DAROSTEP: Evaluating Step Counts as a Biomarker and Its Relationship on Treatment Outcomes in Vulnerable Patients With Metastatic Hormone-Sensitive Prostate Cancer on Darolutamide and Androgen Deprivation Therapy

This prospective clinical trial aims to investigate the impact of darolutamide in combination with standard-of-care androgen deprivation on physical activity, specifically step count, and its correlation with important markers of safety in vulnerable adults who screen positive by a brief geriatric assessment (GA) and metastatic hormone-sensitive prostate cancer.

Start Date01 Nov 2026

Sponsor / Collaborator

The University of Chicago

NCT07395804

/ Not yet recruitingNot Applicable

DAROlutamide DoUBlet Therapy in Daily Practice (DARO-DUB) - Real-world Evaluation of Patients With Metastatic Hormone-sensitive Prostate Cancer (mHSPC) Treated With Darolutamide Plus ADT in Germany

Prostate cancer is a disease where cells in the prostate gland grow out of control. When prostate cancer has spread to other parts of the body but still responds to hormone treatment, it is called metastatic hormone-sensitive prostate cancer (mHSPC).
The usual treatment for this stage of prostate cancer is hormone therapy (called androgen-deprivation therapy or ADT) combined with another medicine that blocks the effect of male hormones on cancer cells, known as an androgen-receptor pathway inhibitor. Darolutamide is a newer type of androgen-receptor inhibitor.
The main goal of this study is to find out how well a combination of two treatments-darolutamide and hormone therapy (also called androgen-deprivation therapy or ADT)-works for men in Germany who have advanced prostate cancer that has spread to other parts of the body and still responds to hormone treatment. The study will look at how many men have very low or undetectable levels of a protein called prostate-specific antigen (PSA) in their blood after 12 months of treatment. PSA is a marker that doctors use to check how active prostate cancer is.
The study will also look at how long men live after starting this treatment, and will collect information about their health, the type of prostate cancer they have, and any other medicines they are taking. The study will last for 5 years. At the start of the study, the study doctor will collect information about each patient's background, such as age, other health problems, and details about their prostate cancer. This information will be taken from the patient's medical records if available. If some information is missing, the doctor may ask the patient directly.
Other information will be collected as the study goes on. This includes details about the patient's treatment, how they are doing during their regular medical visits, and any changes in their health. These check-ups and data collection will happen as part of the patient's usual care, including at the beginning of treatment, during treatment visits, follow-up visits, and at the end of the study observation period.

Start Date28 Feb 2026

Sponsor / Collaborator

Bayer AG

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

464

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.

01 Feb 2026·ANTICANCER RESEARCH

Prolonged Castration Prior to Docetaxel Reduces Febrile Neutropenia in Patients With Metastatic Hormone-sensitive Prostate Cancer Receiving Triple Therapy

Article

Author: Kanesaka, Manato ; Higuchi, Kosuke ; Nakamura, Kazuyoshi ; Kurozumi, Akira ; Tamura, Takaaki ; Fukasawa, Satoshi ; Mikami, Kazuo ; Sazuka, Tomokazu ; Sakamoto, Shinichi ; Sato, Hiroaki ; Arai, Takayuki ; Azuma, Haruhito ; Takeshita, Nobushige ; Suzuki, Noriyuki ; Imamura, Yusuke ; Tsujino, Takuya ; Yamada, Yasutaka ; Shirafuji, Tomoki ; Yamamoto, Satoshi ; Sato, Kodai

BACKGROUND/AIM:

Triplet therapy, combining androgen deprivation therapy (ADT), darolutamide, and docetaxel has recently emerged as the standard first-line treatment for metastatic hormone-sensitive prostate cancer (mHSPC). Febrile neutropenia (FN) is a major clinical issue not only as a serious infection but also as a cause for early cessation or dose reduction of chemotherapy. However, little is known regarding the predictive factors for the development of FN in patients with mHSPC receiving triplet therapy.

PATIENTS AND METHODS:

This study enrolled 60 patients diagnosed with mHSPC across multiple institutions from 2023 to 2025. We examined clinical characteristics, treatment schedules, adverse events, and oncological outcomes. We focused particularly on the development of FN and used logistic regression analysis to investigate the predictive factors.

RESULTS:

The median age was 72 years old, and 43 patients (73.3%) had high-volume disease at diagnosis. Nine patients (15%) developed FN. Multivariate logistic regression analysis identified older age [≥75, p=0.0161; hazard ratio (HR)=7.49], high-volume disease (p=0.0335), and shorter interval from ADT to docetaxel (<40 days) (p=0.0389; HR=7.86) as independent predictive factors of the development of FN. Notably, prolonged castration period prior to docetaxel (≥40 days) significantly reduced the risk of FN from 23.5% to 3.8% (p=0.0001). Patients who developed FN tended to have shorter castration-resistant prostate cancer progression-free survival (CRPC-PFS) compared to those who did not (p=0.0812; HR=3.2).

