Request Demo

Last update 10 Sep 2025

Nivolumab

Last update 10 Sep 2025

Overview

R&D Status

Clinical Result

Translational Medicine

Overview

Basic Info

Drug Type

Monoclonal antibody

Synonyms

Nivolumab (Genetical Recombination), Nivolumab (genetical recombination) (JAN), Nivolumab (USAN/INN)

+ [16]

Target

PD-1

Action

inhibitors

Mechanism

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

Therapeutic Areas

NeoplasmsImmune System DiseasesDigestive System Disorders+ [13]

Active Indication

Microsatellite instability-high Rectal CancerPD-L1 positive Non-Small Cell Lung CancerMetastatic hepatocellular carcinoma+ [504]

Inactive Indication

Acidemia, IsovalericAcquired Immunodeficiency SyndromeAcute lymphoblastic leukemia recurrent+ [108]

Originator Organization

Ono Pharmaceutical Co., Ltd.

Bristol Myers Squibb Co.

Active Organization

Bristol Myers Squibb Co.

The University of Texas MD Anderson Cancer Center

National Cancer Institute

+ [28]

Inactive Organization

Nektar Therapeutics

Regeneron Pharmaceuticals, Inc.

Transgene SA

+ [14]

License Organization

Nektar Therapeutics

NeoImmuneTech, Inc.

Vedanta Biosciences, Inc.

+ [22]

Drug Highest PhaseApproved

First Approval Date

Japan (04 Jul 2014),

Esophageal CarcinomaMelanoma

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

Structure/Sequence

Sequence Code 93681H

Source: *****

Sequence Code 93684L

Source: *****

1,902

Clinical Trials associated with Nivolumab

CTRI/2025/02/079994

/ Not yet recruitingPhase 2IIT

Phase 2 study evaluating the addition of immune-sensitizing radiotherapy and biomarker-driven low-dose nivolumab in locally advanced resectable gastroesophageal junction/gastric cancers - NISaRGA

Start Date05 Feb 2026

Sponsor / Collaborator

Tata Memorial Centre

NCT07128680

/ Not yet recruitingPhase 1IIT

A Randomized Study of Nivolumab and Ipilimumab With and Without EXL01 in First-Line Treatment of Metastatic Renal Cell Carcinoma (mRCC)

This phase I trial tests the safety and effectiveness of nivolumab and ipilimumab with and without EXL01 for the treatment of renal cell cancer that has spread from where it first started (primary site) to other places in the body (metastatic). Immunotherapy with monoclonal antibodies, such as nivolumab and ipilimumab, may help the body's immune system attack the tumor, and may interfere with the ability of tumor cells to grow and spread. EXL01 is a live biotherapeutic product containing a strain of bacteria called Faecalibacterium prausnitzii. It may enhance a patient's response to treatment with immune checkpoint inhibitors like nivolumab and ipilimumab by altering the composition of the bacteria in the gut. Adding EXL01 to treatment with nivolumab and ipilimumab may be safe and more effective than giving nivolumab and ipilimumab alone.

Start Date05 Dec 2025

Sponsor / Collaborator

City of Hope National Medical Center

[+1]

NCT07011550

/ RecruitingPhase 2IIT

Phase 2, Single-arm Trial of BMS-986340 in Association With Nivolumab, Trifluridine/Tipiracil and Bevacizumab for Patients Refractory to Standard of Care Treatment and With Microsatellite-stable Colorectal Cancer

To learn if the drug combination of BMS-986340, nivolumab, trifluridine/tipiracil, and bevacizumab can help to control advanced or metastatic MSS-CRC.

Start Date30 Nov 2025

Sponsor / Collaborator

The University of Texas MD Anderson Cancer Center

100 Clinical Results associated with Nivolumab

100 Translational Medicine associated with Nivolumab

100 Patents (Medical) associated with Nivolumab

10,904

Literatures (Medical) associated with Nivolumab

31 Dec 2025·Human Vaccines & Immunotherapeutics

State of the art of adjuvant immunotherapy in urothelial cancer: New developments and upcoming changes

Review

Author: Marchetti, Andrea ; Mollica, Veronica ; Mottaran, Angelo ; Piazza, Pietro ; Rosellini, Matteo ; Danielli, Linda ; Ricci, Costantino ; Schiavina, Riccardo ; Tassinari, Elisa ; Massari, Francesco ; Santoni, Matteo

In recent years, several clinical trials focused on the potential role of immune-checkpoint inhibitors (ICIs) in the adjuvant treatment of muscle-invasive urothelial cancer (UC). Heretofore, only the anti-programmed death protein 1 (anti-PD1) nivolumab received European Medical Agency (EMA) approval for cisplatin-unfit patients. In our work, we deeply analyzed the results of the three pivotal studies in view of the rapidly evolving therapeutic advanced UC's scenario. Furthermore, there are several ongoing research to investigate ICIs and other emerging immune agents in this setting; results are awaited. Additionally, current efforts have been made to assess the role of these agents in earlier disease settings, particularly in high-risk non-muscle-invasive bladder cancer (NMIBC). In our review, we analyzed the potential role of predictive and/or prognostic biomarkers that may improve patient selection and treatment efficacy. To conclude, we highlighted the upcoming changes that could redefine the standard of care for patients with early-stage UC.

