RecruitingInterventionalPhase 1/Phase 2

A Phase 1/2, Open-label Study of Oral S241656 (BDTX-4933) as Monotherapy and in Combination With Other Anti-Cancer Therapies in Patients With KRAS, BRAF and Other Selected RAS/MAPK Mutation-Positive Malignancies

NCT ID: NCT05786924Sponsor: Institut de Recherches Internationales ServierLast updated: 2026-06-17

Summary

BDTX-4933-101 is a first-in-human, open-label, Phase 1/2 dose escalation, dose optimization and expansion study designed to evaluate the safety and tolerability of S241656 as monotherapy and in combination with other anti-cancer therapies in participants with selected advanced malignancies. The study population for the Dose Escalation part of the study comprises adults with recurrent advanced/metastatic non-small cell lung cancer (NSCLC), Gastrointestinal (GI) cancers, and other solid tumors harboring KRAS, HRAS, NRAS, BRAF, and/or CRAF (Rapidly Accelerated Fibrosarcoma (RAF1)) mutations or alterations. A dose optimization part in adults with NSCLC may follow the dose escalation phase if the sponsor, in consultation with the safety review committee, decides it is necessary to further characterize the optimal dose. However, the study may also proceed directly to the expansion phase. The study population for the Dose Expansion part of the study comprises adults with advanced/metastatic NSCLC with KRAS and/or BRAF mutations, and with Pancreatic Ductal AdenoCarcinoma (PDAC), ColoRectal Cancer (CRC), and Biliary Tract Cancer (BTC) with KRAS, HRAS, NRAS, BRAF, and/or CRAF (RAF1) mutations and alterations. All patients will self-administer S241656 orally in 28-day cycles until disease progression, toxicity, withdrawal of consent, or termination of the study.

Arms & interventions

DrugS241656
RAF inhibitor targeting all classes of oncogenic BRAF alterations (Classes I, II, and III) and constitutively active CRAF, KRAS or NRAS mutations
DrugFOLFOX6/FOLFOX7
Used as a combination therapy and administered intravenously
DrugFOLFIRI
Used as a combination therapy and administered intravenously
DrugCetuximab
Used as a combination therapy and administered intravenously
DrugPanitumumab
Used as a combination therapy and administered intravenously
DrugGemcitabine
Used as a combination therapy and administered intravenously
DrugNab-paclitaxel
Used as a combination therapy and administered intravenously

Outcome measures

Primary

Dose Escalation: Incidence of dose-limiting toxicities (DLTs)
A DLT is defined as any event meeting the DLT criteria occurring within the first 28-day cycle
Time frame: The first 28-day cycle (Cycle 1)
Dose Escalation: Number of Adverse Events (AEs) and Serious Adverse Events (SAEs)
Time frame: Through study completion, approximately 5 years
Dose Optimization/Expansion: Objective response (OR)
Time frame: Through study completion, approximately 5 years

Secondary

Dose Escalation/Expansion: Incidence and severity of treatment-emergent adverse events (TEAEs)
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Maximum plasma concentration (Cmax) of S241656 and its metabolite S243796
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Time of maximum plasma concentration (Tmax) of S241656 and its metabolite S243796
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Area under the plasma drug concentration-time curve (AUC) of S241656 and its metabolite S243796
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Half-life (t1/2) of S241656 and its metabolite S243796
Time frame: Through study completion, approximately 5 years
Dose Escalation: Objective response (OR)
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Disease Control (DC)
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Clinical Benefit (CB)
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Duration of response (DOR)
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Time to response (TTR)
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Progression-free Survival (PFS)
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Overall survival (OS)
Time frame: Through study completion, approximately 5 years
Dose Optimization/Expansion: Number of Adverse Events (AEs) and Serious Adverse Events (SAEs)
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Number of Dose Interruptions
Time frame: Through study completion, approximately 5 years
Dose Escalation/Optimization/Expansion: Number of Dose Reductions
Time frame: Through study completion, approximately 5 years
Dose Escalation: Number of Dose Discontinuations
Time frame: Through study completion, approximately 5 years
Dose Optimization/Expansion: Changes in allelic fraction of DNA sequence variants detected in ctDNA from baseline to on-treatment time points
Time frame: Through study completion, approximately 5 years

