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Last update 07 Nov 2025

Pembrolizumab

Last update 07 Nov 2025

Overview

R&D Status

Clinical Result

Translational Medicine

Overview

Basic Info

Drug Type

Monoclonal antibody

Synonyms

Lambrolizumab, Pembrolizumab (Genetical Recombination), Pembrolizumab (genetical recombination) (JAN)

+ [11]

Target

PD-1

Action

inhibitors

Mechanism

PD-1 inhibitors(Programmed cell death protein 1 inhibitors)

Therapeutic Areas

NeoplasmsImmune System DiseasesInfectious Diseases+ [13]

Active Indication

Locally Advanced Head and Neck Squamous Cell CarcinomaUnresectable Hepatocellular CarcinomaUnresectable Pleural Malignant Mesothelioma+ [345]

Inactive Indication

Acute myeloid leukemia with mutated NPM1Adenocarcinoma, metastaticAdvanced Colorectal Adenocarcinoma+ [90]

Originator Organization

Merck & Co., Inc.

Active Organization

MSD KK (Tokyo)Merck Sharp & Dohme BV

MSD R&D (China) Co. Ltd.

+ [12]

Inactive Organization

Viralytics Pty Ltd.

License Organization

Nektar Therapeutics

NeoImmuneTech, Inc.

Canada Pension Plan Investment Board

+ [80]

Drug Highest PhaseApproved

First Approval Date

United States (04 Sep 2014),

Melanoma

RegulationPriority Review (United States), Breakthrough Therapy (United States), Accelerated Approval (United States), Orphan Drug (United States), PRIME (European Union), Priority Review (China), Orphan Drug (Australia), Priority Review (Australia), Conditional marketing approval (China), Orphan Drug (Japan)

Structure/Sequence

Sequence Code 93660H

Source: *****

Sequence Code 93670L

Source: *****

2,529

Clinical Trials associated with Pembrolizumab

NCT06524544

/ RecruitingPhase 3IIT

A Phase III Randomized Trial of Pembrolizumab in Combination With Sacituzumab Govitecan vs Standard of Care in Anti-PD(L)1-Resistant Advanced Urothelial Cancer

This phase III trial compares the effectiveness of pembrolizumab and sacituzumab govitecan to standard of care in treating patients with urothelial cancer that has spread to nearby tissue or lymph nodes (locally advanced) or that has spread to other places in the body (metastatic). Immunotherapy with monoclonal antibodies, such as pembrolizumab, may help the body's immune system attack the cancer, and may interfere with the ability of tumor cells to grow and spread. Sacituzumab govitecan is a monoclonal antibody, called sacituzumab, linked to a chemotherapy drug called govitecan. Sacituzumab attaches to TROP2 positive tumor cells in a targeted way and delivers govitecan to kill them. The usual treatment approach is treatment with chemotherapy such as cisplatin, carboplatin, gemcitabine, docetaxel or paclitaxel. Cisplatin is in a class of medications known as platinum-containing compounds. It works by killing, stopping or slowing the growth of tumor cells. Carboplatin is in a class of medications known as platinum-containing compounds. It works in a way similar to the anticancer drug cisplatin, but may be better tolerated than cisplatin. Carboplatin works by killing, stopping or slowing the growth of tumor cells. Gemcitabine is a chemotherapy drug that blocks the cells from making deoxyribonucleic acid and may kill tumor cells. Docetaxel is in a class of medications called taxanes. It stops tumor cells from growing and dividing and may kill them. Paclitaxel is in a class of medications called antimicrotubule agents. It stops tumor cells from growing and dividing and may kill them. Giving pembrolizumab and sacituzumab govitecan may be more effective than usual care of carboplatin or cisplatin with gemcitabine, docetaxel or paclitaxel in treating patients with locally advanced or metastatic urothelial cancer.

Start Date20 Jul 2026

Sponsor / Collaborator

National Cancer Institute

NCT07061977

/ RecruitingPhase 3IIT

NRG-GY037: A Phase III Study of Induction Pembrolizumab and Chemotherapy Followed by Chemoradiation and Pembrolizumab Versus Chemoradiation and Pembrolizumab Both Followed by Pembrolizumab for High Risk Locally Advanced Cervical Cancer

This phase III trial compares the addition of induction chemotherapy, with carboplatin, paclitaxel and pembrolizumab, to chemotherapy and radiation, with cisplatin and pembrolizumab followed by pembrolizumab maintenance for the treatment of patients with cervical cancer that has spread to nearby tissue or lymph nodes (locally advanced). Carboplatin is in a class of medications known as platinum-containing compounds. It works in a way similar to the anticancer drug cisplatin, but may be better tolerated than cisplatin. Carboplatin works by killing, stopping or slowing the growth of cancer cells. Paclitaxel is in a class of medications called antimicrotubule agents. It stops cancer cells from growing and dividing and may kill them. Immunotherapy with monoclonal antibodies, such as pembrolizumab, may help the body's immune system attack the cancer, and may interfere with the ability of tumor cells to grow and spread. Radiation therapy uses high energy x-rays, particles, or radioactive seeds to kill cancer cells and shrink tumors. Cisplatin is in a class of medications known as platinum-containing compounds. It works by killing, stopping or slowing the growth of cancer cells. Adding induction chemotherapy to the usual treatment of chemotherapy and radiation followed by maintenance may be more effective in treating patients with high risk, locally advanced cervical cancer.