CONCLUSION:

Older age and high-volume disease were independent risk factors for FN in patients with mHSPC receiving triplet therapy. A longer interval from ADT initiation to docetaxel (≥40 days) was associated with a significantly lower risk of FN, suggesting that extending the pre-docetaxel castration period is a practical, adjustable scheduling strategy to improve treatment safety. These findings may support treatment selection and proactive prevention of FN.

01 Feb 2026·INTERNATIONAL JOURNAL OF UROLOGY

Impact of Immunohistochemical PSA and Ki‐67 Expression on Prognosis in Metastatic Castration‐Sensitive Prostate Cancer

Article

Author: Urabe, Fumihiko ; Imai, Yu ; Umemori, Miyaka ; Sato, Shun ; Takahashi, Hiroyuki ; Iwamoto, Yuya ; Kimura, Takahiro ; Tashiro, Kojiro

ABSTRACT:

Background and Objective:

Treatment selection for metastatic castration‐sensitive prostate cancer (mCSPC) remains challenging, as reliable and practical biomarkers predicting response to androgen receptor pathway inhibitor (ARPI)‐based therapy are limited. We evaluated whether prostate‐specific antigen (PSA) and Ki‐67 expression in diagnostic biopsy specimens can predict oncologic outcomes in patients with mCSPC treated with ARPI–androgen deprivation therapy (ADT) doublet therapy, and whether these biomarkers can guide optimal treatment selection.

Methods:

This retrospective multicenter study included 58 patients with mCSPC who received ARPI–ADT doublet therapy between 2018 and 2024. Immunohistochemical staining for PSA and Ki‐67 was performed on diagnostic biopsy specimens. Receiver operating characteristic curve analyses were used to determine optimal cutoff values for predicting progression to castration‐resistant prostate cancer (CRPC). Survival outcomes were analyzed using the Kaplan–Meier method and Cox proportional hazards models. Exploratory analyses included patients treated with triplet therapy (ADT + docetaxel + darolutamide) or upfront docetaxel.

Results:

Low PSA expression, high Ki‐67 expression, and a bone metastasis extent of disease (EOD) score ≥ 3 were independently associated with shorter CRPC‐free survival (CRPC‐FS). Stratification by risk factors (0, 1, or 2) showed a stepwise decline in CRPC‐FS. In exploratory analyses, triplet therapy achieved the longest CRPC‐FS and progression‐free survival 2 among high‐risk patients, whereas no significant differences among treatment modalities were observed in the low‐risk group.

Conclusion:

Immunohistochemical PSA and Ki‐67 expression provide practical prognostic information for patients with metastatic castration‐sensitive prostate cancer. Combined assessment with EOD ≥ 3 identifies a high‐risk subgroup with unfavorable clinical outcomes.

