From the Cochrane Library: Leukotriene Receptor Antagonists for Eczema
Lauren Marie Toledo, Ramiro Rodriguez, Torunn E Sivesind, Efstratios Vakirlis, Reiji Kojima, Robert P Dellavalle

Abstract
Genes, proteins, chemicals, diseases, species, mutations and cell lines named across the full text — each resolved to its canonical identifier and authoritative record.
|
| Study (year) | ||||
|
| Capella et al (2001) | Friedmann et al (2007) | Nettis et al (2002) | Rahman et al (2006) | Veien et al (2005) |
| Study title | A randomized trial of leukotriene receptor antagonist montelukast in moderate‐to-severe atopic dermatitis of adults | A double‐blind, placebo‐controlled trial of montelukast in adult atopic eczema | Efficacy and tolerability of montelukast as a therapeutic agent for severe atopic dermatitis in adults | Effectiveness of montelukast in the treatment of atopic dermatitis | Montelukast treatment of moderate to severe atopic dermatitis in adults: a randomized, double‐blind, placebo‐controlled trial |
| Participants, N | 32 | 58 | 20 | 31 | 53 |
| Type of trial | Single blind | Double blind | Double blind | Open label | Double blind |
| Length of study | 6 weeks | 8 weeks | 6 weeks | 4 weeks | 4 weeks |
| Intervention vs comparator | Oral montelukast + oral placebo + topical placebo gel vs | Montelukast vs placebo | Montelukast vs placebo | Montelukast vs | Montelukast vs placebo |
| Montelukast dose | 10 mg for adults, 5 mg for children | 10 mg for adults, 5 mg for children | 10 mg for adults, 5 mg for children | 10 mg for adults, 5 mg for children | 10 mg for adults, 5 mg for children |
| Scale | SCORADa | SASSADb | SCORAD | SCORAD | Modified EASIc |
| Study conclusions | Significant improvement in SCORAD scores of both montelukast and placebo groups but no significant difference | No significant difference between montelukast and placebo for pruritus improvement | 20% significant reduction in SCORAD with montelukast. Montelukast was superior | Significant improvement in SCORAD with montelukast compared to conventional treatment. Montelukast was superior | No significant difference between the EASI scores of montelukast and placebo groups |
| Reason for lack of evidence | Low quality of evidence, small sample size, high risk of bias | Low quality of evidence, small sample size | Low quality of evidence, small sample size | Low quality of evidence, small sample size | Low quality of evidence, small sample size, high risk of bias |
| Standard mean difference (95% CI), inverse variance, random | Not provided | –0.03 (–0.54 to 0.49) | 1.09 (0.13 to 2.04) | 10.57 (4.58 to 16.56) | 0.20 (–0.34 to 0.74) |
| Adverse effects | None | Dizziness reported; mild in nature except for a brief septicemic illness | None | None | None |
Peer Reviews
No public reviews on file for this paper yet. If you reviewed it on a platform where reviews are public (OpenReview, ICLR, NeurIPS, ICML), you can paste yours below so the community can read it here.
Videos
No videos yet. Explain this paper in a talk, walkthrough, or lecture? Add one.
Taxonomy
TopicsDermatology and Skin Diseases · Food Allergy and Anaphylaxis Research · Allergic Rhinitis and Sensitization
Introduction
Atopic dermatitis (AD), a chronic inflammatory skin disease, is estimated to affect up to 10% of adults and 20% of children worldwide [1]. Clinical manifestations include pruritus, skin lesions, and dry scaly skin [2,3]. First-line treatment includes topical steroids and emollients, with systemic steroids or immune modulators for moderate-to-severe AD. Despite the standard practice of using topical corticosteroids in AD treatment, long-term use poses the risk of local adverse effects of skin thinning, striae, and purpura, or systemic effects such as growth suppression and suppression of the hypothalamic-pituitary axis [4]. Other medications, such as leukotriene receptor antagonists (LTRAs), are being researched as an alternative treatment option [5]. A 2018 Cochrane review, “Leukotriene receptor antagonists for eczema” [6], examined clinical trials to determine if there is sufficient evidence to recommend LTRAs for use in patients with AD but concluded that there was limited, low-quality evidence of its efficacy and safety.