Start Date26 Jun 2026

Sponsor / Collaborator

National Cancer Institute

NCT07061964

/ RecruitingPhase 2IIT

Single Arm Phase II Study of Bladder Preservation With Immunoradiotherapy After a Clinically Meaningful Response to Neoadjuvant Therapy in Patients With Muscle Invasive Bladder Cancer (BRIGHT)

This phase II trial tests the effect of giving pembrolizumab in combination with radiation therapy after chemotherapy in preventing surgery to remove the bladder in patients with muscle invasive bladder cancer. Standard of care therapy includes chemotherapy before surgery (neoadjuvant) to shrink or get rid of the tumor. Immunotherapy with monoclonal antibodies, such as pembrolizumab, may help the body's immune system attack the tumor, and may interfere with the ability of tumor cells to grow and spread. Radiation therapy uses high energy x-rays, particles, or radioactive seeds to kill cancer cells and shrink tumors. Photon beam radiation therapy is a type of radiation therapy that uses x-rays or gamma rays that come from a special machine called a linear accelerator. The radiation dose is delivered at the surface of the body and goes into the tumor and through the body. Giving pembrolizumab in combination with radiation therapy after neoadjuvant chemotherapy may help prevent surgical removal of the bladder in patients with muscle invasive bladder cancer.

Start Date01 Jun 2026

Sponsor / Collaborator

National Cancer Institute

100 Clinical Results associated with Pembrolizumab

100 Translational Medicine associated with Pembrolizumab

100 Patents (Medical) associated with Pembrolizumab

10,520

Literatures (Medical) associated with Pembrolizumab

01 Feb 2026·COMPUTATIONAL BIOLOGY AND CHEMISTRY

Targeting colorectal cancer liver metastasis through repurposing metabolic and immune inhibitors: A theoretical study

Article

Author: Lahiri, Aditya ; Datta, Aniruddha ; Mondal, Madhurima

Liver metastasis from colorectal cancer is a major cause of death in patients with advanced colorectal cancer (CRC) and remains a difficult challenge in oncology. In spite of commendable developments in medical inventions, the complexity and poor prognosis of metastatic stage, alliterative strategies are required to address Colorectal cancer liver metastasis (CRLM). This paper presents a computational study on drug repurposing for CRLM using a Boolean Network model. We comprehensively analyze CRLM signaling pathways such as WNT, PI3K/AKT/mTOR, MAPK, Hedgehog, TGF-β, NF-kB, NOTCH and HGF and target them with metabolic and immune inhibitors. This study utilizes a computational analysis to evaluate single and multi-agent treatments across scenarios involving single and multiple genetic mutations. Our findings highlights the efficacy of metabolic inhibitors such as Simvastatin, Metformin, and predict compatible partner drugs to enhance their efficacy. Additionally, we predict possible improvements for CRLM treatment using an immunotherapy drug like Pembrolizumab. Overall, this paper suggests potential combinations requiring experimental validation for drug repurposing to improve CRLM treatment outcomes.

01 Jan 2026·TALANTA

Biosimilarity and advanced structural characterization of monoclonal antibodies charge variants using capillary zone electrophoresis and mass spectrometry

Article

Author: Joomun, Rania ; Gahoual, Rabah ; Alez-Martin, Lola ; François, Yannis-Nicolas ; Mignet, Nathalie ; Houzé, Pascal

Monoclonal antibodies (mAbs) structural complexity arises from their macromolecular nature and their propensity to undergo post-translational modifications (PTM), potentially leading to the formation of charge variants. Capillary zone electrophoresis (CZE) showed to be particularly relevant for their analysis, however the selectivity provided by CZE separation is not completely elucidated. In this work, CZE-UV analysis was used to characterize charge variants for biosimilars products corresponding to infliximab. Results demonstrated the possibility to identify faint variations between the different products showing its applicability to contribute to mAbs biosimilarity assessment. Enzymatic treatment allowed to attribute the origin of infliximab charge variants. CZE-UV analysis of pembrolizumab showed that none of the five charge variants separated were originating from C-terminal lysine residues and/or N-glycans. To enable further identification, an analytical strategy was developed to achieve CZE-UV fraction collection and enrichment of mAb charge variants followed by systematic offline characterization in CE coupled to tandem mass spectrometry (MS/MS). CE-MS/MS experiments allowed the identification of different types of PTMs such as N-terminal pyroglutamic acid formation and asparagine deamidation for charge variant fractions correlated with decreased mobility. In addition, for the first time succinimide intermediate formation could be successfully characterized using CE-MS/MS data, which could be correlated to increased mobility. Thus, the CZE-UV separation resulted from the synergistic effect of several simultaneous PTMs affecting the apparent mobilities of the charge variants. As a consequence, experiments illustrated the relevance and potential of intact mAbs analysis using CZE-UV to provide an overview of the structural diversity of therapeutic mAbs.