255

News (Medical) associated with Darolutamide

12 Feb 2026

·www.globenewswire.com

Orion Group Financial Statement Release January–December 2025

ORION CORPORATION FINANCIAL STATEMENT RELEASE 1–12/2025 12 FEBRUARY 2026 at 12:00 EET Orion Group Financial Statement Release January–December 2025 October–December 2025 Highlights Net sales totalled EUR 695.3 (October–December 2024: 434.4) million Operating profit was EUR 328.1 (92.7) millionBasic earnings per share were EUR 1.85 (0.52)Cash flow from operating activities per share was EUR 0.58 (0.63)The outlook for 2026 (provided on 14 January 2026): Net sales are estimated to be EUR 1,900 million to EUR 2,100 million. Operating profit is estimated to be EUR 550 million to EUR 750 million. January–December 2025 Highlights Net sales totalled EUR 1,889.5 (January–December 2024: 1,542.4) million Operating profit was EUR 631.6 (416.6) millionBasic earnings per share were EUR 3.56 (2.35)Cash flow from operating activities per share was EUR 2.25 (2.09)The Board of Directors proposes a dividend of EUR 1.80 (1.64) to be paid for 2025. The dividend is proposed to be paid in two instalments. Key figures 10–12/2510–12/24Change %1–12/251–12/24Change %Net sales, EUR million695.3434.4+60.1%1,889.51,542.4+22.5%EBITDA, EUR million343.0147.1> 100 %688.3509.4+35.1%% of net sales49.3%33.9% 36.4%33.0% Operating profit, EUR million328.192.7> 100 %631.6416.6+51.6%% of net sales47.2%21.3% 33.4%27.0% Profit before taxes, EUR million327.091.7> 100 %627.8413.1+52.0%% of net sales47.0%21.1% 33.2%26.8% Profit for the period, EUR million260.573.4> 100 %500.3329.9+51.7%% of net sales37.5%16.9% 26.5%21.4% Research and development expenses, EUR million70.662.5+13.0%210.4179.6+17.2%% of net sales10.2%14.4% 11.1%11.6% Capital expenditure excluding acquired in business combination, EUR million28.329.8-5.2%112.986.1+31.0%% of net sales4.1%6.9% 6.0%5.6% Acquired in business combination, net of cash, EUR million 4.0 > 100 %Interest-bearing net liabilities, EUR million 144.4121.7+18.7%Basic earnings per share, EUR1.850.52> 100 %3.562.35+51.5%Cash flow from operating activities per share, EUR0.580.63-7.5%2.252.097.8%Equity ratio, % 64.1%61.9% Gearing, % 11.2%12.1% Return on capital employed (before taxes), % 43.8%34.9% Return on equity (after taxes), % 43.7%34.8% Average number of personnel during the period 4,0033,712+7.8% President and CEO Liisa Hurme: Another strong quarter, a great closure to a successful year 2025 "In October–December 2025, our net sales increased by 60.1 percent to EUR 695.3 (434.4) million and operating profit increased more than threefold to EUR 328.1 (92.7) million. Underlying business developed very favourably and in addition the growth both in net sales and especially in operating profit was boosted by the EUR 180 million Nubeqa milestone. Excluding all milestones, our net sales increased by 18.5 percent to EUR 514.0 (433.9) million, and operating profit by 59.2 percent to EUR 146.8 (92.3) million. All of our largest business divisions continued the strong performance we have seen throughout the year. The Innovative Medicines business division more than doubled its net sales in Q4 thanks to the EUR 180 milestone and Nubeqa® sales. Nubeqa® has consistently exceeded expectations, and now we estimate that Orion's annual Nubeqa® net sales have the potential to exceed EUR 1 billion by the end of the current decade. Also the Branded Products, and the Generics and Consumer Health business divisions remained on a solid growth path. Both divisions have strong, high-quality portfolios, which developed well as a whole. The Animal Health business division’s sales continued on a good level. On the R&D front, our clinical development pipeline progressed further with the initiation of a phase 2 trial of ODM-212, which is a TEAD inhibitor, in December. This first trial focuses on rare cancers but we see a lot of potential with ODM-212 and its mode of action in various indications. Thus, we aim to expand the phase 2 program during 2026. Also, as planned, our partner Tenax initiated a second phase 3 trial with levosimendan for pulmonary hypertension in heart failure with preserved ejection fraction. Overall, Orion delivered a very strong performance in 2025, with solid financial results and clear progress in executing our strategy. We took a significant step forward in strengthening our biologics R&D by establishing an R&D center in Cambridge, England. We have also strengthened our US unit with key recruitments and moved our office from New York to Boston, which is a leading biotech hub. Due to Nubeqa’s strong performance and outlook, we gave financial outlook for 2026 already in January. We are expecting another very strong year, during which we will continue our determined work to build well-being and Orion’s future.” Proposal by the Board of Directors of Orion Corporation to the Annual General Meeting 2026 on the resolution on the use of the profit shown on the Balance Sheet and the distribution of dividend Orion Corporation’s distributable funds at 31 December 2025 are EUR 853,045,368.34, of which the profit for the financial year is EUR 482,748,629.26. The Board of Directors proposes to the Annual General Meeting of Orion Corporation to be held on 24 March 2026 that a dividend of EUR 1.80 per share be paid on the basis of the Balance Sheet confirmed for the financial year that ended on 31 December 2025. No dividend shall be paid on treasury shares held by the Company on the record date for dividend payment. According to the proposal, the dividend would be paid in two instalments. The first instalment of EUR 0.90 per share would be paid to a shareholder who is on the record date for the payment of the dividend, 26 March 2026, registered in the Company’s shareholders’ register maintained by Euroclear Finland Oy. The Board of Directors proposes that the first instalment would be paid on 2 April 2026. The second instalment of EUR 0.90 per share would be paid to a shareholder who is on the record date for the payment of the dividend, 20 October 2026, registered in the Company’s shareholders’ register maintained by Euroclear Finland