31 Dec 2025·OncoImmunology

Final 3-year results from the EVIDENS study, an observational study of nivolumab in non-small cell lung cancer

Article

Author: Debieuvre, Didier ; Asselain, Bernard ; Brellier, Florence ; Auliac, Jean-Bernard ; Khalife, Yaacoub ; Cotté, François-Emery ; Barlesi, Fabrice ; Moro-Sibilot, Denis ; Pérol, Maurice ; Bombaron, Pierre ; Dixmier, Adrien ; Raspaud, Christophe ; Benoit, Nicolas ; Audigier-Valette, Clarisse

EVIDENS was a prospective, non-interventional, longitudinal study conducted in non-small cell lung cancer (NSCLC) patients receiving nivolumab in France. It recruited adults with pathologically confirmed NSCLC who initiated nivolumab between October 2016 and November 2017; the final results are reported here. Primary outcomes included baseline characteristics and 36-month overall survival (OS). Secondary outcomes included progression free survival (PFS), objective response rate (ORR), safety and health-related quality of life (HRQoL; assessed regardless of nivolumab continuation or interruption). Overall, 1423 patients were included in the analysis population (median age 66 years; non-squamous histology 69.1%; stage IV disease 91.5%; brain metastases 19.9%). Almost all patients (99.7%) had received prior chemotherapy, and most patients received nivolumab as second-line (73.5%) or later (26.1%) therapy. The 36-month OS rate was 19.7% (95% confidence interval [CI] 17.5-22.0); OS was significantly shorter in patients with squamous versus non-squamous tumors (9.8 [95% CI 8.6-11.2] months vs 11.8 [95% CI 10.2-13.2] months; p = 0.005). The 36-month PFS rate was 8.8% (95% CI 7.3-10.4). The 12-month investigator-assessed best ORR in the overall population was 20.4%. Eastern Cooperative Oncology Group performance status, smoking status, tumor histology, disease stage and liver metastasis independently predicted survival. Grade 3 and 4 treatment-related adverse events were reported in 8.0% and 0.8% of patients, respectively; eight treatment-related deaths occurred (0.005%). HRQoL was maintained with slight improvement throughout the study, without statistical significance. These results confirm that the real-world effectiveness and safety of nivolumab in these patients is similar to that observed in clinical trials.

31 Dec 2025·OncoImmunology

Peripheral memory B cell population maintenance and long-term survival after perioperative chemoimmunotherapy in NSCLC (NADIM trial)

Article

Author: Gil-González, Ángeles ; Martínez-Toledo, Cristina ; Calvo, Virginia ; Nadal, Ernest ; Dómine, Manuel ; Provencio, Mariano ; Insa, Amelia ; García-Grande, Aránzazu ; García Campelo, Rosario ; de Castro Carpeño, Javier ; Collazo-Lorduy, Ana ; Massuti, Bartomeu ; Huidobro Vence, Gerardo ; Sierra Rodero, Belén ; Megias, Diego ; Martinez-Marti, Alex ; Cruz-Bermúdez, Alberto ; Majem, Margarita ; Molina-Alejandre, Marta ; Lobato, Daniel

Perioperative chemoimmunotherapy has significantly improved survival rates for non-small cell lung cancer (NSCLC). However, current tissue biomarkers remain inadequate, underscoring the need for more sensitive and accessible alternatives to monitor relapse risk. Intratumoral B-cells are increasingly recognized for their role in enhancing immunotherapy outcomes, yet the contribution of peripheral B-cells to immune surveillance remains unexplored. Peripheral B-cell immunophenotypes were analyzed from blood samples (at diagnosis, post-neoadjuvant, and at 6- and 12-months of adjuvant treatment) in 41 stage IIIA NSCLC patients treated with perioperative nivolumab plus chemotherapy, included in the NADIM clinical trial (NCT03081689). Results were correlated with 5-year survival outcomes and validated through unsupervised clustering. An increase in the percentage of total B-cells (CD19⁺CD20⁺) and naïve B-cells (CD19⁺CD20⁺CD24⁺CD38⁺CD27^-CD10^-), along with a reduction in CD20 expression on total B-cells, a decrease in the proportion of memory B-cells (CD19⁺CD20⁺CD24⁺CD38^-/lowCD27⁺) and transitional B-cells (CD19⁺CD20⁺CD24⁺⁺CD38⁺⁺CD10⁺), was observed during the time encompassed between the end of neoadjuvant treatment and the posterior 6 months of adjuvant treatment. Higher levels of CD20 expression on total B-cells, along with an increased percentage of memory B-cells, or activated B-cells (CD19⁺CD20⁺CD25⁺), at 6- and 12-months of adjuvant treatment, were associated with increased survival. Conversely, higher levels of a newly described circulating population of CD19⁺CD20^lowCD25^lowCD27^low B-cells during adjuvant treatment were linked to disease progression. Perioperative nivolumab plus chemotherapy in resectable NSCLC patients induces significant changes in peripheral B-cells. The persistence of circulating memory B-cells during adjuvant treatment might play a crucial role in survival.

