Efficacy and Safety Evaluation of Darolutamide+ADT Adjuvant After Radical Prostatectomy (RP) Without ePLND, in High-risk Prostate Cancer Patients Based on Briganti 2019 Nomogram: A Phase II, Single-center, Single-arm, Prospective Study

The goal of this clinical trial is to evaluate whether adjuvant darolutamide plus androgen-deprivation therapy (ADT) can reduce post-operative recurrence and improve disease control in high-risk prostate cancer patients-defined by the Briganti 2019 nomogram-who have undergone radical prostatectomy (RP) without extended pelvic lymph node dissection (ePLND). The main questions it aims to answer are:
1. What proportion of participants remains biochemical-recurrence-free at 2 years, using NCCN criteria (PSA increase >0.1 ng/mL above post-treatment nadir confirmed by two tests ≥2 weeks apart)?
2. What proportion of participants is the 2-year radiographic progression-free survival (rPFS)?
Additional key outcomes include:
* PSA undetectable rates at 6, 12, and 24 months (PSA <0.01 ng/mL).
* Safety and tolerability assessed by CTCAE v5.0.
* Exploratory** patient-reported outcomes: urinary symptoms (IPSS) and quality of life (EQ-5D-3L).
Study type & design: Phase II, single-center, single-arm, prospective interventional study. Enrollment occurs within 12 weeks after RP. ADT is delivered with a GnRH agonist (physician's choice); orchiectomy is excluded. Target sample size is approximately 40 participants; the statistical plan uses a one-sample log-rank framework. Primary and secondary endpoints are assessed over 2 years.
Participants will: Provide informed consent and undergo eligibility confirmation (high-risk per Briganti 2019; post-RP without ePLND; enrollment ≤12 weeks after surgery). Receive darolutamide + ADT according to protocol (GnRH agonist; no orchiectomy). Attend scheduled visits for PSA monitoring, safety labs, and adverse-event assessments (CTCAE v5.0). Undergo radiologic evaluations as per protocol to determine rPFS (RECIST 1.1/PCWG3). Complete IPSS and EQ-5D-3L questionnaires at specified time points to assess urinary symptoms and quality of life.
Primary endpoint: 2-year biochemical-recurrence-free rate. Key secondary endpoints: 2-year rPFS; PSA <0.01 ng/mL at 6/12/24 months; treatment-emergent adverse events.
Exploratory endpoints: IPSS and EQ-5D-3L changes over 2 years.
This trial aims to balance oncologic control with quality of life in a population for whom the therapeutic value of ePLND remains uncertain, by testing whether early adjuvant darolutamide + ADT after RP can meaningfully delay recurrence and progression while maintaining acceptable tolerability.

Start Date01 Jan 2026

Sponsor / Collaborator

Peking University First Hospital

CTIS2025-520482-52-03

/ Not yet recruitingPhase 1/2IIT

Clinical Application of the Androgen Receptor Inhibitor Darolutamide to Upregulate the Prostate-Specific Membrane Antigen (PSMA) Protein Expression in Patients with Hormone Sensitive Prostate Cancer. - The DARO-flare Trial -

Start Date01 Jan 2026

Sponsor / Collaborator-

NCT07142551

/ Not yet recruitingPhase 2IIT

Supraphysiologic Testosterone Priming Induces Darolutamide Extended Response Via Modulation of ANdrogen Receptor (the SPIDERMAN Trial)

The objective of this study is to determine the safety and clinical effects of alternating pharmacologic (i.e. supraphysiologic) testosterone therapy with darolutamide in men with metastatic prostate cancer as first line hormonal therapy. Correlative studies will be conducted to assess the effect of alternating therapy on quality of life, gene expression and metabolic changes associated with alternating therapy.