Oy. The Board of Directors proposes that the second instalment would be paid on 27 October 2026. The Board of Directors proposes that the Annual General Meeting would authorise the Board of Directors to resolve, if necessary, on a new record date for payment and payment date for the second instalment of the dividend in case of changes in the rules of Euroclear Finland Oy or the regulations regarding the Finnish book-entry system or if other rules binding the Company so require. In addition, the Board of Directors proposes to the Annual General Meeting that EUR 500,000 of the Company’s distributable funds be donated to medical research and other purposes of public interest as decided by the Board of Directors. Any remaining distributable funds would be allocated to retained earnings. There have been no material changes in the Company’s financial position since the end of the financial year. The liquidity of the Company is good and, in the opinion of the Board of Directors, the proposed profit distribution would not compromise the liquidity of the Company. Outlook for 2026 (provided on 14 January 2026) Net sales are estimated to be EUR 1,900 million to EUR 2,100 million. Operating profit is estimated to be EUR 550 million to EUR 750 million. Basis for outlook Collaboration agreements with other pharmaceutical companies are an integral part of Orion’s business model. Agreements often include payments recorded in net sales and operating profit that vary greatly from year to year. Forecasting the timing and amount of these payments is difficult. In some cases, they are conditional on terms such as R&D outcomes which are not known until studies have been completed, the progress of R&D projects or the attainment of specified sales levels. Regarding possible new contracts under negotiation, neither the outcome nor the schedule of contract negotiations is generally known before the final signing of the agreement. In 2025, Orion booked one material milestone of EUR 180 million. The outlook for 2026 does not include any material milestone payments. Milestone payments received by Orion in 2021–2025 Year20212022202320242025EUR million323432134183 The outlook does not include income, expenses or other impacts related to any future material product or company acquisition or divestment. Net sales The outlook assumes that the Nubeqa® royalties and product sales booked by Orion will increase clearly in 2026. Orion’s assumption is based on forecasts received from its partner Bayer. However, it is difficult to predict the exact level of product sales and royalties of a strongly growing product for the whole year. In addition, some risk of tariff impact in the US is included in the outlook range. The Branded Products business division is estimated to grow in 2026. Growth is anticipated to be driven by the Respiratory therapy area and the Easyhaler® product portfolio, but also other therapy areas and products are expected to grow. The Animal Health business division is anticipated to grow slightly, with growth coming from various products. The net sales of the Generics and Consumer Health business division are estimated to be at a similar level or slightly higher than in 2025. Operating profit The underlying operating profit growth, i.e. excluding material milestones, is expected to be driven by increasing net sales and especially Nubeqa® royalties. However, it is difficult to predict the exact level of royalties of a strongly growing product for the whole year. Any variance from the predicted level can have a notable impact on Orion’s operating profit. Also, the mechanism by which each quarter’s product deliveries are always fully deducted from the next quarter’s royalty payments causes fluctuation in operating profit. Even though this impact on operating profit is only temporary, the timing of product deliveries may have notable impact on Orion’s operating profit in one calendar year. Significant part of Orion’s Nubeqa® income is coming from the United States and thus changes in the US dollar exchange rate cause fluctuations in Orion’s operating profit. Research and development costs, and in particular their timing, can also cause fluctuations in operating profit. Although the future costs of research and development projects are known quite well in advance, there are uncertainties about their timing. The start of projects may be delayed, and projects may progress faster or slower than expected. Projects may also have to be terminated, in which case the anticipated costs will not be fully realised. Orion estimates that R&D costs in 2026 will increase from 2025. Sales and marketing expenses are expected to increase in 2026. Expenses are increased by additional investments in the sale of the current product portfolio, and Nubeqa® royalty payable as per an agreement with Endo Pharmaceuticals. Capital expenditure The Group’s total capital expenditure in 2026 is not expected to have any significant changes compared to 2025. The estimate of capital expenditure does not include any investments related to any future material product or company acquisition. Near-term risks and uncertainties Orion is exposed to risks that may arise from its operations or changes in the operating environment. The most significant risk factors described below can potentially have an adverse effect on Orion’s business operations, financial position or financial results. Other risks, which are currently either unknown or considered immaterial to Orion may, however, become material in the future. Orion’s own production and other operations are exposed to risks that may materially disrupt their operations or even interrupt them at least temporarily. Such risks include, for example, accidents, damages, natural disasters, strikes, employee illness, conflicts, terrorism, cyber-attacks, hybrid influence, disruption of information or communication systems, disruption of energy supply, and disruption of supply and logistics chains. Orion’s production and business operations are dependent on global supply and logistics chains, the inaction of which may lead to low availability of finished products and raw