Breakthrough Results with Tulisokibart in Ulcerative Colitis Phase 3 Trial

By João L. Carapinha

June 23, 2026

tulisokibart ulcerative colitis

Tulisokibart ulcerative colitis therapy has achieved a critical milestone, becoming the first anti-TL1A monoclonal antibody to demonstrate clinical remission at week 12 in a Phase 3 trial of patients with moderately to severely active disease. Developed to interrupt immuno-fibrosis — the linked processes of chronic inflammation and fibroblast activation — the agent addresses persistent symptoms including diarrhea, rectal bleeding, urgency, and weight loss that remain uncontrolled by existing treatments.

Tulisokibart ulcerative colitis treatment met the primary endpoint of clinical remission per the Modified Mayo Score, along with all key secondary endpoints including endoscopic improvement and histologic-endoscopic mucosal improvement. These Phase 3 results mirror the efficacy signals observed in earlier Phase 2 studies.

ATLAS-UC Induction Design

The ATLAS-UC induction-only study employed a randomized, double-blind, placebo-controlled structure evaluating high-dose intravenous tulisokibart, low-dose intravenous tulisokibart, and placebo. This focused design isolated initial disease control at week 12, providing robust evidence separate from the parallel maintenance evaluation.

Safety Profile and Program Scope

No new safety signals emerged, reinforcing the consistency of tulisokibart’s tolerability across the largest clinical program in the anti-TL1A class. Merck’s Phase 3 ATLAS-UC data will be presented at an upcoming scientific congress and submitted to regulatory authorities.

Immuno-Fibrosis Treatment Horizon

By simultaneously targeting soluble and membrane-bound TL1A, tulisokibart offers a differentiated mechanism that could alter the progressive course of inflammatory bowel disease. Ongoing Phase 3 and Phase 2 trials across seven immune-mediated conditions position the molecule to reshape both clinical practice and health economic models for relapsing fibro-inflammatory disorders.

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