01 Jan 2026·JOURNAL OF PHARMACEUTICAL SCIENCES

Subcutaneously administered anti-PD-(L)1 antibodies are predominantly absorbed via the lymphatic system, resulting in high drug exposure to draining lymph nodes

Article

Author: Fei, Xiaoxuan ; Sun, Lie ; Yan, Simin ; Li, Li ; Zou, Jianjun ; Ge, Weihong ; Hu, Luojuan ; Han, Sifei ; Zhang, Huimin ; Pei, Junyi

Compared to classic intravenous (IV) administration, subcutaneous (SC) delivery of monoclonal antibodies (mAbs) offers new opportunities to improve patient compliance and healthcare efficiency. However, insufficient understanding of drug absorption process following SC administration, particularly the role of lymphatic transport, may hinder the development of SC formulations for mAbs. The current study aimed to examine the absorption route of widely used anti-PD-(L)1 mAbs following SC injection, and four marketed products (Pembrolizumab, Tislelizumab, Envafolimab, Sugemalimab) were selected as the model drugs. In the thoracic lymph duct-cannulated rat model, all mAbs were found to be primarily absorbed via the lymphatics following SC injection, with 63.1-72.0 % of the administered dose recovered in the thoracic lymph, contributing to >80 % of SC bioavailability. This absorption pattern also resulted in elevated exposure of mAbs in draining lymph nodes (an order of magnitude higher drug concentrations compared to the systemic drug exposure). In addition, markedly different lymphatic absorption profiles were observed following SC administration at different sites, reflecting specific draining routes associated with certain anatomical regions in the rat. Our data suggested that the food pad is likely the optimal SC injection site for quantitative studies of lymphatic transport, whereas injection to the lower hind leg (a common SC injection site in previous studies) appeared to underestimate the absolute extent of lymphatic drug transport in the thoracic lymph duct-cannulated rat model, as lymphatic drainage from this region partially bypasses the cannulation site, leading to incomplete collection of draining lymph.

5,951

News (Medical) associated with Pembrolizumab

06 Nov 2025

·ir.cytomx.com

CytomX Therapeutics Announces Third Quarter 2025 Financial Results and Provides Business Update

