On October 20, 2025 Sairopa, a clinical-stage biotechnology company developing innovative cancer immunotherapies, reported new clinical data on ADU-1604, its differentiated CTLA-4 blocking antibody, at the European Society for Medical Oncology (ESMO) (Free ESMO Whitepaper) Congress 2025, taking place October 17-21, 2025 in Berlin, Germany.

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The company presented a scientific poster showcasing significant clinical advances with ADU-1604 in melanoma patients who had previously failed PD-1 inhibitor therapy (n=27). The poster presentation featured the full results from the SRP-21C101 Phase 1 combined dose escalation and dose expansion clinical trial. Clinical efficacy was observed in 4/27 patients indicative of efficacy similar to other CTLA-4 inhibitors. Importantly, ADU-1604 showed a significantly milder safety profile as compared to existing CTLA-4 inhibitors, as evidenced by the reduced severity of immune-related adverse events.

"We are excited to share the clinical results from ADU-1604 in PD1 relapse/refractory melanoma with the international oncology community at ESMO (Free ESMO Whitepaper) Congress," said Laura Lassouw-Polman, Chief Operating Officer at Sairopa. "ADU-1604’s milder safety profile as compared to other CTLA-4 blocking agents will support its future use as combination agent, with PD-1 blocking agents and/or other agents. We are grateful to all patients, their families and investigators that supported our study."

(Press release, Sairopa, OCT 20, 2025, View Source [SID1234656822])

On October 20, 2025 Replimune Group, Inc. (NASDAQ: REPL), a clinical stage biotechnology company pioneering the development of novel oncolytic immunotherapies, reported that the U.S. Food and Drug Administration (FDA) has accepted the resubmission of the Biologics License Application (BLA) for RP1 in combination with nivolumab for the treatment of advanced melanoma in patients who progress on an anti-PD-1 containing regimen. The PDUFA date set by the FDA is April 10, 2026 based on a Class II resubmission timeline.

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"We are pleased the agency has accepted the resubmission of our BLA for RP1," said Sushil Patel, Ph.D., CEO of Replimune. "RP1 plus nivolumab offers a strong risk benefit profile where there are few options for patients with advanced melanoma, who have progressed on PD-1 based therapy. We look forward to working closely with the agency to expedite this review as much as possible for patients’ benefit."

During the past few months, Replimune has been working to address agency feedback. Additional information, data and analyses were included in the resubmission which will be part of the BLA review. The FDA indicated this resubmission is considered to be a complete response to the complete response letter received in July 2025.

About RP1
RP1 (vusolimogene oderparepvec) is Replimune’s lead product candidate and is based on a proprietary strain of herpes simplex virus engineered and genetically armed with a fusogenic protein (GALV-GP R-) and GM-CSF, intended to maximize tumor killing potency, the immunogenicity of tumor cell death, and the activation of a systemic anti-tumor immune response.

(Press release, Replimune, OCT 20, 2025, View Source [SID1234656821])

On October 20, 2025 Redhill Biopharma, a specialty biopharmaceutical company, reported the signing of a strategic partnership with Cumberland Pharmaceuticals Inc. (Nasdaq: CPIX) ("Cumberland"), a specialty pharmaceuticals company with a strong gastrointestinal market presence, whereby Cumberland will invest $4 million for a 30% ownership stake in RedHill’s global Talicia business. The companies will share in the financial performance and operational support for the Talicia brand with RedHill retaining 70% ownership and joint control. All other aspects of RedHill’s business remain unchanged.

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RedHill and Cumberland have also entered into a U.S. Talicia co-commercialization agreement with an equal sharing of the product’s net revenues. Cumberland commits to significant additional investment to support Talicia’s U.S. business, providing the strength of its national sales force to feature and further enhance the brand’s marketing and promotional activities. The partnership is designed to deliver economies of scale and cost reductions through shared responsibility for Talicia’s U.S. sales, marketing, manufacturing, supply, regulatory and administrative operations.