1,987

News (Medical) associated with Nivolumab

08 Sep 2025

·www.globenewswire.com

I-Mab Announces Acceleration of Givastomig Investment and Leadership Appointments

Expands investment in givastomig in 1L metastatic gastric cancers, with plans to initiate a global randomized Phase 2 study in combination with immunochemotherapy, in Q1 2026, with additional Phase 1b cohorts to followReiterates expectations to report topline givastomig Phase 1b dose expansion data in Q1 2026Plans to broaden the 1L development strategy into locally advanced gastric cancer as well as other Claudin 18.2-positive tumor types, including biliary tract cancer (BTC) and pancreatic ductal adenocarcinoma (PDAC)Mr. Wei Fu, I-Mab’s Chairman of the Board of Directors, appointed as Executive Chairman, supported by further executive additions ROCKVILLE, Md., Sept. 08, 2025 (GLOBE NEWSWIRE) -- I-Mab (NASDAQ: IMAB) (I-Mab or the Company), a U.S.-based, global biotech company, focused on the development of precision immuno-oncology agents for the treatment of cancer, today announced accelerated investment in its lead program, givastomig, an investigational Claudin 18.2 (CLDN18.2)-directed bispecific antibody (CLDN18.2 x 4-1BB), including plans to initiate a global randomized Phase 2 study and additional Phase 1b cohorts. The Company also reiterated its expectations to report Phase 1b dose expansion data in Q1 2026. In addition, I-Mab announced leadership additions, including the appointment of Mr. Wei Fu as Executive Chairman, and the appointment of Dr. Sean Cao as Chief Business Development Officer (CBO). “2025 has been a year of significant progress for I-Mab. Compelling Phase 1b combination data and positive investigator engagement have accelerated the givastomig program and reinforced our confidence in its potential to be a best-in-class Claudin 18.2-directed therapy for metastatic gastric cancers in the 1L setting,” said Sean Fu, PhD, Chief Executive Officer of I-Mab. “Based on these accomplishments, we are expanding our investment in givastomig, with plans to initiate a randomized Phase 2 study in Q1 2026.” “This is an exciting time for I-Mab, marked by clinical progress and organizational development,” said Mr. Wei Fu, Executive Chairman of I-Mab. “I am very excited to work side-by-side with Sean Fu and the executive team as we embark on the next stage of the Company’s growth. With each step forward, I-Mab maintains an unwavering focus on value creation, supported by a strong cash balance and dedication to advancing our mission to improve the lives of patients globally.” Givastomig Clinical Program Overview: 1L Gastric Cancer (GC) Studies: Phase 1b dose expansion data expected in Q1 2026: Phase 1b dose expansion cohorts evaluating givastomig at two dose levels (8mg/kg and 12mg/kg) in combination with nivolumab and chemotherapy (n=40) as a first-line (1L) treatment for patients with metastatic gastric cancers.Initiation of a global randomized Phase 2 study in 1L metastatic gastric cancers: The Company intends to initiate a randomized Phase 2 study in 1L metastatic gastric cancers evaluating givastomig in combination with nivolumab and chemotherapy versus nivolumab and chemotherapy alone. Progression free survival (PFS) data are expected in 2027.Initiation of a 1L metastatic GC cohort for patients who do not qualify for checkpoint inhibitors or the existing approved CLDN18.2 1L GC therapy (Double-Low): The Company intends to initiate an additional Phase 1b cohort evaluating givastomig in combination with chemotherapy (n=20) as a 1L treatment for patients with metastatic gastric cancers whose tumors express Claudin 18.2 in <75% of cells (CLDN-Low) and CPS scores <1 (PD-L1 Low), known as (Double-Low) patients. This population represents a significant unmet medical need since these patients are not eligible to receive the existing approved CLDN18.2-directed therapy or immunotherapies. The current standard of care is chemotherapy alone in this patient population. Expansion of Givastomig into Gastrointestinal Malignancies Characterized by CLDN18.2 Expression: 1L Pancreatic Ductal Adenocarcinoma (PDAC): The Company intends to initiate an additional Phase 1b cohort in 1L, CLDN18.2-positive PDAC evaluating givastomig in combination with chemotherapy.1L Biliary Tract Cancer (BTC): The Company intends to initiate an additional Phase 1b cohort in 1L, CLDN18.2-positive BTC evaluating givastomig in combination with a checkpoint inhibitor and chemotherapy. Investigator Initiated Trials (IITs) Broaden Evaluation into Other Tumor Types in a Neoadjuvant Setting: Dr. Kohei Shitara, National Cancer Center Hospital East, Japan: A single arm study evaluating givastomig in combination with a checkpoint inhibitor and chemotherapy as a 1L neoadjuvant therapy for locally advanced, CLDN18.2-positive, resectable gastric cancers.Dr. Jeremy Kratz, University of Wisconsin, sponsored by the Department of Veterans Affairs: A single arm study evaluating givastomig in combination with chemotherapy as a 1L neoadjuvant therapy for CLDN18.2-positive, resectable