- CX-2051 Phase 1 data update on track for Q1 2026 - - CX-2051 Phase 1b CRC combination study with bevacizumab to start in Q1 2026 - - Positive CX-801 Phase 1 monotherapy biomarker data at SITC 2025 supportive of ongoing Phase 1 combination study with KEYTRUDA® (pembrolizumab) in melanoma - - Company to host conference call today at 5 p.m. EST / 2 p.m. PST - SOUTH SAN FRANCISCO, Calif. , Nov. 06, 2025 (GLOBE NEWSWIRE) -- CytomX Therapeutics, Inc. (Nasdaq: CTMX), a leader in the field of masked, conditionally activated biologics, today announced third quarter 2025 financial results and provided a business update. “CytomX continued to execute against its pipeline priorities this quarter, highlighted by robust Phase 1 expansion enrollment for CX-2051. We remain on track for a CX-2051 Phase 1 data update in Q1 2026. Looking ahead to 2026, CX-2051 is well positioned as a first-in-class EpCAM-directed, topoisomerase-1 ADC designed to address the high unmet need in CRC and a wide range of other EpCAM-expressing indications. CytomX’s top priority is to advance CX-2051 towards a potential registrational study in advanced, late-line CRC. Additionally, we continue to plan for focused investments to further unlock the potential of CX-2051, including moving into earlier lines of CRC therapy and additional EpCAM positive cancers,” said Sean McCarthy , D.Phil ., chief executive officer and chairman of CytomX. Dr. McCarthy continued “We are also pleased with the dose escalation progress for our PROBODY® interferon alpha-2b, CX-801, and look forward to presenting encouraging initial biomarker data at SITC which underscore this potent masked cytokine’s therapeutic potential in combination with checkpoint inhibitors in advanced melanoma.” Q3 2025 Pipeline Program Updates: CX-2051 (EpCAM PROBODY Topo-1 ADC) CX-2051 Phase 1 dose expansions across the 7.2 mg/kg, 8.6 mg/kg, and 10 mg/kg doses, administered every three weeks (Q3W) are ongoing. In Q3 2025, dose expansion enrollment continued with the goal of supporting a potential registrational study of CX-2051 monotherapy in advanced CRC. Phase 1 study enrollment is projected to reach approximately 100 patients by the planned CX-2051 Phase 1 update in Q1 2026. A Phase 1b CX-2051 combination study with bevacizumab in CRC is expected to start in Q1 2026, data from which is intended to inform potential late-phase development in earlier lines of CRC therapy. Evaluation ongoing of multiple non-CRC, EpCAM-expressing tumor indications for potential future CX-2051 development. CX-801 (PROBODY Interferon alpha-2b) Society of Immunotherapy of Cancer (SITC) 2025 Annual Meeting CX-801 monotherapy biomarker data in advanced melanoma patients to be presented that support CX-801’s mechanism of action and the ongoing combination study with KEYTRUDA® (pembrolizumab). CX-801 monotherapy has been well tolerated at doses exceeding the approved dose of unmasked IFNα2b.1 Gene expression analysis of pre- and post-treatment patient tumor biopsies demonstrated consistently increased expression of interferon-stimulated genes. Patients demonstrated evidence of T-cell and NK cell activation and upregulation of immune checkpoint genes, including PD-1 and PD-L1. Evidence of sustained elevation of CXCL10 in the tumor but not the blood was observed, suggesting preferential CX-801 activity in the tumor versus the periphery. PK analysis also demonstrated dose-proportional exposure of CX-801, which remained predominantly in its intact (masked) form in circulation. The CX-801 Phase 1 study is ongoing with a focus in advanced melanoma. CX-801 monotherapy dose escalation has reached the fourth dose level. In May 2025 , Phase 1 dose escalation of CX-801 in combination with KEYTRUDA® was initiated. Dose escalation of CX-801 in combination with KEYTRUDA® is currently enrolling the 2nd dose level. Initial clinical data for CX-801 in the combination with KEYTRUDA® in advanced melanoma is anticipated in 2026. CX-801 monotherapy biomarker data in advanced melanoma patients to be presented that support CX-801’s mechanism of action and the ongoing combination study with KEYTRUDA® (pembrolizumab). CX-801 monotherapy has been well tolerated at doses exceeding the approved dose of unmasked IFNα2b.1 Gene expression analysis of pre- and post-treatment patient tumor biopsies demonstrated consistently increased expression of interferon-stimulated genes. Patients demonstrated evidence of T-cell and NK cell activation and upregulation of immune checkpoint genes, including PD-1 and PD-L1. Evidence of sustained elevation of CXCL10 in the tumor but not the blood was observed, suggesting preferential CX-801 activity in the tumor versus the periphery. PK analysis also demonstrated dose-proportional exposure of CX-801, which remained predominantly in its intact (masked) form in circulation. KEYTRUDA® is a registered trademark of Merck Sharp & Dohme LLC , a subsidiary of Merck & Co., Inc., Rahway, NJ , USA Corporate and Financial: Corporate: In October 2025 , announced the appointment of Rachael Lester , MBA as Senior Vice President, Chief Business Officer. Financial: CytomX ended the third quarter of 2025 with $143.6 million of cash, cash equivalents and investments with expected cash runway to the second quarter of 2027. Research Pipeline and Collaborations: CytomX has research collaborations with Bristol Myers Squibb , Amgen, Astellas, Regeneron, and Moderna. Multiple drug discovery programs continue across our research collaborations with a focus on bispecific immunotherapies, including T-cell engagers. At SITC 2025, preclinical data will be presented for CX-908, a dually masked PROBODY T-cell Engager targeting CDH3 and CD3. CX-908 potently induced tumor regressions in established breast and lung cancer xenograft tumor models and demonstrated a 100-fold improvement in tolerability, including significantly reduced cytokine release vs. an unmasked CDH3xCD3 molecule. In October 2025 , announced the appointment of Rachael Lester , MBA as Senior Vice President, Chief Business Officer. CytomX ended the third quarter of 2025 with $143.6 million of cash, cash equivalents and investments with expected cash runway to the second quarter of 2027. CytomX has research collaborations with Bristol Myers Squibb , Amgen, Astellas, Regeneron, and Moderna. Multiple drug discovery programs continue across our research collaborations with a focus on bispecific immunotherapies, including T-cell engagers. At SITC 2025, preclinical data will be presented for CX-908, a dually masked PROBODY T-cell Engager targeting CDH3 and CD3. CX-908 potently induced tumor regressions in established breast and lung cancer xenograft tumor models and demonstrated a 100-fold improvement in tolerability, including significantly reduced cytokine release vs. an unmasked CDH3xCD3 molecule. _______________1 Merck & Co., Inc. (2018). Sylatron (peginterferon alfa-2b) prescribing information. U.S. Food