Clinical Trials: Difference between revisions

Mesothelioma Clinical Trials represent the cutting edge of treatment research, offering patients access to breakthrough therapies before they become widely available. As of January 2026, fifty-three mesothelioma clinical trials are actively recruiting patients across the United States, including revolutionary CAR-T cell therapies achieving 83% one-year survival, the first-ever Phase III trial of a TEAD inhibitor, and AI-designed drugs now in human testing.^[1]

The mesothelioma clinical trial landscape has transformed dramatically, yet patient participation remains critically low at just 8%—a significant drop from 14% in 2023.^[2] This gap exists despite proven survival benefits from trial participation. According to the National Cancer Institute, clinical trials are research studies that test new treatments and are essential to advancing cancer care.^[3] In January 2026, patients have access to immunotherapy combinations extending median survival beyond 18 months, targeted therapies achieving 32% response rates in previously untreatable disease, and cellular therapies demonstrating unprecedented durability. The FDA approved pembrolizumab plus chemotherapy in September 2024 as a new first-line standard, with subcutaneous Keytruda QLEX following in January 2026.^[4] VT3989, the first TEAD inhibitor, will advance to Phase III registration trials in the first half of 2026, representing a major milestone for targeted therapy in this disease. For patients and families navigating treatment decisions alongside legal compensation, specialized mesothelioma attorneys can help coordinate both processes simultaneously.^[5]

Phase III trials represent the final stage before FDA approval and offer patients access to therapies that have already demonstrated efficacy in earlier studies.

The eVOLVE-Meso trial is a Phase III, randomized, open-label, multicenter study testing volrustomig (MEDI5752), a novel PD-1/CTLA-4 bispecific antibody, in combination with carboplatin and pemetrexed.^[8]

Trial Specifications:

• Status: Actively recruiting globally
• Sponsor: AstraZeneca
• Enrollment Target: 825 patients worldwide
• Mechanism: PD-1/CTLA-4 bispecific antibody providing selective CTLA-4 blockade on activated T cells
• Comparator Arms: Platinum-based chemotherapy or nivolumab plus ipilimumab
• Eligibility: Unresectable pleural mesothelioma with no prior systemic therapy
• Locations: United States, Canada, Brazil, China, Europe, Japan
• Expected Completion: Data anticipated post-2026

The ATOMIC-Meso trial has completed, with practice-changing results published in JAMA Oncology in March 2024.^[9]

Published Results (249 patients with non-epithelioid pleural mesothelioma):

• Median overall survival: 9.3 months versus 7.7 months with placebo plus chemotherapy
• Three-year survival: Quadrupled compared to placebo arm
• Progression-free survival: 6.2 months versus 5.6 months (HR 0.65; p=0.02)
• Risk reduction: 35% reduction in progression risk
• Mechanism: Arginine depletion therapy targeting ASS1-deficient tumors

CAR-T (Chimeric Antigen Receptor T-cell) therapy represents one of the most promising frontiers in mesothelioma treatment, with multiple trials demonstrating unprecedented survival outcomes.^[10]

This Phase I dose-escalation study evaluates anti-mesothelin TNaive/SCM hYP218 CAR T cells, designed for enhanced tumor infiltration and persistence.^[11]

Trial Details:

• Status: Recruiting since 2025
• Location: National Cancer Institute, Bethesda, Maryland
• Innovation: Targets membrane-proximal epitope of mesothelin, showing 2-4 fold better tumor killing than membrane-distal approaches in preclinical studies
• Eligibility: Age 18 or older, mesothelin expression greater than 50% of tumor cells, ECOG 0-1
• Monitoring: Patients must remain within 2 hours of NIH for 30 days post-infusion
• Follow-up: 15 years per FDA requirement

This groundbreaking program pioneered regional delivery of CAR-T cells directly into the pleural space, minimizing systemic toxicity while maximizing tumor contact.^[12]

Published Results:

• One-year survival: 83% for malignant pleural mesothelioma patients
• CAR-T persistence: Cells detected in peripheral blood for more than 100 days in 39% of patients
• Durable responses: One patient achieved partial response lasting 26 months
• Safety profile: Intrapleural administration was safe and well tolerated
• Combination approach: 18 patients received CAR-T with pembrolizumab, demonstrating enhanced function

This novel approach uses KIR-CAR T cells targeting mesothelin across multiple tumor types including mesothelioma.^[13]

