, Canada, L8N4A6

London

London, Ontario, Canada, N6A4G5

Canada, Quebec

Montreal

Montréal, Quebec, Canada, H2X0A9

Sherbrooke

Sherbrooke, Quebec, Canada, J1H5N4

Canada

Quebec

Quebec, Canada, G1R 3S3

China, Jiangsu

Nanjing

Nanjing, Jiangsu, China, 210008

China, Jilin

Changchun

Chang chun, Jilin, China, 130021

China, Shanghai

Shanghai

Shanghai, Shanghai, China, 020043

China, Shanxi

Taiyuan

Taiyuan, Shanxi, China, 030001

China

Beijing

Beijing, China, 100041

Beijing

Beijing, China, 100050

Beijing Shi

Beijing, China, 100730

Chongqing

Chongqing, China, 400030

Hangzhou

Hangzhou, China, 310003

Lanzhou

Lanzhou, China, 730030

Nanchang

Nanchang, China, 330006

Shanghai

Shanghai, China, 200040

Suzhou

Suzhou, China, 215004

Denmark

Alborg

Aalborg, Denmark, DK-9000

Aarhus

Aarhus, Denmark, 8200

Herlev

Herlev, Denmark, 2730

Vejle

Vejle, Denmark, DK-7100

Finland

Helsinki

Helsinki, Finland, FI-00029

Seinajoki

Seinäjoki, Finland, FI-60220

Tampere

Tampere, Finland, FI-33520

Turku

Turku, Finland, FI-20520

France

Strasbourg

Strasbourg, Bas-Rhin, France, 67091

Pierre Benite

Pierre-Bénite, Rhone, France, 69495

Creteil

Créteil, Val-de-Marne, France, 94010

Lyon

Lyon, France, 69437

Germany

Emmendingen

Emmendingen, Baden-Wurttemberg, Germany, 79312

Planegg

Planegg, Bayern, Germany, 82152

Braunschweig

Braunschweig, Niedersachsen, Germany, 38100

Dresden

Dresden, Germany, 01307

Lubeck

Lübeck, Germany, 23538

Munster

Münster, Germany, 48149

Italy

Meldola

Meldola, Emilia-Romagna, Italy, 47014

Rome

Rome, Lazio, Italy, 00152

Cremona

Cremona, Lombardia, Italy, 26100

Candiolo

Candiolo, Piemonte, Italy, 10060

Orbassano

Orbassano, Piemonte, Italy, 10043

Arezzo

Arezzo, Toscana, Italy, 52100

Milano

Milano, Italy, 20162

Japan

Kanazawa-shi

Kanazawa-shi, Isikawa, Japan, 920-8641

Yokohama

Yokohama, Kanagawa, Japan, 232-0024

Sendai

Sendai, Miyagi, Japan, 9808574

Sendai

Sendai, Miyagi, Japan, 9818563

Suita

Suita, Osaka, Japan, 565-0871

Osaka-sayama

Ōsaka-sayama, Osaka, Japan, 589-8511

Bunkyō-Ku

Bunkyō-Ku, Tokyo, Japan, 113-8655

Nakano-ku

Nakano-ku, Tokyo, Japan, 164-8541

Sumida-ku

Sumida-ku, Tokyo, Japan, 130-8587

Chiba

Chiba, Japan, 260-0801

Fukuoka

Fukuoka, Japan, 812-0033

Hiroshima

Hiroshima, Japan, 730-8518

Kita-gun

Kita, Japan, 761-0793

Kyoto

Kyoto, Japan, 606-8507

Maebashi

Maebashi, Japan, 371-8511

Nagasaki

Nagasaki, Japan, 852-8501

Osaka

Osaka, Japan, 541-8567

Sapporo

Sapporo, Japan, 003-0804

Tokyo

Tokyo, Japan, 285-8741

Ube

Ube, Japan, 7558505

Korea, Republic of

Goyang-Si

Goyang-si, Gyeonggido, Korea, Republic of, 10408

Busan

Busan, Korea, Republic of, 49241

Daegu

Daegu, Korea, Republic of, 41404

Hwasun

Hwasun, Korea, Republic of, 58128

Seoul

Seoul, Korea, Republic of, 03080

Seoul

Seoul, Korea, Republic of, 05505

Seoul

Seoul, Korea, Republic of, 06273

Seoul

Seoul, Korea, Republic of, 06351

Netherlands

Eindhoven

Eindhoven, Noord Brabant, Netherlands, 5623EJ

Amsterdam

Amsterdam, Noord Holland, Netherlands, 1105AZ

Sneek

Sneek, Netherlands, 8601 ZK

New Zealand

Christchurch

Christchurch, New Zealand, 8013

Dunedin

Dunedin, New Zealand, 9016

Hamilton

Hamilton, New Zealand, 3204

Tauranga

Tauranga, New Zealand, 3112

Poland

Lublin

Lublin, Lubelskie, Poland, 20-582

Siedlce