pancreatic cancer. Governance and Leadership Updates: Mr. Wei Fu, the current Chairman of the Board of Directors (the Board) has been appointed to the role of Executive Chairman by the Board. Additionally, the Board has appointed Dr. Sean Cao to the newly created role of Chief Business Development Officer (CBO). Dr. Cao will devote approximately half of his professional time to I-Mab to further support I-Mab’s growth. Dr. Cao joins I-Mab from CBC Group and affiliates, bringing expertise in business development. About Givastomig Givastomig (TJ033721 / ABL111) is a bispecific antibody targeting Claudin 18.2 (CLDN18.2)-positive tumor cells. It conditionally activates T cells through the 4-1BB signaling pathway in the tumor microenvironment where CLDN18.2 is expressed. Givastomig is being developed for first line (1L) metastatic gastric cancers, with further exploratory studies in other CLDN18.2-positive gastrointestinal tumors. In Phase 1 trials, givastomig has shown promising anti-tumor activity attributable to a potential synergistic effect of proximal interaction between CLDN18.2 on tumor cells and 4-1BB on T cells in the tumor microenvironment, while minimizing toxicities commonly seen with other 4-1BB agents. Givastomig is being jointly developed through a global partnership with ABL Bio, in which I-Mab is the lead party and shares worldwide rights, excluding Greater China and South Korea, equally with ABL Bio. About I-Mab I-Mab (NASDAQ: IMAB) is a U.S.-based, global biotech company, focused on the development of precision immuno-oncology agents for the treatment of cancer. The Company’s differentiated pipeline is led by givastomig, a potential best-in-class, bispecific antibody (Claudin 18.2 x 4-1BB) designed to treat Claudin 18.2-positive gastric cancers. Givastomig conditionally activates T cells via the 4-1BB signaling pathway in the tumor microenvironment where Claudin 18.2 is expressed. Givastomig is being developed for first-line metastatic gastric cancers and other Claudin 18.2-positive gastrointestinal tumors. Additionally, I-Mab is collaborating with its partner, ABL Bio, for the development of ragistomig, a bispecific antibody integrating PD-L1 as a tumor engager and 4-1BB as a conditional T cell activator, in solid tumors. For more information, please visit https://www.i-mabbiopharma.com and follow us on LinkedIn. Forward Looking Statements This announcement contains forward-looking statements. These statements are made under the “safe harbor” provisions of the U.S. Private Securities Litigation Reform Act of 1995. These forward-looking statements can be identified by terminology such as “will”, “expects”, “believes”, “designed to”, “anticipates”, “future”, “intends”, “plans”, “potential”, “estimates”, “confident”, and similar terms or the negative thereof. Statements that are not historical facts, including statements about I-Mab’s beliefs and expectations, are forward-looking statements. Forward-looking statements in this press release include, without limitation, statements regarding: the potential benefits of I-Mab’s drug candidates, including givastomig; anticipated clinical milestones and results, including the timing of initiating clinical studies and reporting data from clinical trials; and the expected impact of the new leadership appointments. Forward-looking statements involve inherent risks and uncertainties that may cause actual results to differ materially from those contained in these forward-looking statements, including but not limited to the following: I-Mab’s ability to demonstrate the safety and efficacy of its drug candidates; the clinical results for its drug candidates, which may or may not support further development or New Drug Application/Biologics License Application (NDA/BLA) approval; the content and timing of decisions made by the relevant regulatory authorities regarding regulatory approval of I-Mab’s drug candidates; I-Mab’s ability to achieve commercial success for its drug candidates, if approved; I-Mab’s ability to obtain and maintain protection of intellectual property for its technology and drugs; I-Mab’s reliance on third parties to conduct drug development, manufacturing and other services; I-Mab’s limited operating history and I-Mab’s ability to obtain additional funding for operations and to complete the development and commercialization of its drug candidates; and those risks more fully discussed in the “Risk Factors” section in I-Mab’s annual report on Form 20-F filed with the SEC on April 3, 2025 as well as the discussions of potential risks, uncertainties, and other important factors in I-Mab’s subsequent filings with the SEC. All forward-looking statements are based on information currently available to I-Mab. I-Mab undertakes no obligation to publicly update or revise any forward-looking statements, whether as a result of new information, future events, or otherwise, except as may be required by law. I-Mab Investor & Media Contacts PJ Kelleher LifeSci Advisors +1-617-430-7579 pkelleher@lifesciadvisors.com IR@imabbio.com