Start Date20 Feb 2026

Sponsor / Collaborator

The Sidney Kimmel Comprehensive Cancer Center

[+1]

100 Clinical Results associated with Darolutamide

100 Translational Medicine associated with Darolutamide

100 Patents (Medical) associated with Darolutamide

482

Literatures (Medical) associated with Darolutamide

01 Mar 2026·Biomaterials advances

PEGylated liposomes co-encapsulating darolutamide and hesperetin for enhanced prostate cancer therapy: 2D, 3D PC3 models and in-vivo evaluation

Article

Author: Khemchandani, Rahul ; Pawar, Avinash ; Pardhi, Ekta ; Mehra, Neelesh Kumar ; Smanthula, Gananadhamu ; Patil, Ruchita

In this study, a darolutamide and hesperetin co-loaded PEGylated liposomal formulation (DHLP) was developed for the treatment of non-metastatic castration-resistant prostate cancer (nmCRPC). The formulation was prepared using the ethanol injection method, followed by membrane extrusion through a 100 nm polycarbonate filter to ensure size uniformity. The optimized DHLP liposomal formulation exhibited a clear bluish appearance, with a mean particle size of 106.5 ± 3.2 nm, a polydispersity index of 0.128 ± 0.023, and a zeta potential of -14.10 ± 0.25 mV, indicating colloidal stability and uniformity. Spherical morphology was confirmed through microscopic analysis. High encapsulation efficiencies were achieved for both DA (90.1 ± 3.3 %) and HE (91.3 ± 2.7 %). For both medication, in vitro drug release experiments showed a sustained release profile from the DHLP. Cytotoxicity assessment in PC3 prostate cancer cells revealed a 2.83-fold increase in cytotoxicity compared to free DA solution, a 3.89-fold increase compared to free HE solution, and a 1.47-fold improvement over the combined DA-HE solution. The combination index value of 0.89 confirmed synergistic anticancer activity. DHLPs inhibited cell migration, increased ROS generation, and reduced 3D spheroid size, with enhanced cellular uptake contributing to improved therapeutic efficacy. In-vivo pharmacokinetic studies in BALB/c mice demonstrated a 1.7- and 3.4-fold increase in the plasma half-life of DA and HE, respectively, compared to their free drug solutions. Biodistribution studies revealed reduced accumulation of DHLP in vital organs compared to the free drug solution. Acute toxicity assessment at three dose levels showed no histopathological alterations, indicating a favorable safety profile. These results imply that DHLP is a potential nanocarrier system for the effective management of prostate cancer.

15 Dec 2025·INTERNATIONAL JOURNAL OF CANCER

Severe cutaneous adverse reactions associated with novel antiandrogens: A disproportionality analysis of three databases

Article

Author: Huang, Zhaohui ; Jiang, Jie ; Yang, Ziwen ; Zhu, Jianhong ; Li, Sha ; Li, Xinyu ; Huo, Xiaotong ; Wu, Junyan

Abstract:

Severe cutaneous adverse reactions (SCARs) encompassing Stevens‐Johnson syndrome (SJS), toxic epidermal necrolysis (TEN), drug reaction with eosinophilia and systemic symptoms (DRESS) and acute generalized exanthematous pustulosis (AGEP) are increasingly reported among patients treated with novel antiandrogens, but the signals of disproportionate reporting and clinical features remain inadequately defined. This study was an observational retrospective pharmacovigilance study using the publicly available FAERS/EudraVigilance/JADER databases. To explore the signals of disproportionate reporting, disproportionality analysis was conducted using information component (IC) and reporting odds ratio (ROR) methodologies. Descriptive statistics were calculated for baseline and demographic information, onset time, and reaction outcomes. There was no disproportional signal for SCARs in patients using abiraterone, enzalutamide, and darolutamide. Significant over‐reporting signals for apalutamide were observed in SJS (FAERS, ROR 025 = 4.12, IC 025 = 1.70, N = 30; EudraVigilance, ROR 025 = 11.54, IC 025 = 2.84, N = 55; JADER, ROR 025 = 2.90, IC 025 = 1.33, N = 25), TEN (FAERS, ROR025 = 4.40, IC025 = 1.75, N = 29, EudraVigilance, ROR 025 = 30.96, IC 025 = 3.74, N = 58; JADER, ROR 025 = 5.34, IC 025 = 1.85, N = 25), DRESS (FAERS, ROR025 = 2.68, IC025 = 1.33, N = 38; EudraVigilance, ROR 025 = 25.06, IC 025 = 3.53, N = 55; JADER, ROR 025 = 0.62, IC 025 = 0.19, N = 6) and AGEP (FAERS, ROR025 = 1.16, IC025 = 0.55, N = 7; EudraVigilance, ROR 025 = 4.18, IC 025 = 1.02, N = 5; JADER, ROR 025 = 1.05, IC 025 = 0.45, N = 4). Incorporated data from 3 databases, the lethal rates of apalutamide‐related SCARs were 24.4% for SJS, 51.1% for TEN, and 10.5% for DRESS. The median time to onset was 41 days for SJS, 29 days for TEN, and 40 days for DRESS, respectively. The postmarketing pharmacovigilance study suggested an association between SCARs and apalutamide use, but not for other novel antiandrogens. As apalutamide gains greater clinical use, practitioners must be aware of apalutamide‐SCARs risk.