and Drug Administration Third Quarter 2025 Financial Results: Cash, cash equivalents and investments totaled $143.6 million as of September 30, 2025 , compared to $158.1 million as of June 30, 2025 . Total revenue was $6.0 million for the quarter ended September 30, 2025 , compared to $33.4 million for the quarter ended September 30, 2024 . The decrease in revenue was driven primarily by the completion of our performance obligations in the Bristol Myers Squibb collaboration and a decrease in Moderna activities due to Moderna budget considerations. Total operating expense in the third quarter of 2025 was $21.7 million compared to $29.3 million in the third quarter of 2024, a decrease of $7.6 million . Research and development expenses were $15.3 million for the three months ended September 30, 2025 , a decrease of $6.1 million compared to the corresponding period of 2024. Reduced research and development expenses were primarily due to a reduction in CX-904 spend due to program de-prioritization in Q1 2025, reduced research expenses following the Q1 2025 restructuring, and lower CX-2051 manufacturing expenses which was partially offset by the increase in CX-2051 clinical spend. General and administrative expenses were $6.4 million for the three months ended September 30, 2025 , a decrease of $1.5 million compared to the corresponding period of 2024. The decrease in general and administrative expenses was primarily driven by personnel costs as well as patent and legal expenses. About CytomX Therapeutics CytomX is a clinical-stage, oncology-focused biopharmaceutical company focused on developing novel conditionally activated, masked biologics designed to be localized to the tumor microenvironment. By pioneering a novel pipeline of localized biologics, powered by its PROBODY® therapeutic platform, CytomX’s vision is to create safer, more effective therapies for the treatment of cancer. CytomX’s multi-modality technology platform has produced therapeutic candidates across multiple treatment modalities including antibody-drug conjugates (ADCs), T-cell engagers, and immune modulators such as cytokines. CytomX’s current clinical-stage pipeline includes CX-2051 and CX-801. CX-2051 is a masked, conditionally activated ADC directed toward epithelial cell adhesion molecule (EpCAM), armed with a topoisomerase-1 inhibitor payload. CX-2051 has potential applicability across multiple EpCAM-expressing epithelial cancers, including CRC, and was discovered in collaboration with ImmunoGen. CX-801 is a masked interferon alpha-2b PROBODY® cytokine with broad potential applicability in traditionally immuno-oncology sensitive as well as insensitive (cold) tumors. CytomX has established strategic collaborations with multiple leaders in oncology, including Amgen, Astellas, Bristol Myers Squibb , Regeneron and Moderna. For more information about CytomX and how it is working to make conditionally activated treatments the new standard-of-care in the fight against cancer, visit www.cytomx.com and follow us on LinkedIn and X (formerly Twitter). CytomX Therapeutics Forward-Looking StatementsThis press release includes forward-looking statements. Such forward-looking statements involve known and unknown risks, uncertainties and other important factors that are difficult to predict, may be beyond our control, and may cause the actual results, performance, or achievements to be materially different from any future results, performance or achievements expressed or implied in such statements, including those related to CX-2051 and CX-801. Accordingly, you should not rely on any of these forward-looking statements, including those relating to the potential benefits, safety and efficacy or progress of CytomX’s or any of its collaborative partners’ product candidates, including CX-2051 and CX-801, the potential benefits or applications of CytomX’s PROBODY® therapeutic platform, CytomX’s or its collaborative partners’ ability to develop and advance product candidates into and successfully complete clinical trials, including the ongoing and planned clinical trials of CX-2051 and CX-801 and the timing of initial and ongoing data availability for our clinical trials, including CX-2051 and CX-801, and other development milestones. Risks and uncertainties that contribute to the uncertain nature of the forward-looking statements include: the unproven nature of CytomX’s novel PROBODY® therapeutic technology; uncertainties around the Company’s ability to raise sufficient funds to carry out its planned research and development; CytomX’s clinical trial product candidates are in the initial stages of clinical development and its other product candidates are currently in preclinical development, and the process by which preclinical and clinical development could potentially lead to an approved product is long and subject to significant risks and uncertainties, including the possibility that the results of preclinical research and early clinical trials, including initial CX-2051 and CX-801 results, may not be predictive of future results; the possibility that CytomX’s clinical trials will not be successful; the possibility that current preclinical research may not result in additional product candidates; CytomX’s dependence on the success of CX-2051 and CX-801; CytomX’s reliance on third parties for the manufacture of the Company’s product candidates; possible regulatory developments in the United States and foreign countries, including China and the European Union ; and the risk that we may incur higher costs than expected for research and development or unexpected costs and expenses. Additional applicable risks and uncertainties include those relating to our preclinical research and development, clinical development, and other risks identified under the heading "Risk Factors" included in CytomX’s Quarterly Report on Form 10-Q filed with the SEC on November 6, 2025 . The forward-looking statements contained in this press release are based on information currently available to CytomX and speak only as of the date on which they are made. CytomX does not undertake and specifically disclaims any obligation to update any forward-looking statements, whether as a result of any new information, future events, changed circumstances or otherwise. PROBODY is a U.S. registered trademark of CytomX Therapeutics, Inc. All other trademarks are the properties of their respective owners. Company Contact: Chris Ogden SVP, Chief Financial Officercogden@cytomx.com Investor Contact:Precision AQ (formerly Stern Investor Relations) Stephanie Ascher Stephanie.Ascher@precisionaq.com Media Contact: Redhouse Communications Teri Dahlman teri@redhousecomms.com __________________(1) The condensed balance sheet as of December 31, 2024 was derived from the audited financial statements included in the Company's Annual Report on Form 10-K for the year ended December 31, 2024 . Source: CytomX Therapeutics Inc.