materials, starting materials, semi-finished products, supplies, equipment and spare parts needed in production. Sales of individual products and also Orion’s sales in individual markets may vary, for example depending on the extent to which the ever-tougher price and other competition prevailing in pharmaceutical markets in recent years will specifically focus on Orion’s products. Changes in pharmaceutical or other regulation in individual markets or more broadly, for example at EU level, may affect the sales and profitability of Orion’s products. Changes in overall market demand may also have negative impact on sales. New tariffs or other possible customs duties on Orion’s products may negatively affect the sales and profitability of Orion’s products. The details of the US pharmaceutical tariffs, their implementation and their impact on Orion still remain unclear. Product deliveries to key partners are based on timetables that are jointly agreed in advance. Nevertheless, they can change, for example as a consequence of decisions concerning adjustments of stock levels. In addition, changes in market prices and exchange rates affect the value of deliveries. Key currencies that carry an exchange rate risk for Orion are the US dollar, the Swedish krona and the Polish zloty. Other significant currencies are the Danish krone and the Norwegian krone. However, the overall effect of the risk arising from currencies of European countries will be abated by the fact that Orion has organisations of its own in most European countries, which means that in addition to sales income there are also costs in these currencies. The current geopolitical conflicts and unrest, and other challenges in the global supply and logistics chains of pharmaceuticals have increased the already elevated risk of supply disruptions. The possible rise of raw material prices and other supply chain costs deteriorates the profitability of Orion’s products, since in the pharmaceutical industry it is very difficult to pass on cost increases to the prices of own products, especially prescription medicines, particularly in Europe. If high cost inflation occurs, it will pose a risk to Orion’s profitability. Authorities and key customers in different countries carry out regular and detailed inspections of drug development and manufacturing at Orion’s sites. Any remedial actions that may be required may at least temporarily have effects that decrease delivery reliability and increase costs. Orion’s product range also contains products manufactured by other pharmaceutical companies and products that Orion manufactures on its own but for which other companies supply active pharmaceutical or other ingredients and components or parts (among these the Easyhaler® products). Possible problems related to the delivery reliability or quality of the products of those manufacturers may cause a risk to Orion’s delivery reliability. The single-channel system used for pharmaceuticals distribution in Finland, in which Orion’s products have been delivered to customers through only one wholesaler, may also cause risks to delivery reliability. Research projects always entail uncertainty factors that may either increase or decrease estimated costs. Although the future costs of research and development projects are known quite well in advance, there are uncertainties about their timing. The start of projects may be delayed, and projects may progress faster or slower than expected having an impact on predicted costs within an individual year. Projects may also have to be terminated, in which case the anticipated costs will not be fully realised. Collaboration arrangements are an important component of Orion’s business model. Possible collaboration and licensing agreements related to these arrangements also often include payments to be recorded in net sales that may materially affect Orion’s financial results. The payments may be subject to conditions relating to the progress of research projects or sales or to new contracts to be signed, and whether these conditions or contracts materialise and what their timing is, will always entail uncertainties. The upfront and milestone payments paid by Orion to its collaborators, which are recorded as investments in intangible assets in balance sheet, include write-down risk that may be realised if, for example, a collaborative research project fails or otherwise has to be discontinued. Webcast and Conference Call A webcast and a conference call for analysts, investors and media representatives will be held on Thursday, 12 February 2026 at 14.00 EET. A link to the live webcast is available on Orion's website at www.orionpharma.com/investors. A recording of the event will be available on the website later the same day. Conference call can be joined by registering through the following link: https://events.inderes.com/orion/q4-2025/dial-in. Phone numbers and the conference ID to access the conference will be provided after the registration. In case you would like to ask a question during the conference, please dial *5 on your telephone keypad to enter the question queue. Questions can also be presented in writing through the question form of the webcast. Upcoming events Annual General Meeting planned to be heldTuesday 24 March 2026Interim Report January–March 2026Thursday 23 April 2026Half-Year Financial Report January–June 2026Friday 17 July 2026Interim Report January–September 2026Wednesday 28 October 2026 The Financial Statements and the Report by the Board of Directors for 2025 will be published on the Company’s website at the latest in week 10/2026. Espoo, 12 February 2026 Board of Directors of Orion Corporation For additional information about the report: Tuukka Hirvonen, Head of Investor Relations, tel. +358 10 426 2721 or +358 50 966 2721 Publisher: Orion Corporation https://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 2025 Orion’s net sales amounted to EUR 1,890 million and the company employs about 4,000 professionals worldwide, dedicated to building well-being. Orion’s A and B shares are listed on Nasdaq Helsinki. Attachment Orion Financial Statement Release 2025

