THE FIRST AND ONLY ARI FDA-APPROVED FOR USE WITH AND WITHOUT DOCETAXEL IN mCSPC^1-4

mCSPC

NUBEQA with ADT demonstrated superior efficacy in mCSPC vs ADT alone^1,5

Statistically significant reduction in the risk of progression or death

Graph showing risk of progression or death with NUBEQA plus ADT vs ADT alone, from the ARANOTE study

THE MEDIAN FOLLOW-UP TIME WAS 25.3 MONTHS FOR NUBEQA + ADT AND 25.0 MONTHS FOR PLACEBO + ADT⁵

At 24 months, 70.3% of patients receiving NUBEQA + ADT vs 52.1% of patients receiving placebo + ADT remained free of radiological progression and were alive after treatment began^5†

*rPFS was defined as the time from randomization to radiological disease progression or death by central blinded review. Radiographic disease progression was defined by identification of 2 or more new bone lesions on a bone scan with confirmation (Prostate Cancer Working Group 3 criteria) and/or progression in soft tissue disease.¹

^†Landmark analysis, limitations include: Ignores all events occurring before the landmark time; omission of high proportion of events with corresponding loss of power. The conditional property of a landmark analysis makes it difficult to generalize its results.

The randomized, double-blind, placebo-controlled phase III ARANOTE trial was designed to assess the efficacy and safety of NUBEQA plus ADT in patients with mCSPC. A total of 669 patients were randomized 2:1 to receive either 600 mg of NUBEQA (N=446) twice daily or placebo (N=223) twice daily in addition to ADT. rPFS was the study primary endpoint.

ADT=androgen deprivation therapy; ARI=androgen receptor inhibitor; CI=confidence interval; HR=hazard ratio; mCSPC=metastatic castration-sensitive prostate cancer; NR=not reached; rPFS=radiological progression-free survival.

ARANOTE Safety Results

Patients receiving NUBEQA stayed on treatment 1.4x longer compared with ADT alone^1,5,6

Patients stayed on NUBEQA for a median duration of therapy of 2+ years concurrent with ADT

Graph showing treatment duration with NUBEQA + ADT compared to ADT alone, based on ARANOTE study.

At the data cutoff date for the primary analysis (June 7, 2024), the median treatment duration was 24.2 months in the NUBEQA group compared with 17.3 months in the placebo group, with a greater proportion of patients in the NUBEQA group (53.8%) still receiving study treatment than in the placebo group (28.3%). The median follow-up time was 25.3 months in the NUBEQA group and 25.0 months in the placebo group.⁵

CHOOSE NUBEQA FOR YOUR PATIENTS WITH mCSPC

Practice Resources

ARANOTE Safety Results

ARASENS:
NUBEQA + ADT + DOCETAXEL

Help patients with mCSPC live longer. NUBEQA in combination with docetaxel significantly reduced the risk of death by nearly a third compared with docetaxel and ADT alone^1,5

Start with a short course of docetaxel (every 3 weeks for 6 cycles)

Graph of risk of death with NUBEQA with docetaxel and ADT vs docetaxel and ADT alone, from the ARASENS study.

*Landmark analysis, limitations include: Ignores all events occurring before the landmark time; omission of high proportion of events with corresponding loss of power. The conditional property of a landmark analysis makes it difficult to generalize its results.

ADT=androgen deprivation therapy; CI=confidence interval; HR=hazard ratio; NE=not estimable; OS=overall survival.

ARASENS Safety Results

Time to disease progression—mCRPC

In ARASENS, time to mCRPC was a secondary endpoint and assessed by PCWG3 criteria^5,6:

The time from randomization to occurrence of the following events, whichever occurred first: PSA progression with serum testosterone at a castrate level (<0.5 ng/mL) or radiographic progression of soft-tissue, visceral, or bone lesions; radiographic progression by soft-tissue/visceral lesions was determined according to RECIST version 1.1
PSA was assessed by central review, however radiographic progression was determined by investigator assessment

Graph showing risk reduction in time to CRPC comparing NUBEQA with docetaxel and ADT vs docetaxel and ADT alone, from the ARASENS study

ADT=androgen deprivation therapy; CI=confidence interval; CRPC=castration-resistant prostate cancer; HR=hazard ratio; mCRPC=metastatic castration-resistant prostate cancer; NE=not estimable; PCWG3=Prostate Cancer Working Group 3; PSA=prostate-specific antigen; RECIST=Response Evaluation Criteria in Solid Tumors.