01 Dec 2025·The French journal of urology

French recommendations from the AFU Cancer Committee for prostate cancer: 2025 summary of changes

Review

Author: Dariane, Charles ; Neuzillet, Yann ; Peyrottes, Arthur ; Sargos, Paul ; Brureau, Laurent ; Rozet, François ; Ploussard, Guillaume ; Fromont, Gaëlle ; Barret, Eric ; Baboudjian, Michaël ; Turpin, Léa ; Rouprêt, Morgan ; Renard-Penna, Raphaële ; Roubaud, Guilhem ; Supiot, Stéphane ; Olivier, Jonathan ; Mathieu, Romain ; Fiard, Gaëlle

PURPOSE OF THIS DOCUMENT:

The Oncology Committee of the French Urology Association (CCAFU) is proposing a 2025 summary of recommendations' changes for the management of prostate cancer (PCa).

METHODS:

A systematic review of the literature from July 2024 to September 2025 was conducted by the CCAFU on the evolutions of diagnostic and therapeutic management of PCa evaluating the newly published references with their level of evidence.

RESULTS:

Biparametric MRI is an alternative to multiparametric MRI imaging to guide biopsy decision making provided that a high-quality imaging and radiology expertise is achieved. Transperineal biopsy is the recommended approach when technically feasible. Whole-gland HIFU in patients fulfilling the HIFI trial criteria is a treatment option for intermediate-risk PCa patients. In case of metastasis-directed therapy outside the context of symptoms for oligometastatic hormone-sensitive PCa (mHSPC) disease, at least 6 months of androgen deprivation therapy (ADT) should be given. In patients with high-risk BCR treated according to the EMBARK criteria, systemic treatment with monotherapy enzalutamide may be considered. The ARPI used in addition to ADT alone can be: abiraterone, apalutamide, darolutamide, enzalutamide. In the case of HRR alterations, the combination of niraparib and abiraterone may be proposed as first-line mHSPC. In the case of a positive radiolabelled PSMA ligand PET/CT scan in a patient progressing after at least one ARPI, internal radiotherapy using [¹⁷⁷ Lu]LuPSMA-617 may be proposed. In patients with no or mildly symptomatic bone metastatic castration-resistant PCa without visceral metastases, the combination of enzalutamide+6 cycles of radium-223 may be proposed.

CONCLUSION:

This 2025 summary of changes of French recommendations on PCa should help physicians to stay up-to-date with recent evolutions and aim to improve the management of PCa patients.

