Neoadjuvant nivolumab or nivolumab plus LAG-3 inhibitor relatlimab in resectable esophageal/gastroesophageal junction cancer: a phase Ib trial and ctDNA analyses

Ronan J. Kelly(Baylor University Medical Center), Blair V. Landon(Johns Hopkins University), Ali H. Zaidi(Allegheny Health Network), Dipika Singh(Bloomberg (United States)), Jenna VanLiere Canzoniero(Johns Hopkins University), Archana Balan(Johns Hopkins University), Russell K. Hales(Johns Hopkins University), Khinh Ranh Voong(Johns Hopkins University), Richard J. Battafarano(Johns Hopkins University), Blair A. Jobe(Allegheny Health Network), Stephen C. Yang(Johns Hopkins University), Stephen Broderick(Johns Hopkins University), Jinny S. Ha(Johns Hopkins University), Kristen A. Marrone(Bloomberg (United States)), Gavin Pereira(Johns Hopkins University), Nisha Rao(Johns Hopkins University), Aryan Borole(Johns Hopkins University), Katerina Karaindrou(Johns Hopkins University), Zineb Belcaid(Johns Hopkins University), James R. White(Johns Hopkins University), Suqi Ke(Johns Hopkins University), Ali Imran Amjad(Allegheny Health Network), Benny Weksler(Allegheny Health Network), Eun Ji Shin(Johns Hopkins University), Elizabeth D. Thompson(Johns Hopkins University), Kellie N. Smith(Bloomberg (United States)), Drew M. Pardoll(Bloomberg (United States)), Chen Hu(Johns Hopkins University), Josephine Feliciano(Johns Hopkins University), Valsamo Anagnostou(Bloomberg (United States)), Vincent K. Lam(Johns Hopkins University)
Nature Medicine
March 19, 2024
10.1038/s41591-024-02877-z
Cited by 106Open Access
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Abstract

Gastroesophageal cancer dynamics and drivers of clinical responses with immune checkpoint inhibitors (ICI) remain poorly understood. Potential synergistic activity of dual programmed cell death protein 1 (PD-1) and lymphocyte-activation gene 3 (LAG-3) inhibition may help improve immunotherapy responses for these tumors. We report a phase Ib trial that evaluated neoadjuvant nivolumab (Arm A, n = 16) or nivolumab-relatlimab (Arm B, n = 16) in combination with chemoradiotherapy in 32 patients with resectable stage II/stage III gastroesophageal cancer together with an in-depth evaluation of pathological, molecular and functional immune responses. Primary endpoint was safety; the secondary endpoint was feasibility; exploratory endpoints included pathological complete (pCR) and major pathological response (MPR), recurrence-free survival (RFS) and overall survival (OS). The study met its primary safety endpoint in Arm A, although Arm B required modification to mitigate toxicity. pCR and MPR rates were 40% and 53.5% for Arm A and 21.4% and 57.1% for Arm B. Most common adverse events were fatigue, nausea, thrombocytopenia and dermatitis. Overall, 2-year RFS and OS rates were 72.5% and 82.6%, respectively. Higher baseline programmed cell death ligand 1 (PD-L1) and LAG-3 expression were associated with deeper pathological responses. Exploratory analyses of circulating tumor DNA (ctDNA) showed that patients with undetectable ctDNA post-ICI induction, preoperatively and postoperatively had a significantly longer RFS and OS; ctDNA clearance was reflective of neoantigen-specific T cell responses. Our findings provide insights into the safety profile of combined PD-1 and LAG-3 blockade in gastroesophageal cancer and highlight the potential of ctDNA analysis to dynamically assess systemic tumor burden during neoadjuvant ICI that may open a therapeutic window for future intervention. ClinicalTrials.gov registration: NCT03044613 .

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