Phase 1Phase 2Executive ChangeImmunotherapy

08 Sep 2025

·www.biospace.com

5 Companies Caught On a Carousel of FDA Confusion

iStock, mpalis Amid an unprecedented turnover in leadership at the FDA and mass layoffs of staff, communication has crumbled and uncertainty runs rampant, leaving small and medium biopharma companies without a clear path forward for their therapies. Change is hard—especially when a new administration comes in gung-ho to overhaul the entire system. For Health Secretary Robert F. Kennedy Jr., this has meant slashing some 10,000 jobs at the Department of Health and Human Services and overseeing an extensive turnover of leadership at the highest levels . At the FDA, Commissioner Marty Makary has announced plans to speed drug reviews through avenues such as the Commissioner’s National Priority Voucher , expedite rare disease therapies through a yet-to-be-defined conditional approval pathway and ban pharmaceutical representatives from some advisory committees. With all this upheaval, many biopharma companies have gotten caught up in the confusion. Ironically, many of them are seeking approval for rare disease therapies. Capricor Therapeutics, Ultragenyx and Replimune have expressed surprise at recent rejections in Duchenne muscular dystrophy (DMD) cardiomyopathy , Sanfilippo syndrome type A and melanoma , respectively. Meanwhile, three deaths stemming from Sarepta’s gene therapy platform—two of which were associated with its DMD therapy Elevidys—prompted the FDA to request the company halt all shipments of the approved therapy. Amidst these developments, Center for Biologics Evaluation and Research Director Vinay Prasad suddenly left his role , only to return less than two weeks later. With rumors swirling of his direct involvement in some regulatory decisions, his temporary ouster only adds to the uncertainty some biotechs are facing. “These companies who don’t have a lot of cash at hand, they’re actually looking to create these treatments for rare diseases,” Rahul Gupta, president of AI/ML company GATC Health, who served as head of the White House Office of National Drug Control Policy under former President Joe Biden, told BioSpace . “They need a very clear framework, a blueprint of what’s acceptable, what’s not acceptable, and how things will go so they’re not feeling like they’re gambling with their limited amount of funds every time they go up to the FDA.” Here, BioSpace unpacks the journeys of five biotechs that have tangled with the new FDA over the past six months. Sarepta’s Summer Saga Like it or not, the biopharma story of the summer belongs to Sarepta Therapeutics. The Massachusetts-based biotech had a difficult spring, with two nonambulatory teenage patients taking Elevidys succumbing to acute liver injury. It appeared that Sarepta was managing the risks, adding a black box warning to Elevidys’ label for acute liver injury and acute liver failure. But after the death of a third patient —a 51-year-old nonambultory man who had been participating in a Phase I study of Sarepta’s SRP-9004 for limb-girdle muscular dystrophy (LGMD), which used the same underlying technology as Elevidys—the FDA acted, requesting that Sarepta stop all shipments of the gene therapy in the U.S. and pause all LGMD clinical trials. The agency also revoked the platform designation the biotech had previously been granted for its viral vector technology. Initially, Sarepta stood its ground, refusing the FDA’s request. Notably, in its July 18 statement, the company said, “We first heard of this potential request earlier in the day at the same time the public and our patient communities did, through media reports.” The company noted in the same press release that it had alerted the FDA to the death on July 3. The agency later confirmed this to be true but told STAT News that the report had been lost in the bureaucracy and that it had, in fact, only learned of the death with the rest of the world when BioCentury reported it . The FDA further stated it had always planned to take action if a third death occurred. Sarepta ultimately relented to the FDA’s request to halt Elevidys shipments, setting off a week of action for patient groups eager to regain access to the treatment. That action apparently worked. On July 28, the FDA did a 180 and recommended that the voluntary hold on Elevidys be lifted for ambulatory patients. The following day, Prasad was out as CBER director —a development multiple sources suggested was connected to the Sarepta saga. The “unprecedented” FDA leaks were “missteps” on the part of CBER that sowed confusion for both Sarepta and patients, BMO Capital Markets’ Kostas Biliouris wrote to investors on July 30. Capricor Communication Kerfluffle Capricor has also reportedly been caught on the carousel of FDA change. The rejection of the company’s cell therapy deramiocel in July “was unexpected given the trajectory of positive [FDA] interactions,” CEO Linda Marbán said during the company’s second-quarter earnings call on Aug. 11. Drama reportedly predated the rejection, however. Nicole Verdun, the former director of the FDA’s Office of Therapeutic Products, and her deputy, Rachael Anatol, were allegedly “put on administrative leave because of an argument about our file, and that Prasad wanted to [reject] us and Nicole was fighting it,” Marbán told BioSpace in an earlier interview, attributing the information to a STAT reporter who’d contacted her after receiving a tip from an agency insider. After Prasad stepped aside from his role on July 29, Marbán expressed optimism about the company’s chances of fighting the rejection. Speaking again with BioSpace after his return less than 10 days later, she said: “My initial reaction was of great surprise. It was pretty clear that he was asked to leave . . . but I think what it showed is that Makary has tremendous faith in him. We all understand the ramifications of that, that there’s not a lot of ladders you can go up besides the Prasad ladder.” Nevertheless, Capricor is full speed ahead with its resubmission plans for deramiocel. The biotech met with the FDA on Aug. 13 for a type A meeting to discuss a path forward, but Marbán said she would appreciate an audience with Prasad, who did not attend the meeting. “We’ve never had any direct communication from or with him. We would like that very much, but nothing so far.” Ultragenyx’s Unread Responses Also on July 11, the FDA declined to approve Ultragenyx’s investigational in vivo gene therapy UX111, which the biotech is proposing for Sanfilippo syndrome type A—an ultrarare disease that leads to neurological symptoms including language and developmental delays and progressive intellectual disability. On the July 17 edition of STAT News ’ podcast, The Readout Loud , Ultragenyx CEO Emil Kakkis said that a number of issues were raised during the CMC inspection process, which the company was in the process of addressing. Ultragenyx had sent the FDA “a number of very large responses,” Kakkis said. However, at the time of the complete response letter (CRL), “they hadn’t actually read or completed review of the last four responses we had given them. They issued the CRL before they had fully reviewed those responses.” Ultragenyx “believes that these [CMC] observations are readily addressable and many have already been addressed,” Kakkis said in a prepared statement on July 11. Ultragenyx plans to resubmit an approval application and anticipates another six-month review period for UX111. Replimune’s Surprise Rejection In contrast to the other three companies on this list, Replimune can apparently thank a legacy FDA leader for the rejection of its candidate. According to reporting by multiple news outlets, Richard Pazdur , director of the FDA’s Oncology Center of Excellence (OCE) and acting director of the Office of Oncologic Diseases, directly intervened to issue the CRL for Replimune’s advanced melanoma drug, RP1. Pazdur has been the agency’s chief cancer strategist for more than 25 years . An unnamed FDA official told STAT News on Aug. 4 that CBER “mishandled the RP1 review from the beginning,” compelling Pazdur and his team to get involved. The situation was exacerbated, the individual added, by the leadership upheaval within CBER. In Replimune’s announcement of the CRL, CEO Sushil Patel expressed surprise with the decision. “The issues highlighted in the CRL were not raised by the agency during the mid- and late-cycle reviews,” he said in a prepared statement. “Additionally, we had also aligned on the design of the confirmatory study. We strongly believe that RP1 in combination with nivolumab [Bristol Myers Squibb’s Opdivo] can bring substantial benefit to advanced melanoma patients.” On Aug. 5, 22 experts who designed and ran RP1’s Phase III trial issued an open letter responding to several issues outlined in the CRL and urging the FDA to “re-review” Replimune’s application. This decision has had further reverberations as well. Late last month, Krystal Biotech discontinued a Phase I/II study of its investigational intratumoral therapy KB707, which it is developing for solid tumors. Speaking with STAT, Stéphane Paquette, Krystal’s vice president for corporate development, said “heightened uncertainty regarding potential accelerated approval pathways” for KB707 following the FDA’s rejection of RP1 contributed to the biotech’s decision. Novavax’s Delay When the FDA missed its deadline to issue a decision regarding the 2024–2025 formulation of Novavax’s COVID-19 vaccine on April 1, concern circulated about what it could mean for the broader vaccines space. While the Maryland-based company did ultimately secure a narrow nod for Nuvaxovid, the approval process represented a potential “harbinger” of a threat to the FDA’s integrity, former FDA associate commissioner Peter Lurie told BioSpace in June. On April 2, Politico reported that deputy FDA commissioner Sara Brenner directly intervened in the review of Novavax’s vaccine application. A few days later, Kennedy said the delay reflected HHS’ “shifting [its] priorities to multiple-antigen vaccines,” causing the company’s shares to drop by 24%. The influence of both Brenner and Kennedy is a significant deviation from normal protocols, Lurie and three other former government officials wrote in an op-ed published in the Journal of the American Medical Association in June. On May 16, the FDA approved Nuvaxovid for all seniors aged 65 years and older and people 12 through 64 years of age at high risk for severe outcomes from COVID-19. Similar restrictions have now also been applied to the three other vaccines marketed in the U.S.—Pfizer and BioNTech’s Comirnaty and Moderna’s Spikevax and mNEXSPIKE—in line with the FDA’s new risk-based approach to COVID-19 vaccination introduced in May.