"This strategic partnership provides an excellent growth opportunity for RedHill and for Cumberland, a highly capable and driven partner with a strong gastroenterology market presence, adding a market-leading approved product to its portfolio. We believe Cumberland can help drive prescriptions and deliver revenue growth, further strengthening Talicia’s U.S. market leadership," said Dror Ben-Asher, RedHill’s CEO. "The transaction highlights the significant standalone value and commercial strength of the Talicia business, and positions RedHill to accelerate growth, reinforce its financial position and reduce costs, while continuing to advance our broader strategic objectives."

"Talicia has an outstanding product profile and represents an excellent strategic fit for Cumberland, providing us with an important growth opportunity," said A.J. Kazimi, Cumberland’s CEO. "These arrangements with RedHill provide us with the only FDA-approved all-in-one, low-dose rifabutin-based therapy to address H. pylori antibiotic resistance in support of patient care. We can build on the excellent foundation RedHill has created for the product, representing a strong growth opportunity for both companies, and we are delighted to be working with them to pursue this potential."

"There is a real problem with H. pylori antibiotic resistance, with eradication treatment failure rates of up to 40% associated with clarithromycin-containing therapies3. Leading U.S. H. pylori treatment guidelines are explicit on the need to avoid using clarithromycin as part of any H. pylori treatment regimen without prior susceptibility testing," said Rick Scruggs, RedHill’s Chief Commercial Officer. "Moreover, H. pylori is a key risk factor for gastric cancer, a cause of approximately 11,000 U.S. deaths4 a year. This is despite it being reported that eradication of H. pylori can lead to a 75% decreased gastric cancer risk.5 The need for effective H. pylori treatment designed to address antibiotic resistance is clear."

The transaction also supports RedHill’s plan to regain compliance with Nasdaq’s minimum stockholders’ equity requirement and maintain its continued listing, supporting access to capital and long-term financial stability. Accordingly, as a result of this transaction, as of the date of this press release, the Company believes it has stockholder’s equity in excess of the $2.5 million requirement for continued listing pursuant to Nasdaq Listing Rule 5550(b)(1). The Company intends to notify Nasdaq of its compliance status so that Nasdaq can make a determination as to whether the Company has regained compliance with all applicable requirements for continued listing on The Nasdaq Capital Market. However, there can be no assurance that Nasdaq will determine that the Company has regained compliance with the Nasdaq continued listing standards.

RedHill is committed to expanding patient access to Talicia globally. This month we announced the licensing of Talicia for new Middle East markets in a deal worth potentially $1.8 million plus sales royalty payments, with efforts to further broaden market access and secure additional non-dilutive ex-U.S. licensing revenue streams ongoing.

Talicia is patent protected through 2042 and received eight years of U.S. market exclusivity under its Qualified Infectious Disease Product (QIDP) designation.

About H. pylori

H. pylori is a bacterial infection that affects approximately 35% of the U.S. adult population6 (an estimated 1.6 million U.S. patients are treated annually) rising to more than 50% globally7. Classified by the World Health Organization (WHO) as a Group 1 carcinogen, H. pylori is the strongest known risk factor for gastric cancer (between 70% to 90% of cases with more than 27,000 Americans diagnosed with gastric cancer annually8 and approximately 800,000 deaths globally per year), a major risk factor for peptic ulcer disease (90% of cases)9 and gastric mucosa-associated lymphoid tissue (MALT) lymphoma10. Eradication of H. pylori is becoming increasingly difficult, with current therapies failing in approximately 25-40% of patients who remain H. pylori-positive due to high resistance of H. pylori to antibiotics, especially clarithromycin, which is still commonly used in standard combination therapies11.

About Talicia

Approved by the FDA for the treatment of H. pylori infection in adults in November 2019, Talicia is a novel, fixed-dose, all-in-one oral capsule combination of two antibiotics (amoxicillin and rifabutin) and a proton pump inhibitor (omeprazole). Talicia received eight years of U.S. market exclusivity under its Qualified Infectious Disease Product (QIDP) designation and is also covered by U.S. patents extending patent protection through 2042 with additional patents and applications pending and granted in various territories worldwide. Talicia is also approved by the United Arab Emirates (UAE) Ministry of Health.