Methods
This Cochrane review extracted data across 5 studies and 202 participants to evaluate the evidence of LTRA effectiveness in AD. Of these studies, 3 assessed the efficacy of LTRAs compared to a placebo and 2 assessed the effectiveness of LTRAs versus conventional treatment (combined antihistamines and topical steroids). All assessed the effectiveness of the LTRA montelukast, met inclusion criteria of being a randomized controlled trial (RCT) and assessing patients with moderate-to-severe eczema, and tested interventions for the acute or chronic phase of AD. Interventions assessed independent administration of montelukast (oral or intravenous) or montelukast in combination with other topical and systemic treatments (corticosteroids, topical calcineurin inhibitors, immunomodulators, or placebo).
Results
Only 1 RCT resulted in greater improvement with LTRA intervention compared to conventional treatment but was of low quality. None of the studies addressed long-term control (primary outcome) or higher quality of life and lower emollient requirement (secondary outcomes) at all (Table 1). The quality of supporting evidence was assessed by GRADE (Grading of Recommendations, Assessment, Development, and Evaluations) based on 5 domains: limitations and risk of bias, inconsistency, direct relation of evidence, imprecision, and publication bias. While valuing the certainty of evidence, it is essential to be aware that judgments may vary between individuals with this method. The authors note it is challenging to draw firm conclusions from the results of these studies because the studies had an unclear or high risk of bias, including but not limited to selection and detection. Limitations of the studies included the absence of testing other LTRAs besides montelukast, inclusion of only adult participants and participants with moderate-to-severe eczema, and a small sample size. Detection biases were present in 2 studies due to the lack of blinding of the outcome assessment; performance bias was of concern in 1 study due to the lack of blinding of participants and personnel in an open RCT. Potential confounders (eg, diet, detergent, household chemicals, climate, location, allergens) were not assessed, which could contribute to an underestimate or overestimate of the true association between LTRAs and AD.
Discussion
Experimental data on the involvement of leukotrienes in allergic inflammation suggests LTRA therapy might be promising for the treatment of AD [3]; however, the results to date are unclear and lack uniformity. The increasing incidence of AD highlights the need for additional investigation to identify the most effective treatments, especially those that can be used as long-term maintenance therapy. While there is no compelling evidence in this review for or against LTRA use for AD treatment, a large, well-designed RCT with multiple LTRAs would help better understand LTRA’s role in long-term AD management.
The reference list from the paper itself. Each links out to its DOI / PubMed record.
- 1Langan SM Mulick AR Rutter CE Silverwood R Asher I García‐Marcos L Ellwood E Bissell K Chiang C Sony AE Ellwood P Marks G Mortimer K Martínez‐Torres AE Morales E Perez‐Fernandez V Robertson S Williams H Strachan DP Pearce N Trends in eczema prevalence in children and adolescents: a Global Asthma Network phase I study Clin Experimental Allergy 2023020853333735210.1111/cea.14276 · doi ↗
- 2Bylund S Kobyletzki LB Svalstedt M Svensson Prevalence and incidence of atopic dermatitis: a systematic review Acta Derm Venereol 2020060910012 adv 00160 10.2340/00015555-35103241264632412646 PMC 9189744 · doi ↗ · pubmed ↗
- 3Frazier W Bhardwaj N Atopic dermatitis: diagnosis and treatment Am Fam Physician 2020051510110590598 32412211 d 1492932412211 · pubmed ↗
- 4Lax S Harvey J Axon E Howells Laura Santer Miriam Ridd Matthew J Lawton Sandra Langan Sinéad Roberts Amanda Ahmed Amina Muller Ingrid Ming Long Chiau Panda Saumya Chernyshov Pavel Carter Ben Williams Hywel C Thomas Kim S Chalmers Joanne R Strategies for using topical corticosteroids in children and adults with eczema Cochrane Database Syst Rev 2022031133 CD 013356 10.1002/14651858.CD 013356.pub 23527539935275399 PMC 8916090 · doi ↗ · pubmed ↗
- 5Nettis ED'Erasmo M Di Leo E Calogiuri G Montinaro V Ferrannini A Vacca A The employment of leukotriene antagonists in cutaneous diseases belonging to allergological field Mediators Inflamm 201020101610.1155/2010/62817110.1155/2010/62817120886028628171 PMC 294567320886028 · doi ↗ · pubmed ↗
- 6Ferguson L Futamura M Vakirlis E Kojima Reiji Sasaki Hatoko Roberts Amanda Mori Rintaro Leukotriene receptor antagonists for eczema Cochrane Database Syst Rev 201810211010 CD 011224 10.1002/14651858.CD 011224.pub 23034349830343498 PMC 6517006 · doi ↗ · pubmed ↗