Phase 3VaccinePhase 1

08 Sep 2025

·www.biopharmadive.com

New Summit data clouds approval pathway in lung cancer

Combining Summit Therapeutics and Akesos closely watched cancer drug with chemotherapy didnt help people with lung cancer live longer than chemo alone in a late-stage study, raising doubts whether the Food and Drug Administration will agree to review it for potential approval.The final analysis of the Harmoni trial, released Sunday at the World Conference on Lung Cancer in Spain, was the first data from a global Phase 3 study for ivonescimab or any drug in its class, which block both the immune pathway PD-1 and the blood vessel-building protein VEGF.Drugmakers have invested heavily in the PD-1-VEGF class, looking to build on the success of PD-1-blocking drugs like Keytruda and Opdivo. More than a dozen are in development, with Merck & Co. and BioNTech notably among the big-name drugmakers that have bought into the field.The Harmoni data will likely make many take a closer look, however. Summit teased the possibility of a positive outcome in May, when results from the trial, which tested the ivonescimab-chemo combination in people with an EGFR mutation and PD-1 expression who already progressed on a VEGF inhibitor, showed the combination reduced the risk of death or progression by 48% compared with chemo plus placebo.At that point, the trial was unable to prove the combination extended survival, as the reported 21% relative reduction in the risk of death failed to achieve statistical significance. Summit said it wanted to do a final analysis with longer follow-up from people from Western countries enrolled in the trial. Without a statistically significant overall survival benefit, the FDA wouldnt approve the drug, the company said at the time.The data released Sunday didnt help its case. The analysis showed that trial participants from North America and the EU, when assessed, together, had only a 16% relative reduction in the risk of death. People enrolled in North America, when analyzed separately from Europe, had a 30% relative risk reduction.Summit executives acknowledged the timing of the survival readouts and their conflicting findings might cast doubt on ivonescimabs effectiveness. [We] knew this was going to be a problem, said Jack West, Summits vice president of clinical development, in a call with Wall Street analysts.However, he said critics should also listen to physicians who have seen the drugs benefits.Some of the conversations I've had just in the last few hours are with people who have actually used ivonescimab, who are extremely committed to it, who have participated in this trial, he said. They've seen what they've come to conclude are really good results as well. And so there's nothing like that clinical experience.Summit shares fell 24% in morning trading.Leerink Partners analyst Daina Graybosch wrote in a note to clients that following the data she believes the FDA wont approve ivonescimab nor will Summit be able to achieve a licensing deal at the substantial valuation expected by investors.Evercore ISI analyst Cory Kasimov, meanwhile, wrote its possible Summit executives could re-open negotiations with the FDA and file on this data. However, its probably better for the company to wait until it has data from trials in a first-line setting, according to his note. '

