What question did this study set out to answer?

This study aims to evaluate the impact of SARS-CoV-2 mRNA vaccines on survival outcomes in patients with solid tumors receiving immunotherapy.

May 29, 2026

Impact of COVID-19 mRNA vaccines on survival outcomes in patients with solid tumors receiving immunotherapy: A large-scale retrospective study.

Key Points

This study aims to evaluate the impact of SARS-CoV-2 mRNA vaccines on survival outcomes in patients with solid tumors receiving immunotherapy.
Multicenter retrospective study using the TriNetX global network
Identified adults with various solid tumors who received immune checkpoint inhibitors
1:1 propensity score matching used to balance demographics and comorbidities.
Vaccination associated with improved median overall survival (1,421 vs 667 days; HR 0.63; 95% CI 0.60-0.66; p<0.001)
Benefit observed across 10 of 12 tumor types, notably in NSCLC and melanoma
No significant survival benefit seen in breast or gallbladder cancer.

Abstract

2637 Background: Immune checkpoint inhibitors (ICIs) became the cornerstone in the treatment of solid tumors. While personalized cancer vaccines have yet to overcome complex scalability and manufacturing challenges, preclinical data suggests SARS-CoV-2 mRNA vaccines prime innate immunity, potentially enhancing ICI efficacy. A study by Grippin et al. evaluated the use of mRNA vaccine in NSCLC and melanoma patients receiving ICI and showed improved median and three-year overall survival (OS). We conducted a multicenter retrospective study to determine if this survival benefit extends across a broader range of ICI-treated solid tumors. Methods: Using the TriNetX global network, we identified adults (≥18) with solid tumors (NSCLC, melanoma, colorectal, hepatobiliary, gallbladder, gastric, bladder, pancreatic, renal, breast, head and neck, and esophageal) who received ICI treatment. The experimental group received SARS-CoV-2 mRNA vaccine within 100 days of ICI initiation; controls received no mRNA vaccine from 100 days pre-index through follow-up. Exclusion criteria: COVID-19 infection within 100 days and through the follow-up period. 1:1 propensity score matching (PSM) balanced demographics and comorbidities. Primary endpoint was median OS, including tumor-specific subgroup analyses. Survival was assessed via Kaplan-Meier and log-rank tests. Results: After PSM, we had 15,374 matched patients (7,687 per group). Vaccination within 100 days of ICI was associated with improved median OS (1,421 vs 667 days; HR 0.63; 95% CI 0.60-0.66; p<.001). Benefit was observed in 10 of 12 tumor types. Strongest effects were in NSCLC (n=7,350; HR 0.64), melanoma (n=2,684; HR 0.61; landmark survival 62.1% vs 50.3%), hepatobiliary (n=1,428; HR 0.64), colorectal (n=1,068; HR 0.67), gastric (n=792; HR 0.68), bladder (n=1,398; HR 0.63), pancreatic (n=240; HR 0.65), renal (n=1,996; HR 0.64), head and neck (n=964; HR 0.68), and esophageal (n=828; HR 0.63). No significant benefit was seen in breast (n=1,412; HR 0.85) or gallbladder cancer (n=58; HR 0.88). Conclusions: SARS-CoV-2 mRNA vaccination within 100 days of ICI therapy was associated with improved survival across solid tumors. These results suggest off-the-shelf RNA therapeutics may be scalable, cost-effective enhancers of cancer immunotherapy. Prospective studies are needed to confirm these findings and define the impact of universal mRNA strategies.

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