EFFICACY IN ADDITIONAL SECONDARY ENDPOINTS

Secondary endpoint results of the ARASENS study^1,5

Secondary endpoint results of the NUBEQA® (darolutamide) ARASENS study

Secondary endpoints were tested with a hierarchical gatekeeping procedure in the order shown above only if the primary endpoint and each preceding secondary endpoint in the hierarchy were statistically significant⁵

^†Time to pain progression was defined as the time from randomization to the time of pain progression. Pain progression is defined as¹:

An increase of 2 or more points in the “worst pain in 24 hours” score (WPS) from nadir observed at 2 consecutive evaluations at least 4 weeks apart, or initiation of short- or long-acting opioid use for pain for at least 7 consecutive days, for asymptomatic patients (WPS=0) at baseline
An increase of 2 or more points in the “worst pain in 24 hours” score (WPS) from nadir observed at 2 consecutive evaluations at least 4 weeks apart, and a WPS of 4 or greater, or initiation of short- or long-acting opioid use for pain for at least 7 consecutive days, for symptomatic patients (WPS ≥1) at baseline

After a short course of concurrent docetaxel, patients receiving NUBEQA stayed on treatment nearly 2.5x longer compared with ADT alone¹

Patients stayed on NUBEQA for a median duration of therapy of 3+ years after a short course of concurrent docetaxel

Median treatment duration at time of data cutoff

Graph showing treatment duration with NUBEQA + ADT + docetaxel compared to ADT alone, based on ARASENS study

Within 6 weeks of starting NUBEQA, start docetaxel at 75 mg/m² once every 3 weeks for 6 cycles.¹

76% of patients (374/495) taking placebo + docetaxel received subsequent life-prolonging systemic antineoplastic therapies^5,6§

§At the data cutoff date (October 25, 2021), 45.9% of patients in the darolutamide group and 19.1% of patients in the placebo group were receiving ongoing study treatment. 495 patients entered active or long-term (survival) follow-up, plus 1 patient who did not enter follow-up but received subsequent therapy. Patients could receive more than 1 subsequent life-prolonging systemic therapy.^5,6

CHOOSE NUBEQA FOR YOUR PATIENTS WITH mCSPC

Practice Resources

ADT=androgen deprivation therapy; ARI=androgen receptor inhibitor; CI=confidence interval; HR=hazard ratio; mCRPC=metastatic castration-resistant prostate cancer; mCSPC=metastatic castration-sensitive prostate cancer; NE=not estimable; OS=overall survival; PCWG3=Prostate Cancer Working Group 3 criteria; PSA=prostate-specific antigen; RECIST=Response Evaluation Criteria In Solid Tumors.

ARASENS Safety Results

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Indications

NUBEQA is an androgen receptor inhibitor indicated for the treatment of adult patients with:

non-metastatic castration resistant prostate cancer (nmCRPC)
metastatic castration-sensitive prostate cancer (mCSPC)
metastatic castration-sensitive prostate cancer (mCSPC) in combination with docetaxel

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Important Safety Information

Warnings & Precautions

Ischemic Heart Disease – Ischemic heart disease, including fatal cases, occurred in patients receiving NUBEQA.

In a pooled analysis of ARAMIS and ARANOTE, ischemic heart disease occurred in 3.4% of patients receiving NUBEQA and 2.2% receiving placebo, including Grade 3-4 events in 1.4% and 0.3%, respectively. Ischemic events led to death in 0.4% of patients receiving NUBEQA and 0.4% receiving placebo.

In ARASENS, ischemic heart disease occurred in 3.2% of patients receiving NUBEQA with docetaxel and 2% receiving placebo with docetaxel, including Grade 3-4 events in 1.3% and 1.1%, respectively. Ischemic events led to death in 0.3% of patients receiving NUBEQA with docetaxel and 0% receiving placebo with docetaxel.