(Press release, RedHill Biopharma, OCT 20, 2025, View Source [SID1234656819])

On October 20, 2025 Merck (NYSE: MRK), known as MSD outside of the United States and Canada, reported new long-term data highlighting the sustained survival benefits of KEYTRUDA (pembrolizumab), Merck’s anti-PD-1 therapy, in treating non-small cell lung cancer (NSCLC). The results are based on the exploratory five-year analyses of KEYNOTE-671 evaluating KEYTRUDA as part of a neoadjuvant followed by adjuvant (perioperative) treatment regimen for patients with resectable NSCLC; and the eight-year analyses of KEYNOTE-024 and -042 and the 10-year analyses of KEYNOTE-001 and -010 evaluating KEYTRUDA as monotherapy in certain patients with locally advanced or metastatic NSCLC.

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"These long-term data mark a milestone for patients and their families and build upon the transformative progress we’ve already made in non-small cell lung cancer," said Dr. Marjorie Green, senior vice president and head of oncology, global clinical development, Merck Research Laboratories. "Across the spectrum of earlier to advanced stages of disease, these results support the long-term survival benefit of KEYTRUDA in certain patients with NSCLC. We look forward to continued advancements and possibilities for KEYTRUDA in cancer treatment."

In the exploratory five-year follow-up data from the Phase 3 KEYNOTE-671 trial, KEYTRUDA in combination with chemotherapy as neoadjuvant treatment, and then continued as a single agent as adjuvant treatment after surgery continued to show clinically meaningful improvements in overall survival (OS) and event-free survival (EFS) outcomes in certain patients with resectable stage II, IIIA or IIIB NSCLC, compared to neoadjuvant placebo plus chemotherapy followed by adjuvant placebo alone. The hazard ratio (HR) for OS for the KEYTRUDA regimen versus the chemotherapy-placebo regimen was 0.74 (95% CI, 0.59-0.92). For EFS, the HR for the KEYTRUDA regimen versus the chemotherapy-placebo regimen was 0.58 (95% CI, 0.48-0.69).

"The five-year benefit demonstrated across overall survival and event-free survival from KEYNOTE-671 supports the continued use of this pembrolizumab-based perioperative regimen as a standard of care for patients with resectable, earlier-stage non-small cell lung cancer," said Dr. Heather Wakelee, principal investigator for KEYNOTE-671, thoracic medical oncologist. "These consistent results are impactful, as they reflect the importance of intervening for certain patients with earlier stages of non-small cell lung cancer." Wakelee is also a professor of medicine at Stanford Medicine.

In the exploratory eight-year analyses from KEYNOTE-024 and KEYNOTE-042 and the exploratory 10-year analyses from KEYNOTE-001 and KEYNOTE-010, KEYTRUDA continued to improve OS in patients with locally advanced or metastatic NSCLC compared to chemotherapy.

In KEYNOTE-001, the median OS for patients receiving KEYTRUDA was 13.2 months (95% CI, 10.5-15.3) in those with any Tumor Proportion Score (TPS) and a median OS of 17.3 months (95% CI,13.7-24.8) in those with a TPS ≥50%. KEYNOTE-001 did not compare KEYTRUDA to another agent or placebo.
In KEYNOTE-010, the median OS for patients receiving KEYTRUDA with a TPS ≥1% was 11.8 months (95% CI, 10.3-13.0) versus 8.3 months (95% CI, 7.5-9.5) for chemotherapy (HR=0.66 [95% CI, 0.58-0.76]). For patients receiving KEYTRUDA, with a TPS ≥50%, the median OS was 16.6 months (95% CI, 12.1-21.2) versus 8.2 months (95% CI, 6.4-9.8) for chemotherapy (HR=0.55 [95% CI, 0.44-0.68]).
In KEYNOTE-024, the median OS for patients receiving KEYTRUDA with a TPS ≥50% was 26.3 months (95% CI,18.3-40.4) versus 13.4 months (95% CI, 9.4-18.3) for chemotherapy (HR=0.65 [95% CI, 0.50-0.83]).
In KEYNOTE-042, the median OS for patients receiving KEYTRUDA with a TPS ≥1% was 16.4 months (95% CI, 14.0-19.6) versus 12.1 months (95% CI, 11.3-13.3) for chemotherapy (HR=0.78 [95% CI, 0.69-0.88]). For patients receiving KEYTRUDA with a TPS ≥50%, the median OS was 20.0 months (95% CI, 15.9-24.2) versus 12.2 months (95% CI, 10.4-14.6) for chemotherapy (HR=0.70 [95% CI, 0.59-0.83]).
Participants from KEYNOTE-001, KEYNOTE-010, KEYNOTE-024 and KEYNOTE-042 who achieved a complete response after taking KEYTRUDA and then had progressive disease were eligible for a subsequent anti-cancer therapy including a second course of KEYTRUDA monotherapy.