Financial StatementPhase 2Phase 3

12 Feb 2026

·www.biospace.com

Celcuity Appoints Charles Romp to its Board of Directors

MINNEAPOLIS, Feb. 12, 2026 (GLOBE NEWSWIRE) -- Celcuity Inc. (Nasdaq: CELC), a clinical-stage biotechnology company pursuing development of targeted therapies for oncology, today announced the appointment of Charles (Chip) R. Romp to its Board of Directors. Mr. Romp brings over 25 years of experience in the pharmaceutical industry to Celcuity, including leadership of sales teams and commercial organizations in the oncology setting. “Chip brings a wealth of oncology-related commercial expertise to our Board,” said Brian Sullivan, Chief Executive Officer and co-founder of Celcuity. “Chip’s deep experience commercializing significant oncology drugs will provide valuable insight to Celcuity as we advance our programs and prepare for the potential approval and launch of gedatolisib later this year.” Mr. Romp is currently Chief Executive Officer of Secura Bio, an integrated, commercial-stage pharmaceutical company dedicated to the worldwide development and commercialization of oncology therapies. Mr. Romp previously served as Executive Vice President, Commercial U.S., at Seagen, Inc., where he was a member of the Executive Committee and oversaw the company's entire commercial organization before its sale to Pfizer. He joined Seagen in 2010 as one of its first commercial employees, where he managed the growth and expansion of ADCETRIS ® (brentuximab vedotin), PADCEV ® (enfortumab vedotin-ejfv), TUKYSA ® (tucatinib), and TIVDAK ® (tisotumab vedotin-tftv). Prior to Seagen, Mr. Romp held several senior sales leadership positions at Genentech, Inc, where he was responsible for both oncology and immunology products, including AVASTIN ® (bevacizumab), RITUXAN ® (rituximab), and XOLAIR ® (omalizumab). Mr. Romp received a Bachelor of Arts from the University of Florida and an MBA from Saint Leo University in Florida. “Gedatolisib has tremendous potential to enhance outcomes for women with breast cancer, which gives Celcuity a very significant opportunity to build an important franchise in oncology,” said Mr. Romp. “I am very excited to join the Board at this important moment in Celcuity’s history and work with Brian and the Board to share my experience commercializing a number of pathbreaking oncology therapeutics." About Celcuity Celcuity is a clinical-stage biotechnology company pursuing the development of targeted therapies for the treatment of multiple solid tumor indications. The company's lead therapeutic candidate is gedatolisib, a potent, pan-PI3K and mTORC1/2 inhibitor that comprehensively blockades the PI3K/AKT/mTOR (“PAM”) pathway. Its mechanism of action and pharmacokinetic properties are differentiated from other currently approved and investigational therapies that target PI3Kα, AKT, or mTORC1 alone or together. A Phase 3 clinical trial, VIKTORIA-1, evaluating gedatolisib in combination with fulvestrant, with or without palbociclib, in patients with HR+/HER2- advanced breast cancer (“ABC”), has completed enrollment, and the company has reported detailed results for the PIK3CA wild-type cohort. A Phase 3 clinical trial, VIKTORIA-2, evaluating gedatolisib plus a CDK4/6 inhibitor and fulvestrant as first-line treatment for patients with HR+/HER2- ABC, is currently enrolling patients. A Phase 1/2 clinical trial, CELC-G-201, evaluating gedatolisib in combination with darolutamide in patients with metastatic castration resistant prostate cancer, is ongoing. More detailed information about Celcuity’s active clinical trials can be found at ClinicalTrials.gov . Celcuity is headquartered in Minneapolis. Further information about Celcuity can be found at . Follow us on LinkedIn and X . Forward-Looking Statements This press release contains statements that constitute “forward-looking statements” within the meaning of the Private Securities Litigation Reform Act of 1995 including statements relating to the potential therapeutic benefits of gedatolisib; the size, design and timing of our clinical trials; our interpretation of clinical trial data; the ability of our data to support the filing of a new drug application (“NDA”) with the U.S. Food and Drug Administration (the “FDA”); our expectations regarding the timing of and our ability to obtain FDA approval under the Real-Time Oncology Review program and to commercialize gedatolisib; and other expectations with respect to gedatolisib. Words such as, but not limited to, “look forward to,” “believe,” “expect,” “anticipate,” “estimate,” “intend,” “confidence,” “encouraged,” “potential,” “plan,” “targets,” “likely,” “may,” “will,” “would,” “should” and “could,” and similar expressions or words identify forward-looking statements. The forward-looking statements included in this press release are based on management's current expectations and beliefs which are subject to a number of risks, uncertainties and factors, including that our clinical results are based on an ongoing analysis of key efficacy and safety data and our interpretation of such data may change; unforeseen delays in the review of our NDA for gedatolisib; and our ability to obtain and maintain regulatory approvals to commercialize gedatolisib. In addition, all forward-looking statements are subject to other risks detailed in our Annual Report on Form 10-K for the year ended December 31, 2024, as such risks may be updated in our subsequent filings with the Securities and Exchange Commission. You are cautioned not to place undue reliance on these forward-looking statements, which speak only as of the date hereof. All forward-looking statements are qualified in their entirety by these cautionary statements, and we undertake no obligation to revise or update this press release to reflect events or circumstances after the date hereof. Contacts: Celcuity Inc. Brian Sullivan, bsullivan@celcuity.com Vicky Hahne, vhahne@celcuity.com (763) 392-0123 Jodi Sievers, jsievers@celcuity.com (415) 494-9924