Monitor for signs and symptoms of ischemic heart disease. Optimize management of cardiovascular risk factors, such as hypertension, diabetes, or dyslipidemia. Discontinue NUBEQA for Grade 3-4 ischemic heart disease.

Seizure – Seizure occurred in patients receiving NUBEQA.

In a pooled analysis of ARAMIS and ARANOTE, Grade 1-3 seizure occurred in 0.2% of patients receiving NUBEQA. Seizure occurred from 261 to 665 days after initiation of NUBEQA.

In ARASENS, seizure occurred in 0.8% of patients receiving NUBEQA with docetaxel, including two Grade 3 events. Seizure occurred from 38 to 1754 days after initiation of NUBEQA.

It is unknown whether anti-epileptic medications will prevent seizures with NUBEQA. Advise patients of the risk of developing a seizure while receiving NUBEQA and of engaging in any activity where sudden loss of consciousness could cause harm to themselves or others. Consider discontinuation of NUBEQA in patients who develop a seizure during treatment.

Embryo-Fetal Toxicity – The safety and efficacy of NUBEQA have not been established in females. NUBEQA can cause fetal harm and loss of pregnancy. Advise males with female partners of reproductive potential to use effective contraception during treatment with NUBEQA and for 1 week after the last dose.

Adverse Reactions

In ARAMIS, serious adverse reactions occurred in 25% of patients receiving NUBEQA and in 20% of patients receiving placebo. Serious adverse reactions in ≥1% of patients who received NUBEQA included urinary retention, pneumonia, and hematuria. Fatal adverse reactions occurred in 3.9% of patients receiving NUBEQA and 3.2% of patients receiving placebo. Fatal adverse reactions that occurred in ≥2 patients who received NUBEQA included death (0.4%), cardiac failure (0.3%), cardiac arrest (0.2%), general physical health deterioration (0.2%), and pulmonary embolism (0.2%). The most common (>2% with a ≥2% increase compared to placebo) adverse reactions, including laboratory test abnormalities, were increased AST (23%), decreased neutrophil count (20%), fatigue (16%), increased bilirubin (16%), pain in extremity (6%), and rash (4%). Clinically relevant adverse reactions occurring in 2% or more of patients treated with NUBEQA included ischemic heart disease (4%) and heart failure (2.1%).

In ARANOTE, serious adverse reactions occurred in 24% of patients receiving NUBEQA. Serious adverse reactions in ≥1% of patients who received NUBEQA included pneumonia (2%), urinary tract infection (1.8%), musculoskeletal pain (1.6%), hemorrhage (1.6%), arrhythmias (1.3%), and spinal cord compression (1.1%). Fatal adverse reactions occurred in 4.7% of patients receiving NUBEQA and those that occurred in ≥2 patients included sepsis (1.1%), craniocerebral injury (0.4%), and myocardial infarction (0.4%). The most common (≥10% with a ≥2% increase compared to placebo) adverse reaction is urinary tract infection (12%). The most common laboratory test abnormalities (≥15% with a ≥5% increase over placebo) are increased AST (32%), increased ALT (28%), increased bilirubin (17%), and decreased neutrophil count (16%). Clinically relevant adverse reactions in <10% of patients who received NUBEQA included arrhythmia (8.8%), pneumonia (3.6%), and myocardial infarction (0.7%).

In ARASENS, serious adverse reactions occurred in 45% of patients receiving NUBEQA with docetaxel. Serious adverse reactions in ≥2% of patients who received NUBEQA with docetaxel included febrile neutropenia (6%), neutrophil count decreased (2.8%), musculoskeletal pain (2.6%) and pneumonia (2.6%). Fatal adverse reactions occurred in 4% of patients receiving NUBEQA with docetaxel. Fatal adverse reactions in ≥2 patients who received NUBEQA included COVID-19/COVID-19 pneumonia (0.8%), myocardial infarction (0.3%), and sudden death (0.3%). The most common (≥10% with a ≥2% increase over placebo with docetaxel) adverse reactions are constipation (23%), rash (20%), decreased appetite (19%), hemorrhage (18%), increased weight (18%), and hypertension (14%). The most common laboratory test abnormalities (≥30%) are anemia (72%), hyperglycemia (57%), decreased lymphocyte count (52%), decreased neutrophil count (49%), increased AST (40%), increased ALT (37%), and hypocalcemia (31%). Clinically relevant adverse reactions in <10% of patients who received NUBEQA with docetaxel included fractures (8%), ischemic heart disease (3.2%), seizures (0.6%), and drug-induced liver injury (0.3%).