Additional details about the study designs and results from KEYNOTE-671, KEYNOTE-001, KEYNOTE-010, KEYNOTE-024 and KEYNOTE-042, including selected results of previously reported primary analyses, are described below.

"Historically, patients with advanced non-small cell lung cancer faced a poor prognosis, with long-term survival considered unlikely," said Edward B. Garon, MD, MS, professor of medicine, principal investigator for KEYNOTE-001, David Geffen School of Medicine, the University of California, Los Angeles. "The long-term results from these four trials show that pembrolizumab has helped change what certain patients with advanced NSCLC can hope to achieve."

To date, KEYTRUDA monotherapy or combination regimens have demonstrated sustained survival benefits of five years or more across multiple types of cancer, including certain types of metastatic NSCLC (KEYNOTE-189, KEYNOTE-407), melanoma (KEYNOTE-006, KEYNOTE-054), advanced head and neck (KEYNOTE-048), bladder (KEYNOTE-045) and endometrial (KEYNOTE-775) cancers.

The late-breaking five-year data from KEYNOTE-671 were presented during a mini oral session at the European Society for Medical Oncology (ESMO) (Free ESMO Whitepaper) Congress 2025 (Presentation #LBA67). The eight-year data from KEYNOTE-024 and KEYNOTE-042 and 10-year data from KEYNOTE-001 and KEYNOTE-010 were presented during a poster session at the ESMO (Free ESMO Whitepaper) Congress 2025 (Presentation #3208P).

Study design and additional five-year data from KEYNOTE-671

KEYNOTE-671 is a multicenter, randomized, double-blind, placebo-controlled Phase 3 trial (ClinicalTrials.gov; NCT03425643) evaluating KEYTRUDA in combination with neoadjuvant chemotherapy, followed by surgery and continued adjuvant treatment with KEYTRUDA as a single agent, versus placebo plus neoadjuvant chemotherapy, followed by resection and adjuvant placebo, in patients with resectable stage II, IIIA or IIIB (T3-4N2) NSCLC (per the eighth edition of the American Joint Committee on Cancer [AJCC] Cancer Staging Manual). The trial’s dual primary endpoints are EFS and OS. Key secondary endpoints include pathologic complete response (pCR) and major pathological response (mPR). The study enrolled 797 patients who were randomly assigned (1:1) to receive either:

KEYTRUDA (200 mg intravenously [IV] every three weeks) plus chemotherapy (cisplatin [75 mg/m2 , IV; given on Day 1 of each cycle] and either gemcitabine [1,000 mg/m2, IV; given on Days 1 and 8 of each cycle] or pemetrexed [500 mg/m2 , IV; given on Day 1 of each cycle]) for up to four cycles as neoadjuvant therapy prior to surgery. Within 4-12 weeks following surgery, KEYTRUDA (200 mg) was administered every three weeks for up to 13 cycles, or;
Placebo (saline IV every three weeks) plus chemotherapy (cisplatin [75 mg/m2 , IV; given on Day 1 of each cycle] and either gemcitabine [1,000 mg/m2, IV; given on Days 1 and 8 of each cycle] or pemetrexed [500 mg/m2, IV; given on Day 1 of each cycle]) for up to four cycles as neoadjuvant therapy prior to surgery. Within 4‑12 weeks following surgery, placebo was administered every three weeks for up to 13 cycles.
After a median follow-up of 60.4 months (range, 42.6-85.8), the five-year OS rate was 64.6% (95% CI, 59.5%-69.2%) for the KEYTRUDA regimen versus 53.6% (95% CI, 48.3%-58.6%) for the chemotherapy-placebo regimen. Median OS was not reached (NR) (95% CI, NR-NR) for patients who received the KEYTRUDA regimen versus 70.7 months (95% CI, 53.7-NR) for patients who received the chemotherapy-placebo regimen.