Phase 3Executive ChangeClinical Result

09 Feb 2026

·www.fiercepharma.com

Editor’s Corner: Pharma's slack tightening across pipelines, trust

Senior leaders from Bayer and Bristol Myers Squibb shared insights on navigating strategic constraints facing the pharmaceutical industry during Fierce JPM Week in San Francisco. Large drugmakers once had more room to absorb failure, both financially and reputationally, particularly during the height of the pre-pandemic era. Blockbuster franchises could offset years of uneven R&D returns, and missteps could more easily be managed.That room has narrowed. Revenue declines after patent loss are steep, with branded sales eroding quickly as generics or biosimilars enter the market. By 2030, more than $200 billion in biopharma industry revenues will face loss-of-exclusivity exposure, with another $200 billion at risk in the early 2030s as additional exclusivity cliffs hit.At the same time, scrutiny of pricing, patient access and corporate behavior has intensified from regulators and the public alike. That pressure is increasingly being reflected in how the industry is perceived.Declining satisfaction and perceptions of value, along with shifts in how younger people consume health information, have left the pharmaceutical industry facing a trust deficit. Combined with ongoing concerns about pricing and corporate motives, that gap suggests the pandemic-era boost to pharma’s reputation is fading and will require greater transparency and engagement to rebuild. The environment has created a narrowing margin for error, which was reflected in two conversations I had with senior executives from Bayer and Bristol Myers Squibb during Fierce JPM Week in San Francisco last month. One focused on pipeline discipline, the other on trust and corporate credibility. Both pointed to an underlying shift, with pharmas making earlier, harder decisions about development and capital while balancing competing demands from regulators, policymakers and the public. Decisions made years in advance Time is never neutral for companies built on blockbuster drugs. Patents expire, revenue erodes, and replacement products must be in motion long before losses show up in quarterly earnings reports.Christine Roth, Bayer’s executive vice president and head of global product strategy and commercialization, was direct about the typical timeline for major patent cliffs: planning needs to begin nearly a decade in advance.“It doesn’t happen in 12 months,” Roth said. “These are decisions you make eight years out.”The company spent the past five years pruning programs that were scientifically intriguing but commercially unlikely to differentiate, per Roth, while narrowing its focus to areas where it believed it could sustain scale, particularly oncology and cardiology.The German conglomerate made those decisions in anticipation of significant sales drops across key franchises. Xarelto, the blood thinner that began facing generic competition after its U.S. patent expired last year, saw sales fall 32.7% to 540 million euros in the three months ended Sept. 30. Pressure is also building elsewhere in the portfolio. Bayer, which handles ex-U.S. commercialization for Regeneron-partnered ophthalmology blockbuster Eylea, is facing a new biosim threat in Europe as of November. To help offset the revenue losses and drive growth, the company is relying on newer launches and indication expansions. Bayer’s Nubeqa was first cleared in 2019 for use in combination with androgen deprivation therapy (ADT) and the chemotherapy docetaxel to treat patients with metastatic castration-sensitive prostate cancer. In June 2025, it gained approval for use alongside ADT in patients who cannot tolerate chemotherapy.That expansion has begun to show up in the numbers, with Nubeqa sales up 50% year over year in the three months ended Sept. 30. In the same period, momentum began to build for Bayer's chronic kidney disease drug Kerendia, which was first approved in 2021 and picked up a second indication for heart failure last summer. Sales rose 75% year over year.Preparing for exclusivity losses also involved major changes to who gets a voice early at Bayer. Commercial teams are now embedded in discovery, weighing in on modality, formulation and competitive positioning well before a candidate reaches the clinic, Roth said. Questions that once surfaced at launch now arise at target selection.The shift is about timing. It results in fewer projects, earlier stops and capital concentrated on assets that clear both scientific and market hurdles, according to Roth. That discipline is being imposed as the economics of drug development grow less forgiving. A 2025 analysis of Deloitte data found that while overall return on investment in drug R&D ticked up modestly, the average cost to bring a new drug to market remains high, roughly $2.2 billion per asset, and peak sales forecasts per asset are slipping in many therapeutic areas outside GLP-1s.Those economic constraints are now shaping behavior inside companies.At Bayer, Roth described a cultural shift away from what she called “progression-seeking,” the instinct to push a program forward because it belongs to your team, toward “truth-seeking,” where teams evaluate their projects against the broader portfolio and step aside when necessary.“People need to put on their enterprise hat and think, based on what I’ve seen across the pipeline, is my project still one of the highest-impact opportunities?” Roth said. “Or is it time for us to free up resources so we can either start something that looks more promising or pour some gas on something that’s really moving ahead?”Pharma R&D has historically been tribal, with scientists fiercely protecting their programs. Getting people to kill their own work voluntarily requires a completely different incentive structure.Bayer's answer is what the company calls “dynamic shared ownership,” rolled out in 2024 and 2025 under CEO Bill Anderson, who took over in early 2023. Strip away the corporate jargon and, per Roth, it means this: every role exists to serve a product, a customer, or the teams that support them. “If you're not in service of a product, a customer or a product and customer team, then you probably won't be at Bayer for very much longer,” Roth said. That carries weight. Bayer has cut more than 13,500 jobs under Anderson's leadership.Describing what things look like now, Roth said the company ties budgets to specific development milestones, such as filing an investigational new drug application or reaching clinical trial benchmarks, rather than fixed annual allocations. Funding flows based on progress, and teams are judged on whether they hit objectives rather than how much of a budget they spend. Trust as currency On the same stage that day, Wendy Bartie, Bristol Myers Squibb's executive vice president of corporate affairs, was addressing a different constraint: credibility.“It is rare, if ever, that our industry or our companies aren't managing through some topic or issue that has the ability to impact reputation,” she said. “It's just the world in which we live and operate.”For BMS, trust is not optional. Bartie calls it “the trust advantage,” which she said determines whether a company has a seat at the table to advocate its position and whether it receives the benefit of the doubt when difficult issues arise.Her formula is straightforward: “You tell people what you're going to do and you actually show up and you do it.”The public, policymakers, investors and other stakeholders “will always view us through the lens of their vested interests,” Bartie said. She described the framework she uses internally to help teams navigate competing stakeholder expectations.“What is always consistent, irrespective of who your stakeholder is: I want you to tell me what you're doing. I want you to be really clear about what you're doing. I want you to explain the trade-offs and why you made the decisions that you made,” she said. “And I want you to operate with the highest degree of integrity.” Corporate affairs, in her view, serves as the connective tissue across an organization, translating business strategy into credible narratives for diverse stakeholders while bringing external expectations back into internal decision-making. That internal discipline, Bartie argued, matters most when it shows up in how patients actually access care.Access to care is where credibility ultimately gets tested, she said. “How you look, who you love, [and] where you live should not determine if you live,” she said, framing equity as a strategic necessity rather than a peripheral concern.She pointed to BMS’ work in Africa, where the company has expanded beyond HIV and AIDS into mental health, sickle cell disease and cancer. In the U.S., BMS is using community pharmacies for cardiovascular monitoring and virtual models for mental health in rural areas.These efforts are central to how the industry earns and preserves its credibility, she said. A common thread Roth and Bartie were addressing different audiences about different problems. One focused on the internal economics of drug development—the other on the external politics of trust. Taken together, their remarks point to a common reality: the constraints around the traditional pharmaceutical model are tightening.Capital is being allocated more selectively, reputational flexibility has thinned and decisions that once could be delayed are being pulled forward. The old playbook hasn't disappeared. What has changed is the degree of tolerance built into the system, both in how companies develop drugs and in how and when they explain their choices to the world around them.

