What question did this study set out to answer?

This research aims to uncover the effects of TGF-β inhibition on immune resistance in advanced gastric cancer and identify predictive biomarkers for treatment response.

May 29, 2026

Potential effects of TGF-β inhibition on immune resistance by targeting immunosuppressive microenvironment in advanced gastric cancer (AGC): Multi-omics post-hoc analysis of the K-Umbrella-06 trial.

Key Points

This research aims to uncover the effects of TGF-β inhibition on immune resistance in advanced gastric cancer and identify predictive biomarkers for treatment response.
Examined 30 HER2-negative advanced gastric cancer patients from K-Umbrella-06 trial (NCT04835896) receiving bintrafusp alfa plus paclitaxel.
Analyzed tissue samples using AI-powered whole-slide imaging for fibroblast and endothelial cell assessment.
Conducted transcriptomic profiling and ctDNA sequencing to identify mechanisms of resistance and predictive biomarkers.
Median progression-free survival (mPFS) was 3.8 months, and median overall survival (mOS) was 8.9 months in treated patients.
High fibroblast density predicted better outcomes (mPFS: 4.3 vs. 2.0 months, HR 0.29, P=0.007; mOS: 20.4 vs. 5.8 months, HR 0.28, P=0.012).
The immune-excluded phenotype led to a higher overall response rate (60% vs. 18.2%) compared to inflamed or desert types.

Abstract

2612 Background: TGF-β signaling promotes immune exclusion by driving fibrosis and hindering T-cell infiltration. We performed multi-omics post-hoc analyses of K-Umbrella-06 to identify mechanisms and predictive biomarkers for TGF-β/PD-L1 dual blockade in HER2-negative AGC. Methods: K-Umbrella-06 (NCT04835896) was an investigator-initiated, single-arm, phase Ib/II study enrolling HER2-negative AGC pts who had progressed on 1st-line treatment. Pts received bintrafusp alfa (TGF-β trap/anti–PD-L1) and weekly paclitaxel. Pretreatment H notably, 5 patients achieved durable responses with PFS exceeding 3 years. AI-WSI analysis revealed that high fibroblast density (≥median) was a significant predictor of superior outcomes (mPFS: 4.3 vs. 2.0 months, HR 0.29, P=0.007; mOS: 20.4 vs. 5.8 months, HR 0.28, P=0.012). Conversely, patients with higher intratumoral EC density had shorter mPFS (2.0 vs. 5.9 months, HR 2.29, P=0.058) and mOS (4.0 vs. 8.9 months, HR 1.61, P=0.285). Notably, patients with the immune-excluded phenotype achieved a higher ORR (60.0% vs. 18.2%) and prolonged survival compared to inflamed/desert types. These biomarkers were not predictive in the nivolumab + paclitaxel cohort, suggesting a TGF-β specific effect. Transcriptomic profiling of responders showed enrichment in TGF-β signaling (normalized enrichment score NES 2.87, P<0.001) and SMAD2/3 activity (NES 2.99, P<0.001), alongside increased naive CD8+ T cells and inflamed EC cells. Conversely, non-responders exhibited higher M2 macrophage and abundant angiogenic tip cells. Serial ctDNA analysis identified emergent TGF-β pathway alterations as a potential mechanism of acquired resistance (OR 7.30, P=0.08). Conclusions: Integrated AI-WSI, transcriptomic, and longitudinal ctDNA analyses suggest that TGF-β pathway activation and an immune-excluded phenotype are associated with clinical benefit from bintrafusp alfa plus paclitaxel, and may identify a responder subset distinct from conventional PD-1/PD-L1–based therapy. These findings support further evaluation of anti–TGF-β strategies for AGC with an immunosuppressive tumor microenvironment. Clinical trial information: NCT04835896 .

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