Phase 1Executive ChangeFinancial Statement

05 Nov 2025

·www.fiercepharma.com

After shaky Q3, Novo's new CEO says company's diabetes and obesity turnaround is a 'marathon, not a sprint'

In Q3, Novo Nordisk ginned up sales of 74.9 billion Danish kroner ($11.5 billion), up 5% from the sum it generated in 2024’s third quarter but down sequentially from the previous two earnings periods in 2025. Less than three months into his tenure, Novo Nordisk’s new CEO has undeniably left his mark on the company, launching a sweeping restructuring drive and recently cutting in on Pfizer’s planned acquisition of metabolic biotech Metsera in a bid to restore Novo’s diabetes and obesity supremacy. Now, speaking to reporters during his first quarterly conference call at the company helm, Maziar Mike Doustdar made clear Wednesday that expanding access to Novo’s medicines—and continuing to unlock novel avenues for sales—will be key as Novo aims to address its recent growth slowdown.The need for a turnaround at the Danish drug giant was apparent in the company’s third-quarter earnings, which paled in comparison to the recent performance of its chief rival in the diabetes and obesity space, Eli Lilly.For the three months that ended in September, Novo Nordisk ginned up sales of 74.9 billion Danish kroner ($11.5 billion), up 5% from the sum it generated in 2024’s third quarter but down sequentially from the previous two quarters in 2025, according to a financial workbook the company posted alongside its Nov. 05 earnings announcement.Looking at the numbers, Novo’s total GLP-1 sales for the period, which primarily include Wegovy in obesity and Ozempic in type 2 diabetes, clocked in at 36.7 billion kroner ($5.6 billion), up around 5% from the amount they generated over the same period last year.For comparison, Lilly last week reported a stellar Q3 in which combined sales of its GIP/GLP-1 drugs reached $10.1 billion. The sales haul from Lilly's tirzepatide molecule has, for two periods now, eclipsed the world’s previous best-selling medicine, Keytruda. Novo was first to market with an obesity GLP-1 in Wegovy, which unlocked a wave of public and industry interest in the class’s impressive potential in weight loss and other related conditions. Nevertheless, Novo Nordisk has grappled with supply issues, access hurdles and, more recently, fierce competition from Eli Lilly’s rival GIP/GLP-1 agonists Mounjaro and Zepbound.Add to that a rampant compounding problem in the U.S., and Novo’s share price has taken a sharp nosedive since around the midpoint of last year.Now, Novo is narrowing its guidance again for 2025, setting the expectation to deliver revenue growth in the range of 8% to 11%. As of August, Novo had said it expected to chart growth between 8% and 14%. The company is also cutting its operating profit forecast from a previous range of 10% to 16% growth to just 4% to 7%.On a conference call Wednesday morning, Novo CEO Doustdar attributed the guidance downgrade to expected “lower growth for GLP-1 treatments in diabetes and obesity,” signaling that Novo is far from out of the woods when it comes to its metabolic market struggles.Throughout the call, Doustdar laid out his thesis for Novo’s return to growth, as well as the bona fides that he feels qualify him to shepherd the Danish drug giant.Reporters also pressed Doustdar directly—as someone who cut his teeth on the sales side of Novo’s business—on his feelings about losing ground in the market to Eli Lilly’s rival incretin meds Mounjaro and Zepbound.“I would say that, as a person who has grown up in the commercial part of the organization, you never liked losing market share. So, that goes without saying,” Doustdar said.“But it is really not about market share when you’re dealing with obesity at this point of time,” he continued. “It is about market access and expanding the market. There are a billion people out there that are suffering from this condition. Unfortunately, us and all of our competitors combined are going back and forth trying to find one or two million patients and share that part of the pie. That is not the way to give access to these innovative medications.”Doustdar added that he believes semaglutide—the molecule underpinning Wegovy and Ozempic—has “huge potential” to reach “many, many more patients,” stressing that Novo will home in on “market expansion as we go forward.”Novo Nordisk, like many of its Big Pharma peers, has turned to direct-to-consumer sales channels as a potential avenue to expand access to its drugs. Growing its offering—dubbed NovoCare Pharmacy—in that area will be paramount to meeting increasing “consumer-like behavior” in the market, Doustdar noted.“I think one of the major issues that we are trying to address is that there are 100 million patients in [the] U.S. today that are suffering from obesity. Fifty-five million of them are insured,” the CEO explained. “Unfortunately, many of these individuals, despite their insurances, are still not getting proper access to medications. That’s also why they go to the cash channels.”As for Doustdar’s personal capacity to guide Novo back to the top of the diabetes and obesity market, “I would not have taken the job if I didn’t feel confident that we’ll be able to contain and sustain Novo Nordisk leadership in diabetes and obesity,” Doustdar said during Wednesday’s call. “That is what we do,” he added, noting that “it’s a marathon, not a sprint.”“There is no doubt that right now we are seeing some headwinds—competitor headwinds. But this is also when we are at our best and strongest,” Doustdar stressed.He pointed not only to the strength and global recognition of semaglutide, but also Novo’s R&D pipeline and the manufacturing infrastructure it’s built out as evidence that the company has laid the groundwork to succeed.Where the question of GLP-1 access is concerned, pricing conversations are sure to follow, and Doustdar was also quick to confirm that Novo is working with the White House to reach an accord on the costs of its medications in the U.S.“What I will be able to tell you is that we have been in dialogues with the U.S. government for a long time now,” Doustdar said. “Our aims are quite aligned with one another. We would like to get our medications access to as many Americans as possible. Unfortunately, that’s not the case today. So, those discussions and dialogues are ongoing.”While the CEO’s comments provided little color on the particulars of the pricing talks, they lent weight to reports earlier this week that Novo and Lilly have engaged in talks with the U.S. government to offer obesity drugs at prices as low as $149 a month in exchange for coverage commitments from federal payers.While several other drugmakers have been clear about their role in discussions with the Trump administration to lower drug prices—and win some relief from the government’s threatened pharmaceutical import tariffs—Novo has generally been quieter on the U.S. policy front in 2025.Novo announced that Doustdar would replace the company’s previous CEO, Lars Fruergaard Jørgensen, back in July. At the time, the company was clear that it needed new leadership to navigate “recent market challenges”—alluding to Lilly and the U.S. compounding industry—and to restore the company’s share price.Since assuming the chief executive’s seat in early August, Doustdar has certainly made a strong impression on the company, kicking off a cost savings drive that will result in some 9,000 layoffs worldwide and last week, making a surprise counteroffer in Pfizer’s attempt to purchase obesity biotech Metsera.The company will also host an extraordinary general meeting later this month to appoint several new members to its board of directors following a stalemate in leadership discussions with Novo’s chief shareholder, the Novo Nordisk Foundation. In another new shake-up at the Danish drugmaker, Henrik Wulff, who’s served as Novo’s EVP of chemistry, manufacturing and controls (CMC) and product supply for a decade, will part ways on Jan. 1. Wulff’s role will be taken over by Kasper Bødker Mejlvang, who is currently Novo’s SVP for the Japan region, the company said in a Nov. 5 securities filing.Mejlvang himself has been with Novo for more than 20 years, primarily working in the areas of supply and CMC, the company said.