Drug Approval

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
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
Castration-sensitive prostate cancer	China	Bayer HealthCare Pharmaceuticals, Inc.	16 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.

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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

Indication

Phase

Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT02200614 (ARAMIS, Pubmed \| Cancer Med)	Phase 3	Castration-Resistant Prostatic Cancer	1,509	Darolutamide + ADT	wchzvwocwz(syapugbpdg): HR = 0.36 (95.0% CI, 0.26 - 0.48) View more	Positive	01 Jan 2026
				Placebo + ADT
ChiCTR2500096436 (DAPLOM, ESMO_ASIA2025)	Phase 2	Castration-sensitive prostate cancer	60	Darolutamide + ADT + prostate arterial docetaxel infusion	iejtvogppc(algqtiiffg) = xvlpnmlfkq yjitnarclo (uhghaoscjz )	Positive	05 Dec 2025
ARAMIS (ESMO_ASIA2025)	Phase 3	Castration-Resistant Prostatic Cancer	76	Darolutamide + androgen-deprivation therapy	zsqpfztzal(gfvfhxsxdg) = rqffmpwsdb apoejgzrdh (mptqpmyevs ) View more	Positive	05 Dec 2025
ESMO_ASIA2025	Not Applicable	Hormone-dependent prostate cancer	25	Darolutamide + Docetaxel + ADT	ayurwpkmnl(fvxpbqqdsl) = zwzoysgxqk vwnuwnlubr (gqpjlvxlvl ) View more	Positive	05 Dec 2025
ESMO_ASIA2025	Not Applicable	Hormone-dependent prostate cancer	8	Darolutamide + Trans-arterial chemoperfusion by Docetaxel + ADT	qdekjuulym(bzlbyssubs) = glrbdslbev wrttfrahrq (jztmnxfudx ) View more	Positive	05 Dec 2025
NCT05794906 (ARASTEP, Pubmed \| Future Oncol)	Phase 3	Non-metastatic prostate cancer	970	Darolutamide + ADT	fhlvvccitk(ofwvyyinkz) = vfgtljppfu xozfqpmdvw (clffdslgih ) View more	Positive	14 Nov 2025
				Placebo + ADT	fhlvvccitk(ofwvyyinkz) = tkqbhcuxyt xozfqpmdvw (clffdslgih ) View more
NCT04122976 (DAROL, ESMO2025)	Not Applicable	Castration-Resistant Prostatic Cancer	799	Darolutamide	ixwpqzunlp(xpnsnrvktl) = ovrbxjieqp vwkryanvuk (kajhpimmud ) View more	Positive	17 Oct 2025
				Placebo	ixwpqzunlp(xpnsnrvktl) = lddnkotmrh vwkryanvuk (kajhpimmud ) View more
NCT02799602 (ARASENS, ESMO2025)	Phase 3	Metastatic Prostate Carcinoma	847	Lead-in ADT used	imqhzkjoav(rlctuxkxpa) = vxpxjyraof kuswwfhsla (vngghxlvwy ) View more	Positive	17 Oct 2025
				No lead-in ADT	imqhzkjoav(rlctuxkxpa) = rhxbqfiwgg kuswwfhsla (vngghxlvwy ) View more
ESMO2025	Not Applicable	Castration-sensitive prostate cancer	455	Darolutamide + Docetaxel	wcmybdxjrh(vuookzqiht) = acmjirswnp dmzxquxxdm (puoojawgxe )	Positive	17 Oct 2025
				Apalutamide	wcmybdxjrh(vuookzqiht) = eygucreqre dmzxquxxdm (puoojawgxe )
NCT06029036 (ESMO2025)	Phase 2	Neoadjuvant	53	Darolutamide + ADT	hvitjqcnss(lglbucqhwg) = yeqcdgynan zoejdpphgp (xftqipofdp ) View more	Positive	17 Oct 2025

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