The five-year EFS rate was 49.9% (95% CI, 44.6%-55.0%) for the KEYTRUDA regimen versus 26.5% (95% CI, 21.7%-31.5%) for the chemotherapy-placebo regimen. Median EFS was 57.1 months (95% CI, 38.0-NR) for patients who received the KEYTRUDA regimen versus 18.4 months (95% CI, 14.8-22.1) for patients who received the chemotherapy-placebo regimen.

At the five-year follow-up analysis, Grade ≥3 treatment-related adverse events (TRAEs) occurred in 45.2% of patients receiving the KEYTRUDA regimen and 37.8% of patients receiving the chemotherapy-placebo regimen. Grade ≥3 immune-mediated adverse events (AEs) and infusion reactions occurred in 6.3% of patients receiving the KEYTRUDA regimen and 1.8% of patients receiving the chemotherapy-placebo regimen.

At the study’s previously reported primary analysis, KEYNOTE-671 showed that treatment with the KEYTRUDA regimen reduced the risk of death by 28% (HR=0.72 [95% CI, 0.56-0.93]; p=0.0103) versus the chemotherapy-placebo regimen. For patients who received the KEYTRUDA regimen, median OS was not reached (95% CI, NR-NR) versus 52.4 months (95% CI, 45.7-NR) for patients who received the chemotherapy-placebo regimen. Additionally, the KEYTRUDA regimen reduced the risk of EFS events by 42% (HR=0.58 [95% CI, 0.46-0.72]; p<0.0001) versus the chemotherapy-placebo regimen. For patients who received the KEYTRUDA regimen, median EFS was not reached (95% CI, 34.1-NR) versus 17.0 months (95% CI, 14.3-22.0) for patients who received the chemotherapy-placebo regimen.

(Press release, Merck & Co, OCT 20, 2025, View Source [SID1234656818])

Long-term follow-up data from exploratory analyses of KEYNOTE-001, KEYNOTE-010, KEYNOTE-024 and KEYNOTE-042

In KEYNOTE-010, KEYNOTE-024 and KEYNOTE-042, KEYTRUDA continued to improve OS compared to chemotherapy. In these studies, data showed KEYTRUDA improved OS compared to chemotherapy in patients whose tumors expressed PD-L1 (TPS ≥50%). Overall survival results from these long-term follow-up analyses showed:

KEYTRUDA

Chemotherapy

KEYNOTE-001a,b,c

Any TPS

n/N = 54/550

N/A

10y OS rate (95% CI), %

11.3% (8.5%-14.5%)

N/A

Median OS (95% CI), months

13.2 (10.5-15.3)

N/A

TPS ≥50%

n/N = 25/165

N/A

10y OS rate

19.3% (13.1%-26.5%)

N/A

Median OS (95% CI), months

17.3 (13.7-24.8)

N/A

KEYNOTE-010b,d

TPS ≥1%

n/N = 53/690

n/N = 9/343

10y OS rate

9.3% (7.0%-12.1%)

1.9% (0.7%-4.6%)

Median OS (95% CI), months

11.8 (10.3-13.0)

8.3 (7.5-9.5)

HR (95% CI)

0.66 (0.58–0.76)

TPS ≥50%

n/N = 35/290

n/N = 6/152

10y OS rate

15.5% (11.1%-20.5%)

2.7% (0.7%-7.4%)

Median OS (95% CI), months

16.6 (12.1-21.2)

8.2 (6.4-9.8)

HR (95% CI)

0.55 (0.44-0.68)

KEYNOTE-024a

TPS ≥50%

n/N = 36/154

n/N = 14/151

8y OS rate

24.3% (17.6%-31.5%)

12.8% (7.6%-19.3%)

Median OS (95% CI), months

26.3 (18.3-40.4)

13.4 (9.4-18.3)

HR (95% CI)

0.65 (0.50-0.83)

KEYNOTE-042a

TPS ≥1%

n/N = 66/637

n/N = 27/637

8y OS rate

12.0% (9.5%-14.8%)

