| Literature DB >> 31035465 |
Nicole Green1, Talya Miller2, David Suskind3, Dale Lee4.
Abstract
Inflammatory bowel disease (IBD) is a chronic inflammatory condition affecting the gastrointestinal tract. The rising incidence of IBD has been associated with urbanization and shifts toward a Westernized diet. The intestinal microbiome has been a focus of disease pathogenesis and also therapeutic intervention. Dietary therapy for IBD has been well-studied with exclusive enteral nutrition, a formula-based diet with the exclusion of foods. In addition, interest in food-based exclusion diets has been increasing, with patients and families leading the charge. Challenges with dietary therapy for IBD include the lack of understanding of a detailed mechanistic pathway to explain the impact of diet on IBD pathogenesis and the difficult nature of designing and implementing dietary clinical trials. Epidemiological studies have demonstrated associations and intervention studies have demonstrated efficacy, but specific dietary targets remain as hypotheses at present. Current IBD therapy focuses on suppression of the immune system, yet the incomplete efficacy of present drugs suggests that other therapies must be developed and employed. Dietary interventions, with known ability to modulate the intestinal microbiome, are a unique opportunity to improve outcomes in IBD. Dietary intervention trials are challenging, and capturing both broad dietary patterns as well as exposure to individual food compounds is important. With increasing patient interest and preliminary research in dietary therapy indicating efficacy, it is imperative to further advance the science of utilizing diet in IBD, as well as to support patients by proactively addressing diet within their care plan.Entities:
Keywords: Crohn; diet; exclusive enteral nutrition; inflammatory bowel disease; nutrition; ulcerative colitis
Mesh:
Substances:
Year: 2019 PMID: 31035465 PMCID: PMC6566428 DOI: 10.3390/nu11050947
Source DB: PubMed Journal: Nutrients ISSN: 2072-6643 Impact factor: 5.717
Hypothesized Mechanisms of Action for Diet Therapy in Inflammatory Bowel Disease (IBD).
| Category of Mechanism | Hypothesized Mechanism | EEN | Exclusion Diets |
|---|---|---|---|
| Mechanical/physical | Liquid nutrition | x | |
| Alteration of gut motility | x | x | |
| Gut rest | x | ||
| Nutritional status | Improved nutrient delivery | x | |
| Improved caloric delivery | x | ||
| Epithelial barrier | Decreased permeability | x | x |
| Restitution of intestinal barrier | x | x | |
| Improved delivery of fiber (SCFA * production) | x | ||
| Immune system | Limited antigen exposure | x | |
| Antigenic monotony | x | ||
| Direct anti-inflammatory effect | x | x | |
| Alteration in bile acids | x | x | |
| Microbiome | Shift of gut microbiome | x | x |
| Stabilize gut microbiome | x | x | |
| Specific avoidances | Avoidance of food additives | x | |
| Avoidance of deleterious food substances | x | x | |
| Anti-inflammatory effect | Provide beneficial substance | x | x |
| Increased antioxidant consumption | x |
* SCFA: short-chain fatty acid.
Comparison of Dietary Therapy and Drug Therapy.
| Dietary Therapy | Drug Therapy | |
|---|---|---|
| Driven by patient/family interest | ++ | |
| Ability to personalize | ++ | + |
| Directly impacts quality of life * | ++ | |
| Importance of family support | ++ | + |
| Challenges with compliance | ++ | + |
| Challenges with study design | ++ | |
| Risk of nutrient deficiency | ++ | |
| Works in combination with other therapies | ++ | ++ |
| Physician-driven | ++ | |
| Targets known pathway | ++ | |
| Greater risk of infection | ++ | |
| Greater risk of cancers | ++ | |
| Insurance coverage | ++ | |
| Partnership with large industry to study ** | ++ |
* Independent of disease activity. ** Formula companies have supported the design and implementation of some studies on EEN, but the majority of dietary trials do not have corporate backing.
Dietary Therapy for IBD: Now and the Future.
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| EEN in pediatric Crohn’s disease |
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| Impact of dietary therapies with/without concomitant immunosuppression |