Eligibility criteria

Sex: AllAge: 18 Years and olderHealthy volunteers: No

Key Inclusion Criteria: * Life expectancy of ≥ 12 weeks in the opinion of the investigator. * Histologically or cytologically confirmed recurrent locally advanced (unresectable) or metastatic solid tumors with documented RAS or RAF mutations or alterations. * Adequate bone marrow and organ function. * Recovered from toxicity to prior anti-cancer therapy. Part 1 Dose Escalation cohort ONLY: * Part 1A: Advanced/metastatic NSCLC with KRAS non-G12C, HRAS, NRAS, BRAF or CRAF (RAF1) mutations or alterations * Part 1B: Advanced/metastatic GI tumors (e.g., PDAC, CRC, and BTC) with KRAS, HRAS, NRAS, BRAF, and/or CRAF (RAF1) mutations or alterations * Part 1C: Advanced/metastatic PDAC with KRAS, HRAS, NRAS, BRAF, and/or CRAF (RAF1) mutations or alterations * Part 1D: Colorectal adenocarcinoma with KRAS, HRAS, NRAS, BRAF, and/or CRAF (RAF1) mutations or alterations * Part 1E: Other advanced/metastatic non-GI, non-NSCLC solid tumors with KRAS, HRAS, NRAS, BRAF, CRAF (RAF1) mutations or alterations Part 2 Dose Optimization and Expansion cohorts ONLY: * Part 2A: Advanced/metastatic NSCLC with KRAS non-G12C mutations and/or BRAF mutations * Part 2A1: Advanced/metastatic NSCLC with KRAS non-G12C mutations * Part 2A2: Advanced/metastatic NSCLC with BRAF mutations * Part 2A3: Advanced/metastatic NSCLC with KRAS non-G12C or BRAF mutations or alterations and active CNS metastatic disease * Part 2A4: Advanced/metastatic NSCLC with a KRAS G12C mutation * Part 2B1: Advanced/metastatic PDAC with KRAS, HRAS, NRAS, BRAF, and/or CRAF (RAF1) mutations or alterations * Part 2B2: Advanced/metastatic CRC with KRAS, HRAS, NRAS, BRAF, and/or CRAF (RAF1) mutations or alterations * Part 2B3: Advanced/metastatic BTC (adenocarcinoma) with KRAS, HRAS, NRAS, BRAF, and/or CRAF (RAF1) mutations or alterations Key Exclusion Criteria: * Cancer that has a known MEK1/2 mutation. * Known allergy/hypersensitivity to excipients of S241656 or to any of the registered IMPs administered in combination. * Any contra-indication, to use of any of the combination chemotherapy or anti-EGFR therapy partners administered as part of this trial. * Major surgery within 4 weeks of study entry or planned during study. * Ongoing anticancer therapy. * Ongoing radiation therapy. * Uncontrolled or active clinically relevant bacterial, fungal, or specific viral infection requiring systemic therapy. * Clinically significant cardiovascular disease. * Symptomatic spinal cord compression. * Evidence of active malignancy (other than study-specific malignancies) requiring systemic therapy within the next 2 years. * History or current evidence of retinal vein occlusion (RVO) or current risk factors for RVO. * Females who are pregnant or breastfeeding. * Actively receiving systemic treatment or direct medical intervention on another therapeutic clinical study. * Prior use of experimental agents that target the KRAS/BRAF/MEK/ERK pathway.