238

News (Medical) associated with Darolutamide

03 Dec 2025

·endpoints.news

Orion's €180M milestone payment; Iolyx partners dry eye candidate

Plus, news about QurAlis, Clene, ADC Therapeutics and Junevity: 💶 Orion to receive €180M milestone payment: The cash will come from Bayer, on the back of sales of prostate cancer therapy Nubeqa. Subsequently, Orion also updated its full-year sales outlook. — Reynald Castaneda 👁️ Iolyx finds a partner, raises money: California biotech Iolyx Therapeutics has nabbed a $15 million Series B from Frazier Life Sciences and GC&H. The startup also forged a partnership with Laboratoires Théa that is worth up to $280 million. Théa will get exclusive worldwide rights outside Asia to develop and market ILYX-002 for ocular surface diseases. Théa will run Phase 3 studies. The small biotech disclosed Phase 2 data in autoimmune dry eye disease in May. — Kyle LaHucik 💰 QurAlis gets another $25M: The Cambridge, MA-based biotech reeled in the money from existing investors, CEO Kasper Roet exclusively told Endpoints News . The biotech last disclosed an $88 million Series B in 2023 and a $45 million upfront neuro deal with Lilly in 2024. With extra runway from the insider round money, QurAlis has now pushed out its Series C raise until after its STMN2 data readout in the first half of 2026, Roet said. The experimental medicine, dubbed QRL-201, is in a proof-of-concept trial in ALS. The biotech also has investigational drugs for rare epilepsy, pain, Fragile X and other indications. — Kyle LaHucik 📊 Clene presents analyses for ALS drug, to seek FDA meeting: The biotech is developing a treatment based on gold nanocrystals to treat ALS. Researchers revealed three post-hoc analyses claiming to show its drug provided a benefit on biomarkers that could impact survival times. Clene is seeking accelerated approval for the drug, called CNM-Au8, and hopes to meet with regulators by the end of March 2026. In 2023, the FDA found Clene’s biomarker research to be “insufficient” to support approval. — Max Gelman 📊 ADC Therapeutics’ Zynlonta combo data: The biotech’s CD19-directed ADC in combination with Roche’s Columvi produced an overall response rate of almost 90% in patients with second-line or later relapsed or refractory diffuse large B cell lymphoma (DLBCL), including a 78% complete response rate. The open-label Phase 1b study had enrolled 49 DLBCL patients as of the November cutoff date. 💰 Junevity gets another $10M: The San Francisco startup expanded its seed round to develop an siRNA for type 2 diabetes and obesity. The money will get the biotech through “initial clinical studies,” Junevity said. The biotech anticipates entering Phase 1 in the second half of next year, and sees potential in pairing up with GLP-1s to reduce the dosing frequency of those blockbuster treatments. Investors include Goldcrest Capital and Godfrey Capital. — Kyle LaHucik

Phase 1Phase 2Phase 3Clinical Result

03 Dec 2025

·www.globenewswire.com

Inside information: Orion to receive EUR 180 million milestone and updates full-year outlook for 2025

ORION CORPORATION STOCK EXCHANGE RELEASE – INSIDE INFORMATION 3 DECEMBER 2025 at 09.00 EET Inside information: Orion to receive EUR 180 million milestone and updates full-year outlook for 2025 Orion Corporation has been informed that it will receive a milestone payment of EUR 180 million related to sales of Nubeqa®, which will be recorded in the fourth quarter of 2025. Due to receiving the milestone, Orion updates the full-year outlook for 2025 in terms of both net sales and operating profit. New full-year outlook for 2025, provided on 3 December 2025 Net sales are estimated to be EUR 1,820 million to EUR 1,900 million. Operating profit is estimated to be EUR 590 million to EUR 670 million. Previous full-year outlook for 2025, provided on 28 October 2025 Net sales are estimated to be EUR 1,640 million to EUR 1,720 million. Operating profit is estimated to be EUR 410 million to EUR 490 million. Orion Corporation Liisa HurmePresident and CEO René LindellCFO Contact person:Tuukka Hirvonen, Head of Investor Relations tel. +358 10 426 2721 Publisher:Orion CorporationCommunicationsOrionintie 1A, FI-02200 Espoo, Finlandhttp://www.orionpharma.com Orion is a globally operating Nordic pharmaceutical company – a builder of well-being for over a hundred years. We develop, manufacture and market human and veterinary pharmaceuticals and active pharmaceutical ingredients. Orion has an extensive portfolio of proprietary and generic medicines and consumer health products. The core therapy areas of our pharmaceutical R&D are oncology and pain. Proprietary products developed by Orion are used to treat cancer, neurological diseases and respiratory diseases, among others. In 2024 Orion's net sales amounted to EUR 1,542 million and the company employed about 3,700 professionals worldwide, dedicated to building well-being. Orion's A and B shares are listed on Nasdaq Helsinki.