4.7% (3.1%-6.9%)

Median OS (95% CI), months

16.4 (14.0-19.6)

12.1 (11.3-13.3)

HR (95% CI)

0.78 (0.69-0.88)

TPS ≥50%

n/N = 41/299

n/N = 13/300

8y OS rate

16.6% (12.5%-21.1%)

6.8% (4.1%-10.5%)

Median OS (95% CI), months

20.0 (15.9-24.2)

12.2 (10.4-14.6)

HR (95% CI)

0.70 (0.59-0.83)

n/N, number of patients in KEYNOTE-587/number of patients in parent study.

afirst-line therapy

bsecond-line+ therapy

cIn KEYNOTE-001, KEYTRUDA was not compared to any other agent or placebo.

dtwo doses of pembrolizumab treatment were combined for these analyses

Limited additional lung cancer-specific deaths occurred since the previously reported five-year data across all four trials.

At the conclusion of these initial studies, participants were eligible to transition to the KEYNOTE-587 extension study for long-term follow-up. The primary endpoint for KEYNOTE-587 is OS. For patients in KEYNOTE-587, the median time from first treatment in KEYNOTE-001 or randomization in KEYNOTE-010, KEYNOTE-024 and KEYNOTE-042 to data cutoff was 124.6 months (range, 118.5-142.2), 115 months (range, 108.8-124.6), 106.4 months (range, 102.4-114.3) and 99 months (range, 86.6-110.2), respectively.

Study design and additional data from KEYNOTE-001

Ten-year outcomes for KEYTRUDA were measured in the Phase 1b KEYNOTE-001 trial (ClinicalTrials.gov; NCT01295827), which evaluated 550 patients with treatment-naïve or previously treated advanced NSCLC. Patients received 2 mg/kg IV of KEYTRUDA every three weeks or 10 mg/kg IV of KEYTRUDA every two weeks or every three weeks. The primary endpoint was overall response rate (ORR) and secondary endpoints included progression-free survival (PFS) and OS.

At the study’s previously reported primary analysis, KEYNOTE-001 showed that KEYTRUDA demonstrated an ORR of 41% in patients with a TPS ≥50%; all responses were partial responses (95% CI, 29-54). Of the patients who responded, 84% continued to respond to treatment with KEYTRUDA, including 11 patients with ongoing responses of six months or longer.

Study design and additional data from KEYNOTE-010

Ten-year outcomes for KEYTRUDA were measured in the Phase 2/3 KEYNOTE-010 trial (ClinicalTrials.gov; NCT01905657), which evaluated patients with metastatic NSCLC whose tumors expressed PD-L1 (TPS ≥1%) that had progressed after platinum-containing chemotherapy and, if appropriate, targeted therapy for EGFR or ALK genomic tumor aberrations. The trial enrolled 1,033 patients who were randomized (1:1:1) to receive 2 mg/kg IV or 10 mg/kg IV of KEYTRUDA every three weeks or chemotherapy (docetaxel) every three weeks. The primary endpoints for this trial were OS and PFS, and secondary endpoints included ORR and duration of response (DOR).

At the study’s previously reported primary analysis, KEYNOTE-010 showed that 2 mg/kg of KEYTRUDA reduced the risk of death by 29% (HR=0.71 [95% CI, 0.58-0.88]; p<0.001), and 10 mg/kg of KEYTRUDA reduced the risk of death by 39% (HR=0.61 [95% CI, 0.49-0.75]; p<0.001) in patients with a TPS ≥1% versus chemotherapy. Two mg/kg of KEYTRUDA reduced the risk of disease progression or death by 12% (HR=0.88 [95% CI, 0.73-1.04]; p=0.068) and 10 mg/kg of KEYTRUDA reduced the risk of disease progression or death by 21% (HR=0.79 [95% CI, 0.66-0.94]; p=0.005) in patients with a TPS ≥1% versus chemotherapy. Additionally, the analysis showed that 2 mg/kg of KEYTRUDA reduced the risk of death by 46% (HR=0.54 [95% CI, 0.38-0.77]; p<0.001), and 10 mg/kg of KEYTRUDA reduced the risk of death by 50% (HR=0.50 [95% CI, 0.36-0.70]; p<0.001) in patients with a TPS ≥50% versus chemotherapy. Two mg/kg of KEYTRUDA reduced the risk of disease progression or death by 42% (HR=0.58 [95% CI, 0.43-0.77]; p<0.001), and 10 mg/kg of KEYTRUDA reduced the risk of disease progression or death by 41% (HR=0.59 [95% CI, 0.45-0.78]; p<0.001) in patients with a TPS ≥50% versus chemotherapy.