Phase 3Clinical Result

100 Deals associated with Nivolumab

External Link

KEGG	Wiki	ATC	Drug Bank
D10316	Nivolumab	L01XC17	DB09035

R&D Status

Approved

10 top approved records.

to view more data

Indication	Country/Location	Organization	Date
Microsatellite instability-high Rectal Cancer	Japan	Ono Pharmaceutical Co., Ltd.	25 Aug 2025
PD-L1 positive Non-Small Cell Lung Cancer	China	Bristol-Myers Squibb Pharma EEIG	22 Jul 2025
Metastatic hepatocellular carcinoma	Australia	Bristol-Myers Squibb Australia Pty Ltd.	26 Jun 2025
Malignant neoplasm of gastro-oesophageal junction	European Union	Bristol-Myers Squibb Pharma EEIG	17 Mar 2025
Malignant neoplasm of gastro-oesophageal junction	Iceland	Bristol-Myers Squibb Pharma EEIG	17 Mar 2025
Malignant neoplasm of gastro-oesophageal junction	Liechtenstein	Bristol-Myers Squibb Pharma EEIG	17 Mar 2025
Malignant neoplasm of gastro-oesophageal junction	Norway	Bristol-Myers Squibb Pharma EEIG	17 Mar 2025
Advanced Hepatocellular Carcinoma	European Union	Bristol Myers Squibb Co.	08 Mar 2025
Advanced Hepatocellular Carcinoma	Iceland	Bristol Myers Squibb Co.	08 Mar 2025
Advanced Hepatocellular Carcinoma	Liechtenstein	Bristol Myers Squibb Co.	08 Mar 2025
Advanced Hepatocellular Carcinoma	Norway	Bristol Myers Squibb Co.	08 Mar 2025
Unresectable Hepatocellular Carcinoma	European Union	Bristol Myers Squibb Co.	08 Mar 2025
Unresectable Hepatocellular Carcinoma	Iceland	Bristol Myers Squibb Co.	08 Mar 2025
Unresectable Hepatocellular Carcinoma	Liechtenstein	Bristol Myers Squibb Co.	08 Mar 2025
Unresectable Hepatocellular Carcinoma	Norway	Bristol Myers Squibb Co.	08 Mar 2025
Carcinoma	Japan	Ono Pharmaceutical Co., Ltd.	09 Feb 2024
Mesothelioma, Malignant	Japan	Ono Pharmaceutical Co., Ltd.	24 Nov 2023
Resectable Lung Non-Small Cell Carcinoma	European Union	Bristol-Myers Squibb Pharma EEIG	14 Jul 2023
Resectable Lung Non-Small Cell Carcinoma	Iceland	Bristol-Myers Squibb Pharma EEIG	14 Jul 2023
Resectable Lung Non-Small Cell Carcinoma	Liechtenstein	Bristol-Myers Squibb Pharma EEIG	14 Jul 2023

Developing

10 top R&D records.

to view more data

Indication	Highest Phase	Country/Location	Organization	Date
Mismatch repair-deficient Colonic Cancer	NDA/BLA	China	Bristol-Myers Squibb (China) Investment Co. Ltd.	18 Apr 2024
Mismatch repair-deficient Rectal Cancer	NDA/BLA	China	Bristol-Myers Squibb (China) Investment Co. Ltd.	18 Apr 2024
Advanced Gastric Adenocarcinoma	Phase 3	United States	National Cancer Institute	24 Jun 2024
Advanced Gastroesophageal Junction Adenocarcinoma	Phase 3	United States	National Cancer Institute	24 Jun 2024
Metastatic gastric adenocarcinoma	Phase 3	United States	National Cancer Institute	24 Jun 2024
stomach adenocarcinoma	Phase 3	United States	National Cancer Institute	24 Jun 2024
Mediastinal large B-cell lymphoma	Phase 3	United States	National Cancer Institute	05 Oct 2021
Mediastinal large B-cell lymphoma	Phase 3	Australia	National Cancer Institute	05 Oct 2021
Mediastinal large B-cell lymphoma	Phase 3	Canada	National Cancer Institute	05 Oct 2021
Refractory Cancer	Phase 3	United States	Bayer AG	01 Jun 2021