Drug Interactions

Effect of Other Drugs on NUBEQA – Concomitant use of NUBEQA with a combined P-gp and strong or moderate CYP3A4 inducer decreases darolutamide exposure which may decrease NUBEQA activity. Avoid concomitant use of NUBEQA with combined P-gp and strong or moderate CYP3A4 inducers.

Concomitant use of NUBEQA with a combined P-gp and strong CYP3A4 inhibitor increases darolutamide exposure which may increase the risk of NUBEQA adverse reactions. Monitor patients more frequently for NUBEQA adverse reactions and modify NUBEQA dosage as needed.

Effects of NUBEQA on Other Drugs – NUBEQA is an inhibitor of BCRP transporter. Concomitant use of NUBEQA increases the AUC and C_max of BCRP substrates, which may increase the risk of BCRP substrate-related toxicities. Avoid concomitant use with drugs that are BCRP substrates where possible. If used together, monitor patients more frequently for adverse reactions, and consider dose reduction of the BCRP substrate drug.

NUBEQA is an inhibitor of OATP1B1 and OATP1B3 transporters. Concomitant use of NUBEQA may increase the plasma concentrations of OATP1B1 or OATP1B3 substrates. Monitor patients more frequently for adverse reactions of these drugs and consider dose reduction while patients are taking NUBEQA.

Review the Prescribing Information of drugs that are BCRP, OATP1B1, and OATP1B3 substrates when used concomitantly with NUBEQA.

Please see the full Prescribing Information.

You are encouraged to report side effects or quality complaints of products to the FDA by visiting www.fda.gov/medwatch or calling 1-800-FDA-1088.

References: 1. NUBEQA (darolutamide) [prescribing information]. Whippany, NJ: Bayer HealthCare Pharmaceuticals, Inc.; June 2025. 2. Erleada (apalutamide) [prescribing information]. Horsham, PA: Janssen Products, LP; August 2024. 3. Xtandi (enzalutamide) [prescribing information]. Northbrook, IL: Astellas Pharma US, Inc.; January 2025. 4. Zytiga (abiraterone acetate) [prescribing information]. Horsham, PA: Janssen Biotech, Inc.; November 2024. 5. Saad F, Vjaters E, Shore N, et al; ARANOTE Study Investigators. Darolutamide in combination with androgen-deprivation therapy in patients with metastatic hormone-sensitive prostate cancer from the Phase III ARANOTE trial. J Clin Oncol. 2024;42(36):4‌2‌7‌1‌-‌4‌2‌8‌1. 6. Data on file. Bayer HealthCare Pharmaceuticals, Inc.; Whippany, NJ.

References: 1. NUBEQA (darolutamide) [prescribing information]. Whippany, NJ: Bayer HealthCare Pharmaceuticals, Inc.; June 2025. 2. Erleada (apalutamide) [prescribing information]. Horsham, PA: Janssen Products, LP; August 2024. 3. Xtandi (enzalutamide) [prescribing information]. Northbrook, IL: Astellas Pharma US, Inc.; January 2025. 4. Zytiga (abiraterone acetate) [prescribing information]. Horsham, PA: Janssen Biotech, Inc.; November 2024. 5. Smith MR, Hussain M, Saad F, et al; ARASENS Trial Investigators. Darolutamide and survival in metastatic, hormone-sensitive prostate cancer. N Engl J Med. 2022;386(12):1132-1142. 6. Data on file. Bayer HealthCare Pharmaceuticals, Inc.; Whippany, NJ.

THE FIRST AND ONLY ARI FDA-APPROVED FOR USE WITH AND WITHOUT DOCETAXEL IN mCSPC^1-4

NUBEQA with ADT demonstrated superior efficacy in mCSPC vs ADT alone^1,5

Patients receiving NUBEQA stayed on treatment 1.4x longer compared with ADT alone^1,5,6

CHOOSE NUBEQA FOR YOUR PATIENTS WITH mCSPC