Study design and additional data from KEYNOTE-024

Eight-year outcomes for KEYTRUDA were measured in the Phase 3 KEYNOTE-024 trial (ClinicalTrials.gov; NCT02142738), which evaluated patients with previously untreated metastatic NSCLC whose tumors express high levels of PD-L1 (TPS ≥50%) with no EGFR or ALK genomic tumor aberrations. The trial enrolled 305 patients who were randomized (1:1) to receive 200 mg of KEYTRUDA every three weeks or platinum-based chemotherapy. The primary endpoint for this trial was PFS, and secondary endpoints included OS and ORR. In this study, 10.3% (209) of patients transitioned to KEYNOTE-587.

At the study’s previously reported primary analysis, KEYNOTE-024 showed that KEYTRUDA reduced the risk of disease progression or death by 50% (HR=0.50 [95% CI, 0.37-0.68]; p<0.001) versus chemotherapy. Additionally, KEYTRUDA reduced the risk of death by 40% (HR=0.60 [95% CI, 0.41-0.89]; p=0.005) versus chemotherapy.

Study design and additional data from KEYNOTE-042

Eight-year outcomes for KEYTRUDA were measured in the Phase 3 KEYNOTE-042 trial (ClinicalTrials.gov; NCT02220894), which evaluated patients with stage III NSCLC who were not candidates for surgical resection or definitive chemoradiation, or metastatic NSCLC, and whose tumors expressed PD-L1 (TPS ≥1%) and who had not received prior systemic treatment for metastatic NSCLC. The trial enrolled 1,251 patients who were randomized (1:1) to receive 200 mg of KEYTRUDA every three weeks or platinum-based chemotherapy. The primary endpoint for this trial was OS in patients with a TPS ≥50%, ≥20% or ≥1% and secondary endpoints included PFS and ORR as assessed by blinded independent central review (BICR) according to RECIST v1.1 in patients with a TPS ≥50%, ≥20% or ≥1%. In this study, 4.4% (50) of patients transitioned to KEYNOTE-587.

At the study’s previously reported primary analysis, KEYNOTE-042 showed that KEYTRUDA reduced the risk of death by 31% (HR=0.69 [95% CI, 0.56-0.85]; p=0.0006) in patients with a TPS ≥50% and by 19% (HR=0.81 [95% CI, 0.71-0.93]; p=0.0036) in patients with a TPS ≥1% versus chemotherapy. Median OS was 20.0 months (95% CI, 15.4-24.9) for KEYTRUDA in patients with a TPS ≥50% versus 12.2 months (95% CI, 10.4-14.2) for chemotherapy, and 16.7 months (95% CI, 13.9-19.7) for KEYTRUDA in patients with a TPS ≥1% versus 12.1 months (95% CI, 11.3-13.3) for chemotherapy.

About lung cancer

Lung cancer is the leading cause of cancer death worldwide. In 2022 alone, there were approximately 2.4 million new cases and 1.8 million deaths from lung cancer globally. Non-small cell lung cancer is the most common type of lung cancer, accounting for about 80% of all cases. In 2025, the overall five-year survival rate for patients diagnosed with lung cancer was 27% in the United States. Improved survival rates are due, in part, to earlier detection and screening, reduction in smoking, advances in diagnostic and surgical procedures, as well as the introduction of new therapies. Early detection and screening remain an important unmet need, as 44% of lung cancer cases are not found until they are advanced.