Siedlce, Mazowieckie, Poland, 08-110

Warszawa

Warszawa, Mazowieckie, Poland, 02-797

Gdynia

Gdynia, Pomorskie, Poland, 81-519

Katowice

Katowice, Poland, 40611

Slovakia

Bratislava

Bratislava, Slovakia, 851 05

Kosice

Košice, Slovakia, 040 01

Kosice

Košice, Slovakia, 041 91

Martin

Martin, Slovakia, 036 59

Nitra

Nitra, Slovakia, 949 01

Poprad

Poprad, Slovakia, 058 45

Presov

Prešov, Slovakia, 080 01

Trencin

Trenčín, Slovakia, 911 01

Sala

Šaľa, Slovakia, 927 01

Spain

A Coruna

A Coruña, A Coruna, Spain, 15706

Oviedo

Oviedo, Asturias, Spain, 33011

Barcelona

Barcelona, Spain, 08036

Madrid

Madrid, Spain, 28007

Madrid

Madrid, Spain, 28041

Salamanca

Salamanca, Spain, 37007

Valencia

Valencia, Spain, 46009

Sweden

Orebro

Örebro, Orebro Ian, Sweden, SE-70185

Stockholm

Stockholm, Sodermandlands Ian, Sweden, SE-17176

Uppsala

Uppsala, Uppsala Lan, Sweden, SE-751-85

Malmo

Malmö, Sweden, SE-20502

Taiwan

Kaohsiung City

Kaohsiung City, Taiwan, 807

Taipei

Taipei, Taiwan, 100

Taipei

Taipei, Taiwan, 111

Taipei

Taipei, Taiwan, 11490

United Kingdom

Exeter

Exeter, Devon, United Kingdom, EX2 5DW

Scunthorpe

Scunthorpe, North Lincolnshire, United Kingdom, DN157BH

Nottingham

Nottingham, United Kingdom, NG5 1PB

Rhyl

Rhyl, United Kingdom, LL18 5UJ

Sponsors and Collaborators

Myovant Sciences GmbH

Investigators

• Study Director: Myovant Medical Monitor; Myovant Sciences

  Study Documents (Full-Text)

Documents provided by Myovant Sciences GmbH:

Study Protocol  [PDF] October 23, 2018

Statistical Analysis Plan  [PDF] November 7, 2019

More Information

Publications:

Shore ND, Saad F, Cookson MS, George DJ, Saltzstein DR, Tutrone R, Akaza H, Bossi A, van Veenhuyzen DF, Selby B, Fan X, Kang V, Walling J, Tombal B; HERO Study Investigators. Oral Relugolix for Androgen-Deprivation Therapy in Advanced Prostate Cancer. N Engl J Med. 2020 Jun 4;382(23):2187-2196. doi: 10.1056/NEJMoa2004325. Epub 2020 May 29.

Publications automatically indexed to this study by ClinicalTrials.gov Identifier (NCT Number):

Shore ND, Sutton J. Plain language summary of the HERO study comparing relugolix with leuprolide for men with advanced prostate cancer. Future Oncol. 2022 Jul;18(21):2575-2584. doi: 10.2217/fon-2022-0172. Epub 2022 May 19.

• Responsible Party: Myovant Sciences GmbH
• ClinicalTrials.gov Identifier: NCT03085095
• Other Study ID Numbers: MVT-601-3201; 2017-000160-15 ( EudraCT Number )
• First Posted: March 21, 2017
• Results First Posted: March 25, 2021
• Last Update Posted: January 18, 2022
• Last Verified: January 2022

Individual Participant Data (IPD) Sharing Statement:

• Plan to Share IPD: No

• Studies a U.S. FDA-regulated Drug Product: Yes
• Studies a U.S. FDA-regulated Device Product: No
• Product Manufactured in and Exported from the U.S.: No

Additional relevant MeSH terms:

Prostatic Neoplasms; Genital Neoplasms, Male; Urogenital Neoplasms; Neoplasms by Site; Neoplasms; Genital Diseases, Male; Genital Diseases; Urogenital Diseases; Prostatic Diseases; Male Urogenital Diseases; Leuprolide; Relugolix; Fertility Agents, Female; Fertility Agents; Reproductive Control Agents; Physiological Effects of Drugs; Antineoplastic Agents, Hormonal; Antineoplastic Agents; Androgen Antagonists; Hormone Antagonists; Hormones, Hormone Substitutes, and Hormone Antagonists