• Status: Completed enrollment of Cohorts 1-3 without dose-limiting toxicities as of May 2025
• Sites: Multiple US locations including Penn Medicine
• Safety: No dose-limiting toxicities in completed cohorts

VT3989 represents a breakthrough in targeting the previously "undruggable" Hippo/YAP/TEAD pathway, which is dysregulated in the majority of mesotheliomas.^[14]

ESMO 2025 Results (Published Nature Medicine December 2025):

• Objective response rate: 32% in 22 mesothelioma patients at optimized dose
• Disease control rate: 86% when incorporating optimal dose and UACR threshold
• Median progression-free survival: 10 months
• Duration of response: 8 patients on treatment more than 1 year; one approaching 2 years
• Selected dose: 100 mg two-weeks-on/two-weeks-off for Phase III
• Safety: Favorable profile with mostly grade 1-2 toxicities; proteinuria reversible with dose adjustment
• Tumor types: Activity demonstrated in both NF2-mutant and wild-type tumors

Regulatory Designations:

• FDA Orphan Drug Designation^[15]
• FDA Fast Track Designation

This pan-TEAD inhibitor was designed using Insilico Medicine's Chemistry42 AI platform, representing the first AI-designed drug to enter clinical testing for mesothelioma.^[16]

Development Timeline:

• September 2020: AI platform launched
• June 2023: Recommended for preclinical studies
• April 2024: AACR presentation showing broad cancer-killing effects
• June 2024: FDA Orphan Drug Designation granted
• August 2024: IND clearance received
• January 22, 2025: First patient dosed in China
• 2026: US enrollment expected

Mechanism: Pan-TEAD inhibitor blocking the palmitoylation site, disrupting YAP/TAZ-TEAD transcriptional activity

Novartis discontinued development of IAG933 in October 2025 following underwhelming ESMO 2025 data showing only 13% objective response rate in 30 pleural mesothelioma patients. QTc prolongation dose-limiting toxicities in 4 patients contributed to the decision.^[17]

The KEYNOTE-483 trial led to FDA approval for first-line treatment of unresectable advanced or metastatic malignant pleural mesothelioma on September 17, 2024.^[18]

Trial Results:

• Median overall survival: 16.9 months versus 14.1 months with chemotherapy alone
• Hazard ratio: 0.79 (95% CI: 0.63-0.99; p=0.0209)
• Confirmed objective response rate: 52% versus 29%
• Median duration of response: 6.9 versus 6.8 months
• Regimen: Pembrolizumab with pemetrexed and platinum chemotherapy

January 2026 Update: FDA approved Keytruda QLEX (subcutaneous pembrolizumab) on January 11, 2026, offering a 1-minute injection every 3 weeks as an alternative to IV infusion for all 38 pembrolizumab indications including mesothelioma.

CheckMate 743 remains the only Phase 3 trial demonstrating survival improvement sustained over 3 years with first-line immunotherapy in unresectable malignant pleural mesothelioma.^[19]

Three-Year Follow-up Results:

• Three-year overall survival: 23.2% versus 15.4% with chemotherapy
• Sustained benefit: Observed regardless of histology
• Duration of response: Longer with dual immunotherapy at 3 years
• Safety: Consistent profile with no new signals at long-term follow-up

This PD-L1/VEGF-A bispecific antibody demonstrated remarkable activity at ASCO 2025, particularly in peritoneal mesothelioma.^[20]

Phase 2 Trial Results (31 patients with unresectable mesothelioma):

• Confirmed overall response rate: 51.6%
• Peritoneal mesothelioma cohort (8 patients): 75% ORR, 100% disease control rate
• Median exposure: 16.0 months (95% CI 8.1-19.5)
• Median follow-up: 19.3 months
• Safety: 93.5% experienced grade 3/4 adverse events; no treatment-related deaths

Phase 3 trial planning is underway (NCT07133750 registered July 2025).