AcquisitionExecutive Change

05 Nov 2025

·pharma.economictimes.indiatimes.com

Merck secures $700 million funding from Blackstone to develop cancer therapy

Bengaluru: Merck said on Tuesday that it has entered into an agreement to receive funds managed by Blackstone Life Sciences for $700 million to develop an experimental cancer therapy. Under the terms of the agreement, Blackstone's drug development unit will fund a portion of the development costs to test sac-TMT , an experimental antibody-drug conjugate . Antibody-drug conjugates are designed to deliver an anti-cancer drug more precisely to malignant cells, causing less damage to healthy cells than chemotherapy. Merck is currently evaluating sac-TMT in 15 global late-stage trials spanning six tumor types, including breast, endometrial and lung cancers. The company is working on adding new drugs to its pipeline as its blockbuster cancer drug Keytruda faces competition from cheaper biosimilars later this decade. "We are making important investments...to sustain our business for the future, while remaining disciplined towards maintaining an appropriate financial profile," said Caroline Litchfield, chief financial officer, Merck. The payment is expected to be made throughout 2026, the companies said. Blackstone is eligible to receive low-to-mid single-digit royalties on net sales of sac-TMT, contingent upon receipt of regulatory approval in the U.S. Sac-TMT targets a protein called trophoblast cell-surface antigen 2, found on the surface of various cancer cells. Antibody-drug conjugates that target this protein have shown encouraging anti-tumor activity in clinical studies, Merck said. The company added that it will retain control over the development, manufacturing and commercialization of sac-TMT, and Blackstone will not receive any rights to the cancer therapy. Sac-TMT is being developed as part of an exclusive license and collaboration agreement with Sichuan Kelun-Biotech Biopharmaceutical. (Reporting by Sneha S K in Bengaluru; Editing by Vijay Kishore)

License out/inADC

100 Deals associated with Pembrolizumab

External Link

KEGG	Wiki	ATC	Drug Bank
D10574	Pembrolizumab	L01XC18	DB09037

R&D Status

Approved

10 top approved records.

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Indication	Country/Location	Organization	Date
Locally Advanced Head and Neck Squamous Cell Carcinoma	Iceland	Merck Sharp & Dohme BV	30 Oct 2025
Locally Advanced Head and Neck Squamous Cell Carcinoma	Liechtenstein	Merck Sharp & Dohme BV	30 Oct 2025
Locally Advanced Head and Neck Squamous Cell Carcinoma	Norway	Merck Sharp & Dohme BV	30 Oct 2025
Unresectable Hepatocellular Carcinoma	China	Merck Sharp & Dohme LLC	10 Jun 2025
Unresectable Pleural Malignant Mesothelioma	Iceland	Merck Sharp & Dohme BV	16 Apr 2025
Unresectable Pleural Malignant Mesothelioma	Norway	Merck Sharp & Dohme BV	16 Apr 2025
Unresectable Urothelial Carcinoma	European Union	Merck Sharp & Dohme BV	25 Jul 2024
Unresectable Urothelial Carcinoma	Iceland	Merck Sharp & Dohme BV	25 Jul 2024
Unresectable Urothelial Carcinoma	Liechtenstein	Merck Sharp & Dohme BV	25 Jul 2024
Unresectable Urothelial Carcinoma	Norway	Merck Sharp & Dohme BV	25 Jul 2024
Advanced Endometrial Carcinoma	United States	Merck Sharp & Dohme LLC	17 Jun 2024
Microsatellite instability-high Endometrial Carcinoma	United States	Merck Sharp & Dohme LLC	17 Jun 2024
Mismatch repair-deficient Endometrial Carcinoma	United States	Merck Sharp & Dohme LLC	17 Jun 2024
Advanced gastric carcinoma	Japan	MSD KK (Tokyo)	17 May 2024
recurrent gastric cancer	Japan	MSD KK (Tokyo)	17 May 2024
Unresectable Biliary Tract Carcinoma	Canada	Merck Sharp & Dohme Corp.	09 May 2024
Advanced biliary tract cancer	China	Merck Sharp & Dohme LLC	30 Jan 2024
Locally Advanced Cholangiocarcinoma	China	Merck Sharp & Dohme LLC	30 Jan 2024
stomach adenocarcinoma	Norway	Merck Sharp & Dohme BV	20 Dec 2023
HER2 negative Gastric Cancer	United States	Merck Sharp & Dohme LLC	16 Nov 2023

Developing

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Muscle Invasive Bladder Carcinoma	NDA/BLA	United States	Merck & Co., Inc.	23 Oct 2025
Recurrent Platinum-Resistant Ovarian Carcinoma	NDA/BLA	United States	Merck & Co., Inc.	20 Oct 2025
Small intestine carcinoma	NDA/BLA	European Union	Merck Sharp & Dohme Corp.	25 Mar 2022
Ovarian Epithelial Carcinoma	Phase 3	United States	Merck Sharp & Dohme Corp.	13 Dec 2021
Ovarian Epithelial Carcinoma	Phase 3	Japan	Merck Sharp & Dohme Corp.	13 Dec 2021
Ovarian Epithelial Carcinoma	Phase 3	Belgium	Merck Sharp & Dohme Corp.	13 Dec 2021
Ovarian Epithelial Carcinoma	Phase 3	Canada	Merck Sharp & Dohme Corp.	13 Dec 2021
Ovarian Epithelial Carcinoma	Phase 3	Colombia	Merck Sharp & Dohme Corp.	13 Dec 2021
Ovarian Epithelial Carcinoma	Phase 3	Denmark	Merck Sharp & Dohme Corp.	13 Dec 2021
Ovarian Epithelial Carcinoma	Phase 3	Germany	Merck Sharp & Dohme Corp.	13 Dec 2021