View on ClinicalTrials.gov

Conditions

Non-small Cell Lung CancerHistiocytic NeoplasmHistiocytosisBRAF Gene MutationBRAF V600EBRAF V600 MutationBRAF Mutation-Related TumorsBRAFMetastatic Lung Non-Small Cell CarcinomaMetastatic Lung CancerRecurrent Lung CancerRecurrent Lung Non-Small Cell CarcinomaNSCLCSolid TumorSolid CarcinomaKRAS G12DKRAS G12VKRAS Mutation-Related TumorsNRAS Gene MutationThyroid CancerThyroid CarcinomaColorectal CancerColorectal CarcinomaRecurrent Histiocytic and Dendritic Cell NeoplasmBrain MetastasesRecurrent NSCLCKRAS G13CAcquired Resistance to KRAS G12C InhibitorKRAS G12AKRAS G12FKRAS G12RKRAS G13D

Study details

Enrollment: 554 participants

Start date: 2023-04-18

Est. completion: 2028-06

Central contacts

Institut de Recherches Internationales Servier (I.R.I.S.), Clinical Studies Department · Contact

+33 1 55 72 60 00 scientificinformation@servier.com

Keywords

BRAF Class IBRAF Class IIBRAF Class IIIKRASIntolerant histiocytic neoplasmBDTX-4933Phase 1dose escalationdose expansionMAPKmitogen-activated protein kinaseRAS

Study locations (20)

Banner Health- MD Anderson Cancer Center

Gilbert, Arizona, 85234

Recruiting

Brandi Luzania · Contact

480-256-5488 Brandi.Luzania@bannerhealth.com

Jiaxin Niu, MD · Principal Investigator

The Angeles clinic - A cedars SINAI AFFILIATE

Los Angeles, California, 90025

Recruiting

USC Norris Comprehensive Cancer Center

Los Angeles, California, 90033

Recruiting

University of California, San Francisco (UCSF)

San Francisco, California, 94143

Recruiting

University of Colorado - Aurora Cancer Center

Aurora, Colorado, 80045

Not Yet Recruiting

Halle Kuykendall · Contact

720-848-0356 halle.kuykendall@cuanschutz.edu

Yale University School of Medicine - Yale Cancer Center

New Haven, Connecticut, 06520-8028

Recruiting

Georgetown University Lombardi Cancer Center

Washington D.C., District of Columbia, 20007

Not Yet Recruiting

· Contact

202-444-2223 Chul.Kim@gunet.georgetown.edu

Chul Kim, MD · Principal Investigator

Dana-Farber Cancer Institute

Boston, Massachusetts, 02215

Recruiting

Start Your Patient Journey to Cancer Care and Support · Contact

877-442-3324

South Texas Accelerated Research Therapeutics (START) Midwest

Grand Rapids, Michigan, 49546

Recruiting

Julie Burns · Contact

616-954-5559 julie.burns@startmidwest.com

Jade Blakeman · Contact

616-954-5551 jade.blakeman@startmidwest.com

Masonic Cancer Center University of Minnesota

Minneapolis, Minnesota, 55455

Recruiting

Amit Kulkarni, MBBS · Contact

612-624-0123 kulkarni@umn.edu

Sara Crane · Contact

crane202@umn.edu

Washington University

St Louis, Missouri, 63130

Recruiting

Medical Oncology Clinical Call Center · Contact

314-747-1171 MedicalOncologyClinicalCallCenter@dom.wustl.edu

NYU Langone Medical Center - Perlmutter Cancer Center (NYU Cancer Institute)

New York, New York, 10016

Recruiting

Memorial Sloan Kettering Cancer Center

New York, New York, 10065

Recruiting

Michael Offin, MD · Contact

· Contact

646-608-3763

Duke University School of Medicine

Durham, North Carolina, 27710

Recruiting

Cleveland Clinic

Cleveland, Ohio, 44195

Recruiting

Sarah Canon Research Institute (SCRI) Oncology Partners

Nashville, Tennessee, 37203

Recruiting

MD Anderson Cancer Center

Houston, Texas, 77030

Recruiting

START San Antonio

San Antonio, Texas, 78229

Recruiting

NEXT Virginia

Fairfax, Virginia, 22031

Recruiting

Blake Patterson · Contact

703-783-4505 bpatterson@nextoncology.com

Fred Hutchinson Cancer Research Center

Seattle, Washington, 98109

Recruiting

Rebecca Wood · Contact

206-606-6970 rwood1@seattlecca.org