On October 20, 2025 Leap Therapeutics, Inc. (Nasdaq:LPTX), a biotechnology company focused on developing targeted and immuno-oncology therapeutics, reported final results from Part B of the DeFianCe study (NCT05480306), a Phase 2 study of sirexatamab (DKN-01), an anti-DKK1 monoclonal antibody, in combination with bevacizumab and chemotherapy (Sirexatamab Arm) compared to bevacizumab and chemotherapy (Control Arm) in patients with microsatellite stable (MSS) colorectal cancer (CRC) who have received one prior systemic therapy for advanced disease. The final clinical results were presented on behalf of the DeFianCe study investigators by Zev Wainberg, MD, Professor of Medicine and Co-Director of the GI Oncology Program at UCLA in a Mini Oral session at the European Society for Medical Oncology (ESMO) (Free ESMO Whitepaper) Congress 2025 in Berlin, Germany.

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"Circulating DKK1 is a negative prognostic factor and elevated in patients with advanced, metastatic CRC. The data presented at ESMO (Free ESMO Whitepaper) demonstrate that sirexatamab, which binds to and removes free DKK1, has significant potential to provide a survival benefit for CRC patients who have high DKK1 levels and who are likely to have poor outcomes receiving the current standard of care alone," said Dr. Wainberg. "Sirexatamab has the potential to be a valuable addition to the CRC treatment paradigm as a targeted therapeutic for patients with high DKK1 and should move forward to be evaluated in a biomarker-focused registrational trial."

The DeFianCe study was a two part, open-label, multi-country study. Part A of the DeFianCe study enrolled 33 patients, including a significant number of patients who had early progression on first-line therapy, previous exposure to bevacizumab, tumors with RAS mutations, or liver and lung metastases. The study expanded into a 188 patient Part B randomized controlled trial. The primary objective of the study was progression-free survival PFS. Secondary objectives included objective response rate (ORR), duration of response, and overall survival (OS). A key pre-defined exploratory population was those patients who had high levels of circulating DKK1, as measured by a biomarker assay.

Key Part B DeFianCe Study Findings:

· Across the DKK1-high (upper median) patients (n=88):
o ORR was 38.0% in the Sirexatamab Arm compared to 23.7% ORR in the Control Arm.
o mPFS was 9.03 months in the Sirexatamab Arm compared to 7.06 months in the Control Arm, Hazard Ratio (HR) 0.61, p-value = 0.0255.
o mOS was not reached in the Sirexatamab Arm compared to 14.39 months in the Control Arm, HR 0.42, p-value = 0.0118.

· Across the DKK1-high (upper quartile) patients (n=44):
o ORR was 44.0% in the Sirexatamab Arm compared to 15.8% ORR in the Control Arm.
o mPFS was 9.36 months in the Sirexatamab Arm compared to 5.88 months in the Control Arm, HR 0.46, p-value = 0.0168.
o mOS was not reached in the Sirexatamab Arm compared to 9.66 months in the Control Arm, HR 0.17, p-value < 0.001.

· In the full intent-to-treat population (n=188):
o ORR was 35.1% in the Sirexatamab Arm compared to 26.6% ORR in the Control Arm.
o mPFS was 9.2 months in the Sirexatamab Arm compared to 8.3 months in the Control Arm, HR 0.84, p-value = 0.1712.
o Event-free rate favors Sirexatamab Arm beginning at month 9 (53 vs 47%) with further separation at month 12 (34 vs 23%).

· Sirexatamab, in combination with chemotherapy and bevacizumab, was safe and well tolerated
o Overall treatment-emergent adverse effects (TEAE) profile was similar between the Sirextamab and Control Arms, suggesting sirexatamab did not impact the safety profile when combined with the standard of care.

"The DeFianCe study results demonstrate the significant potential of sirexatamab in patients with advanced CRC. Patients with this aggressive cancer, particularly those with high DKK1 levels, have poor overall survival outcomes and few promising second-line or later options," said Douglas E. Onsi, President and Chief Executive Officer of Leap. "Sirexatamab has repeatedly demonstrated its potential as a novel, first-in-class antibody targeting DKK1 that provides deep and durable benefit for patients in desperate need of new therapies. With support from a recently completed financing, Leap plans to engage with regulatory authorities over the registrational path for sirexatamab in CRC and to optimize the DKK1 biomarker diagnostic test that could be used to identify these CRC patients with poor prognosis."

(Press release, Leap Therapeutics, OCT 20, 2025, View Source [SID1234656817])