EASL 2026 Closes in Barcelona — Week Establishes MASH as Multi-Mechanism Field and HBV/HDV as Multi-Modality Cure Race
EASL 2026 closed in Barcelona on May 30 after a week that reshaped two liver-disease narratives. On MASH: the GLP-1/glucagon peptide cohort (survodutide NEJM 47-62% MASH improvement, pemvidutide Best of EASL with cardiometabolic and fibrosis data, MetaVia DA-1726 9.1% weight loss) competed against THR-β agonism (Madrigal Rezdiffra, Aligos ALG-055009 46% liver fat), RNAi (Arrowhead ARO-INHBE), and FGF21 analogs (the Akero and 89bio programs that drew $5.2B and $3.5B acquisitions). On HBV/HDV: the entry-inhibitor peptides (Gilead's newly approved bulevirtide, Assembly's oral ABI-6250) shared the stage with gene editing (Precision PBGENE-HBV cccDNA elimination), epigenetic silencing (TUNE-401), capsid modulation plus ASO sequencing (Aligos), and therapeutic vaccines (Brii BRII-179). The combined week confirmed that liver disease is now a multi-mechanism therapeutic arena where peptides anchor the metabolic and entry-inhibitor lanes while gene and immune modalities pursue functional cure. ADA 2026 (June 5-8 New Orleans) is the next major readout window for the metabolic-peptide side.