The NIPU trial (Phase II, NCT04300244) demonstrated statistically significant survival improvement when UV1 telomerase vaccine was added to nivolumab plus ipilimumab.^[21]

Results (118 patients randomized):

• Median overall survival: 15.4 months with UV1 versus 11.1 months without—statistically significant
• Median progression-free survival: 4.2 months versus 2.9 months
• Objective response rate: 31% versus 16%
• Safety: Comparable adverse event rates between groups
• Regulatory Status: FDA Fast Track Designation granted February 2024

Most mesothelioma clinical trials require patients to meet specific baseline criteria. The National Cancer Institute provides guidance on understanding clinical trial eligibility.^[22]

ECOG Performance Status:

• ECOG 0: Fully active, able to carry on all pre-disease activities without restriction
• ECOG 1: Restricted in physically strenuous activity but ambulatory and able to carry out light work
• ECOG 2: Some trials accept for exceptional cases
• Alternative measure: Karnofsky score 70% or higher

• Absolute neutrophil count 1,500/μL or higher
• Platelet count 100,000/μL or higher
• Hemoglobin 9.0 g/dL or higher
• Creatinine clearance 45 mL/min or higher
• Bilirubin 1.5x upper limit of normal or lower

• Histologically confirmed mesothelioma (pathology report required)
• Measurable disease by modified RECIST criteria
• No untreated brain metastases
• Specific histology requirements vary by trial
• Some trials require specific biomarker expression (mesothelin greater than 50% for certain CAR-T trials)

• TNhYP218 CAR-T trial (NCT06885697)
• Multiple additional mesothelioma studies
• Travel assistance programs available
• Contact: NCI Cancer Information Service 1-800-4-CANCER^[23]

• 16+ active mesothelioma trials
• VT3989 TEAD inhibitor trial (lead investigator: Dr. Timothy Yap)
• Specialized mesothelioma program
• Telemedicine consultations offered^[24]

• Intrapleural CAR-T program (NCT04577326)
• International patient services
• Dedicated mesothelioma team^[25]

• ISM6331 trial site
• ICARuS II peritoneal trial (NCT06057935)
• Multiple systemic therapy trials

• SMARTER trial headquarters
• International enrollment accepted
• Modified surgical protocols

• Study drug or intervention
• Trial-specific tests and procedures
• Additional monitoring visits required by protocol
• Some travel expenses (varies by trial)

• Standard of care treatments
• Routine doctor visits
• Hospital stays if not trial-related
• Most travel and lodging expenses

The Affordable Care Act requires most health plans to cover routine patient costs in clinical trials.^[26]

• Medicare: Covers qualifying trials for Medicare beneficiaries
• Private insurance: 44 states require coverage; check your state's mandates
• Medicaid: Coverage depends on state regulations
• VA benefits: VA covers trial participation at approved facilities for eligible veterans

^[27]

VT3989 Phase III:

• First registrational trial of a TEAD inhibitor in mesothelioma
• Based on ESMO 2025 data showing 32% ORR
• Third-line indication^[28]

BNT327/PM8002 Phase III:

• NCT07133750 registered July 2025
• Building on exceptional Phase 2 results

ISM6331 US Enrollment:

• Expected to open following January 2025 China enrollment
• First AI-designed mesothelioma drug

MVdeltaC First-in-Human:

• Measles virus-based immunotherapy
• FDA Orphan Drug Designation June 2025
• Clinical trial planned for 2026

Antibody-Drug Conjugates (ADCs):

• SGN-MesoC2 recruiting (updated November 2025)
• Rinatabart Sesutecan (GEN1184/PRO1184) recruiting (updated December 2025)^[29]

• ClinicalTrials.gov: Official NIH database with all registered trials^[30]
• NCI Cancer Information Service: 1-800-4-CANCER
• EmergingMed Navigator: Free matching service
• Lazarex Cancer Foundation: Financial assistance for trial costs^[31]

1. What phase is the trial? (Phase I = safety focus, Phase II = efficacy, Phase III = comparison)
2. What are the specific eligibility requirements?
3. How many visits are required and where?
4. What costs will I be responsible for?
5. Can I leave the trial if needed?
6. How will this affect my other treatment options?
7. What are the known risks and potential benefits?
8. What happens if the treatment works—can I continue receiving it?

^[32]

Patients participating in clinical trials can simultaneously pursue legal compensation from asbestos trust funds and responsible companies. This compensation is entirely separate from trial participation and can help cover expenses not covered by the trial, including travel, lodging, lost wages, and care for family members.^[33]

• Asbestos Trust Funds — Access $30+ billion in asbestos trust fund compensation
• Veterans Benefits — Veterans disability claims and healthcare coverage
• Choosing a Mesothelioma Attorney — What to look for in mesothelioma legal representation
• Mesothelioma Treatment Centers — Specialized mesothelioma treatment facilities nationwide
• Understanding Your Diagnosis — Medical information for newly diagnosed patients