Clinical Result

Indication

Phase

Evaluation

View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT03838159 (NADIM II, WCLC2025)	Phase 2	Non-small cell lung cancer stage IIIB Neoadjuvant	86	Nivolumab in combination with platinum-based chemotherapy	orpyuhxjvq(tqsopmgcpw) = wpriggprbp cyxtiivgnx (npfukgbwoy ) View more	Positive	09 Sep 2025
				Platinum-based chemotherapy	orpyuhxjvq(tqsopmgcpw) = pzigasnwhl cyxtiivgnx (npfukgbwoy ) View more
NCT04205552 (NADIM 2, WCLC2025)	Phase 3	Non-Small Cell Lung Cancer Neoadjuvant	86	Nivolumab plus chemotherapy	zfapxodxgi(pfqyhnvitr) = nhldkggngv pfmdjiysxu (sgorhedvhx )	Positive	09 Sep 2025
				Chemotherapy alone	zfapxodxgi(pfqyhnvitr) = mvfumwzsxq pfmdjiysxu (sgorhedvhx )
NCT03918252 (WCLC2025)	Phase 2	Malignant Pleural Mesothelioma Neoadjuvant	30	Neoadjuvant Nivolumab	lzgucbxfyr(myhfrbdmfv) = issubmmdkr hzajnnrdxa (qxoaqtwuaj, 47.8 - 83.4) View more	Positive	09 Sep 2025
				Neoadjuvant Nivolumab + Ipilimumab	lzgucbxfyr(myhfrbdmfv) = kxfdgjwkbj hzajnnrdxa (qxoaqtwuaj, 56.0 - 90.3) View more
NADIM II (WCLC2025)	Phase 2	Non-Small Cell Lung Cancer Neoadjuvant	86	Nivolumab + platinum-based chemotherapy	icoqhezsur(evqbnpwpik): HR = 0.28 (95.0% CI, 0.092 - 0.83) View more	Positive	09 Sep 2025
				platinum-based chemotherapy
NCT03918252 (WCLC2025)	Phase 2	Mesothelioma Neoadjuvant	30	Nivolumab	dqpssylmus(iyltgwrkhd) = gyfgaungbh dcuhryouit (myocfrwkhz, 47.8 - 83.4) View more	Positive	08 Sep 2025
				ipilimumab+Nivolumab	dqpssylmus(iyltgwrkhd) = hhcvpxazhh dcuhryouit (myocfrwkhz, 56.0 - 90.3) View more
NCT01928576 (NA_00084192, WCLC2025)	Phase 2	Advanced Lung Non-Small Cell Carcinoma Second line	40	Azacitidine+Entinostat+Nivolumab (ICB-naïve patients)	jxhunyugur(hocbxnhvje) = khqsttuydh mosfsguyne (vdhnbegvma, 5 - 51) View more	Positive	07 Sep 2025
				Azacitidine+Entinostat+Nivolumab (ICB-refractory disease patients)	jxhunyugur(hocbxnhvje) = wxmzpdxork mosfsguyne (vdhnbegvma, 0 - 58) View more
NCT04695977 (CTgov)	Phase 2/3	Melanoma \| Metastatic melanoma \| Unresectable Melanoma	20	Nivolumab (Nivolumab Monotherapy)	mjaujafntr = eredengmvw engjdsvkmj (xrgozvzbbj, qrllupbdjd - fxsuibzuut) View more	-	05 Sep 2025
				CMP-001+Nivolumab (CMP-001 and Nivolumab)	mjaujafntr = fygajiypfi engjdsvkmj (xrgozvzbbj, cwkvsywccs - xlcnvrcffu) View more
NCT02998528 (CheckMate 816, Pubmed \| N Engl J Med) Manual	Phase 3	Resectable Lung Non-Small Cell Carcinoma Neoadjuvant	358	Nivolumab plus Chemotherapy	txclmllvvw(qihyivyqon) = jskvzexjxn nuptqhawsn (kutgbrrydi ) View more	Positive	21 Aug 2025
				Chemotherapy alone	txclmllvvw(qihyivyqon) = gynoprswep nuptqhawsn (kutgbrrydi )
NCT03739619 (CTgov)	Phase 1/2	Relapsing classical Hodgkin lymphoma \| Refractory Hodgkin Lymphoma \| Classical Hodgkin's Lymphoma ... View more	3	Nivolumab+bendamustine+Gemcitabine	vmbeqlxsxz = rzznfqyovw joqrjxgvzx (zlxwmbjehf, himwjkifqs - ypzqcyavzl) View more	-	06 Aug 2025
NCT03697564 (CTgov)	Phase 2	Pancreatic adenocarcinoma \| Pancreatic Cancer	2	Cabiralizumab+Nivolumab 10 MG/ML Intravenous Solution [OPDIVO]+Gemcitabine	ledxetyzfl = ugcjqzefxb faebfhcoba (qpctjygsah, xtpzelxcju - mflhsajnac) View more	-	06 Aug 2025

Translational Medicine

Boost your research with our translational medicine data.

view full example data

Deal

Boost your decision using our deal data.

view full example data

Core Patent

Boost your research with our Core Patent data.

view full example data

Clinical Trial

Identify the latest clinical trials across global registries.

view full example data

Approval

Accelerate your research with the latest regulatory approval information.

view full example data

Biosimilar

Competitive landscape of biosimilars in different countries/locations. Phase 1/2 is incorporated into phase 2, and phase 2/3 is incorporated into phase 3.

view full example data

Regulation

Understand key drug designations in just a few clicks with Synapse.

view full example data

AI Agents Built for Biopharma Breakthroughs

Accelerate discovery. Empower decisions. Transform outcomes.

Get started for free today!

Accelerate Strategic R&D decision making with Synapse, PatSnap’s AI-powered Connected Innovation Intelligence Platform Built for Life Sciences Professionals.

Start your data trial now!

Synapse data is also accessible to external entities via APIs or data packages. Empower better decisions with the latest in pharmaceutical intelligence.

Bio

Bio Sequences Search & Analysis

Chemical

Chemical Structures Search & Analysis