Clinical Result

Indication

Phase

Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT04370509 (CTgov)	Phase 2	Metastatic Renal Cell Carcinoma \| Advanced Renal Cell Carcinoma \| Renal Cell Carcinoma ... View more	6	Cytoreductive Nephrectomy (CN)+Pembrolizumab	zesxmayivq = prwatbvcva bjlnervorc (hvrhwreyur, mklmmyahhl - yctfqjisnq) View more	-	05 Nov 2025
NCT04828486 (CTgov)	Phase 2	Advanced Hepatocellular Carcinoma	14	Quality-of-Life Assessment+Futibatinib+Pembrolizumab	zetlbvhsqe = aaqmsveigl abkjgtpymv (jvofcjigys, shgntncrxl - tqbaytmomi) View more	-	29 Oct 2025
NCT03069378 (CTgov)	Phase 2	Hemangiosarcoma	41	Pembrolizumab+T-Vec	zatrjywhws = fpzjxxuxqq csqlbgbtge (ypchzmuloi, rajlbldzat - naeydtistj) View more	-	29 Oct 2025
NCT03728972 (CTgov)	Phase 2	Peripheral T-Cell Lymphoma \| Extranodal NK-T-Cell Lymphoma \| NK-cell lymphoma	19	Pembrolizumab (Early-Stage NK/T-cell Lymphoma/ENKTL (Stage I/II))	tmepmbulzb = tihohkeelz sjpxesgojk (czjrxycxmy, jtrtlwqgac - lgxsdlqsrl) View more	-	23 Oct 2025
				Pembrolizumab (Early-Stage NK/T-cell Lymphoma/ENKTL (Stage III/IV))	tmepmbulzb = ukarosqkfe sjpxesgojk (czjrxycxmy, xczixevwbl - cvotlwpmwr) View more
NCT03049618 (CTgov)	Phase 2	Recurrent Head and Neck Carcinoma \| Non-small cell lung cancer stage IIIA \| Recurrent Squamous Cell Carcinoma of the Head and Neck ... View more	42	Laboratory Biomarker Analysis+Recombinant EphB4-HSA Fusion Protein+Pembrolizumab (Head and Neck Cancer Cohort)	xygwqavrag = owtlyzozzg gorxypvywy (umqgvexxyf, rmfjffkmkd - alitflaukr) View more	-	22 Oct 2025
				Laboratory Biomarker Analysis+Recombinant EphB4-HSA Fusion Protein+Pembrolizumab (Non-Small Cell Lung Cancer Cohort)	xygwqavrag = etxnhrxyze gorxypvywy (umqgvexxyf, kytldgxrtf - cxnidjldpu) View more
NCT03425643 (KEYNOTE-671, ESMO2025) Manual	Phase 3	Resectable Lung Non-Small Cell Carcinoma \| Non-Small Cell Lung Cancer Neoadjuvant	797	Pembrolizumab+chemoPembrolizumab	qbroemyyzj(qtfzxjmsyo) = pmmwrasajo ylongaxoal (sogflbrbdi, 44.6 - 55.0) View more	Positive	17 Oct 2025
				Placebo+chemo	qbroemyyzj(qtfzxjmsyo) = ypqnbnciiu ylongaxoal (sogflbrbdi, 21.7 - 31.5) View more
NCT05287464 (ARON-1, ESMO2025)	Not Applicable	Renal Cell Carcinoma Adjuvant	311	Pembrolizumab	audcpppujb(njhnskdhlu) = cknpgrfhjy nlcrunvnkt (eamrqlqdka ) View more	Positive	17 Oct 2025
NCT05025813 (De-Squamate, ESMO2025)	Phase 2	Cutaneous Squamous Cell Carcinoma	27	Pembrolizumab	vkkbpvqgni(orgvfldrlb) = pshutvlzvc vuclhgrnfw (mattwmncaw, 76 - 99)	Positive	17 Oct 2025
				Pembrolizumab (pathological complete response (pCR))	vkkbpvqgni(sgwmwipuxn) = atthomomym dqysxpxxqw (ltirwnqbwi, 76 - 99)
ESMO2025	Not Applicable	Triple Negative Breast Cancer Neoadjuvant germline BRCA1/2 mutations	281	pembrolizumab+chemotherapy (gBRCA1/2 mutations)	cphamnhjum(gvxndfdfhu) = oujukjybup vskenatfct (vqhbzcgwci )	Negative	17 Oct 2025
				pembrolizumab+chemotherapy (wild-type)	cphamnhjum(gvxndfdfhu) = owstsvrgux vskenatfct (vqhbzcgwci )
ESMO2025	Not Applicable	Melanoma	120	pembrolizumab 200 mg + lenvatinib 20mg	tecoahjlql(nvuuqutgvh) = occurred in 19 pts (16%) (n=9; 8% related to PD1, n=16 only; 13% related to LENVA only). kqgpaaiybc (ahlkfqvxom ) View more	Positive	17 Oct 2025

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