Financial Statement

01 Dec 2025

·endpoints.news

Janux’s prostate cancer immunotherapy’s response rate drops, according to new early-stage data

Janux Therapeutics’ lead T cell engager has shown response rates of 30% in a new data cut from an early-stage study in prostate cancer. The product, named JANX007, is in a Phase 1 trial called ENGAGER-PSMA-01 in metastatic castration-resistant prostate cancer (mCRPC). A year ago, the company released positive early results from 16 patients in this trial, leading the company’s stock to climb 66%. On Monday, Janux posted updated results from 104 patients who were treated in the Phase 1a dose escalation part of the ENGAGER trial. Janux also disclosed data on five patients in a Phase 1b expansion of the study. In both parts, JANX007 — which targets PSMA and CD3 — was infused either weekly or every two weeks. Patients in the Phase 1a part of the trial had already been given a median of four prior lines of therapy. Those in the expansion part had not received a taxane, a common type of chemotherapy treatment. This means they roughly corresponded to first- or second-line patients, according to Cowen analysts. The San Diego biotech said that as of an Oct. 15 data cutoff, confirmed and unconfirmed partial responses were seen in 30% of evaluable patients across both parts of the study. This was a drop from the previous cut, in which four of eight patients had partial responses. The company’s stock $JANX plunged in after-hours trading, losing 43%. In the trial, radiographic progression-free survival (rPFS) was between 7.9 and 8.9 months in both the once-weekly and every-two-week cohorts. rPFS among patients who were given the drug every two weeks was longer than in those who were infused weekly, Janux said. This is somewhat surprising, since more frequent administration would typically produce a more profound effect. Among the five patients in the expansion, there were “rapid and deep” reductions in levels of prostate-specific antigen, a marker of prostate cancer, Janux said. A tumor burden analysis suggested that rPFS could improve in JANX007-treated earlier-line patients. Analysts from Cowen wrote in a Nov. 6 note that “consultants would view PFS data in the low double digits as compelling.” Cases of cytokine release syndrome, a side effect of immunotherapy, were limited to the first cycle of treatment and were grades 1 and 2. The company identified a mitigation strategy for this side effect which maintained the grade 1 and 2 CRS profile, though Janux did not offer details. Janux CEO David Campbell said JANX007’s safety profile “compares favorably to both approved and investigational therapies in mCRPC.” He added that the possibility of dosing patients every two weeks might give the drug “meaningful convenience advantages.” The biotech is investigating JANX007 as a monotherapy and in combination with Bayer’s androgen receptor inhibitor Nubeqa in taxane-naïve mCRPC patients. It also plans to test the drug in patients who do not respond to PARP inhibitors. Editor’s note: This story has been updated to add the reaction in the company’s shares on Monday.

Clinical ResultPhase 1Immunotherapy

100 Deals associated with Darolutamide

External Link

KEGG	Wiki	ATC	Drug Bank
D11045	Darolutamide	L02BB06	DB12941

R&D Status

Approved

10 top approved records.

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Indication	Country/Location	Organization	Date
Castration-sensitive prostate cancer	United States	Bayer HealthCare Pharmaceuticals, Inc.	03 Jun 2025
Hormone-dependent prostate cancer	European Union	Bayer AG	20 Mar 2023
Hormone-dependent prostate cancer	Iceland	Bayer AG	20 Mar 2023
Hormone-dependent prostate cancer	Liechtenstein	Bayer AG	20 Mar 2023
Hormone-dependent prostate cancer	Norway	Bayer AG	20 Mar 2023
Metastatic Prostate Carcinoma	Japan	Bayer AG	24 Feb 2023
Metastatic castration-resistant prostate cancer	United States	Bayer HealthCare Pharmaceuticals, Inc.	05 Aug 2022
Prostatic Cancer	Brazil	Bayer AG	01 Jan 2020
Castration-Resistant Prostatic Cancer	United States	Bayer HealthCare Pharmaceuticals, Inc.	30 Jul 2019

Developing

10 top R&D records.

to view more data

Indication	Highest Phase	Country/Location	Organization	Date
Localized Prostate Carcinoma	Phase 3	France	Bayer AG	10 Apr 2025
Localized Prostate Carcinoma	Phase 3	Martinique	Bayer AG	10 Apr 2025
Recurrent Prostate Carcinoma	Phase 3	United States	Bayer AG	03 Apr 2023
Recurrent Prostate Carcinoma	Phase 3	China	Bayer AG	03 Apr 2023
Recurrent Prostate Carcinoma	Phase 3	Japan	Bayer AG	03 Apr 2023
Recurrent Prostate Carcinoma	Phase 3	Australia	Bayer AG	03 Apr 2023
Recurrent Prostate Carcinoma	Phase 3	Austria	Bayer AG	03 Apr 2023
Recurrent Prostate Carcinoma	Phase 3	Belgium	Bayer AG	03 Apr 2023
Recurrent Prostate Carcinoma	Phase 3	Brazil	Bayer AG	03 Apr 2023
Recurrent Prostate Carcinoma	Phase 3	Canada	Bayer AG	03 Apr 2023

