4.4 Review

Can we change the natural course of inflammatory bowel disease?

Journal

THERAPEUTIC ADVANCES IN GASTROENTEROLOGY
Volume 16, Issue -, Pages -

Publisher

SAGE PUBLICATIONS LTD
DOI: 10.1177/17562848231163118

Keywords

complications; Crohn's disease; disease modification; disease progression; inflammatory bowel disease; treat-to-target; ulcerative colitis

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Inflammatory bowel diseases (IBD) are chronic lifelong diseases characterized by inflammation and irreversible damage to the gastrointestinal tract. The impact of early initiation of IBD-specific therapy on long-term disease progression needs to be further explored. Surgery and hospitalization rates have been used as surrogate markers to measure disease progression in IBD, but they may not accurately reflect the effectiveness of medical therapies.
Inflammatory bowel diseases (IBD), including Crohn's disease (CD) and ulcerative colitis (UC), are lifelong diseases characterized by chronic inflammation of the gastrointestinal tract leading to its progressive and irreversible destruction. Whether early initiation of IBD-specific therapy impacts the long-term course of the disease remains unclear and has to be further explored in prospective disease-modification trials. Historically, surgery and hospitalization rates have been the surrogate markers to measure disease progression in IBD, providing an overview of the effectiveness of medical therapies. However, neither surgery nor hospitalization necessarily reflects a fail in therapeutic medical management, and many confounding factors make them biased outcomes. The Selecting Endpoints for Disease-Modification Trials consensus has defined the disease-modification endpoints required for these trials, including the impact of the disease on patient's life (health-related quality of life, disability, and fecal incontinence), the mid-term disease complications (bowel damage in CD, IBD-related surgery and hospitalizations, disease extension in UC, extra-intestinal manifestations, permanent stoma, short bowel syndrome), and the development of dysplasia/cancer and mortality in the long term. Most available data in the literature regarding the impact of current therapies on disease progression focused on anti-tumor necrosis factor agents and are based on retrospective or post-hoc studies. Thus, prospective disease-modification trials are pressingly required to explore the effectiveness of early intensified treatment in patients with severe disease or at risk for disease progression.

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