Clinical Result

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View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


ARAMIS (ESMO_ASIA2025)	Phase 3	Castration-Resistant Prostatic Cancer	76	Darolutamide + androgen-deprivation therapy	qicchaiqol(ayhucqiwso) = eznymmouay wabofvicld (hsiygyuxqt ) View more	Positive	05 Dec 2025
ChiCTR2500096436 (DAPLOM, ESMO_ASIA2025)	Phase 2	Castration-sensitive prostate cancer	60	Darolutamide + ADT + prostate arterial docetaxel infusion	cpzlfgdvfn(eqawbinpfy) = uzddmzwzle sbzpkupuqx (sxrtrzhklj )	Positive	05 Dec 2025
ESMO_ASIA2025	Not Applicable	Hormone-dependent prostate cancer	8	Darolutamide + Trans-arterial chemoperfusion by Docetaxel + ADT	idtdnvcxbm(wfmgkdtsxb) = fekdynbxtf pwjorbajec (ppyizranwd ) View more	Positive	05 Dec 2025
ESMO_ASIA2025	Not Applicable	Hormone-dependent prostate cancer	25	Darolutamide + Docetaxel + ADT	lnhnukmsor(wwkimbfxix) = jehpzzuqlk icmpwloypf (pxrqpkdgxd ) View more	Positive	05 Dec 2025
NCT05794906 (ARASTEP, Pubmed \| Future Oncol)	Phase 3	Non-metastatic prostate cancer	970	Darolutamide + ADT	hhrmavdjzu(ttnojaghif) = buabbgxpzp ztjvbvgkik (pyjduiilaf ) View more	Positive	14 Nov 2025
				Placebo + ADT	hhrmavdjzu(ttnojaghif) = pcujzdfotc ztjvbvgkik (pyjduiilaf ) View more
NCT04122976 (DAROL, ESMO2025)	Not Applicable	Castration-Resistant Prostatic Cancer	799	Darolutamide	jqdvbmjsoa(nwpzmowrcz) = nfbacipaxc aewllqijav (xbbwvlzwps ) View more	Positive	17 Oct 2025
				Placebo	jqdvbmjsoa(nwpzmowrcz) = laqxmhenmw aewllqijav (xbbwvlzwps ) View more
ARAMIS (ESMO2025)	Phase 3	Castration-Resistant Prostatic Cancer	4,117	Darolutamide + ADT	aujmxyokig(uqkdvcxlwh) = wmvpedxtsh oijfoalolt (aoltodzaks )	Positive	17 Oct 2025
				Apalutamide + ADT	aujmxyokig(uqkdvcxlwh) = zvfouexxfx oijfoalolt (aoltodzaks )
NCT06029036 (ESMO2025)	Phase 2	Neoadjuvant	53	Darolutamide + ADT	wsniccwlcu(lzixmmfsfe) = jrbbaleunh mftnqhrtyb (bnaoylhwhf ) View more	Positive	17 Oct 2025
NCT02799602 (ARASENS, ESMO2025)	Phase 3	Metastatic Prostate Carcinoma	847	Lead-in ADT used	kkffxtsbip(jnmhbbgvtq) = cnacjqqwfa ptofyigmcp (vgaepemuga ) View more	Positive	17 Oct 2025
				No lead-in ADT	kkffxtsbip(jnmhbbgvtq) = kujsijjmwe ptofyigmcp (vgaepemuga ) View more
ESMO2025	Not Applicable	Hormone-dependent prostate cancer	242	Darolutamide+ADT+DOC (DAR)	cpgwtrltgf(zetbycqaqi) = bnyxfijkxo yxitgwetpv (gzdflwalqc, 51.0 - 72.9) View more	Positive	17 Oct 2025
				Abiraterone+ADT+DOC (ABI)	cpgwtrltgf(zetbycqaqi) = xbruzcbtgl yxitgwetpv (gzdflwalqc, 32.0 - 63.0) View more

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