Allergic Rhinitis and Allergic Sensitization in Pediatric Otitis Media with Effusion: A Systematic Review and Meta-Analysis with Narrative Synthesis of Eustachian Tube Dysfunction
Highlights
- Allergic rhinitis/rhinitis was significantly associated with pediatric otitis media with effusion, with a pooled odds ratio of 3.73 in the primary random-effects meta-analysis.
- Atopy or IgE sensitization was also associated with OME, but the evidence was based on fewer studies and showed high heterogeneity.
- Allergic rhinitis and allergic sensitization should be considered potential contributing factors in selected pediatric OME phenotypes, especially when persistent nasal symptoms coexist with ear complaints, hearing concerns, or abnormal tympanometry.
- The findings support phenotype-based ENT and allergy/immunology assessment, but do not justify treating all pediatric OME as allergy-driven disease.
Abstract
1. Introduction
2. Materials and Methods
2.1. Study Design and Reporting
2.2. Eligibility Criteria
2.3. Information Sources and Search Strategy
2.4. Study Selection
2.5. Data Extraction
- a = exposed participants with outcome;
- b = exposed participants without outcome;
- c = unexposed participants with outcome;
- d = unexposed participants without outcome.
2.6. Outcomes
2.7. Risk of Bias Assessment
2.8. Statistical Analysis
3. Results
3.1. Search Results and Study Selection
3.2. Characteristics of Included Studies
3.3. Primary Meta-Analysis: Allergic Rhinitis/Rhinitis and OME
3.4. Expanded Sensitivity Analysis
3.5. Exploratory Quantitative Synthesis of Atopy/IgE Sensitization and OME
3.6. Narrative Synthesis of Eustachian Tube Dysfunction and Middle-Ear Dysfunction
3.7. Qualitative and Mechanistic Evidence
3.8. Risk of Bias
4. Discussion
4.1. Main Findings
4.2. Clinical and Methodological Heterogeneity
4.3. Confounding and Interpretation of Crude Estimates
4.4. Biological Plausibility
4.5. Eustachian Tube Dysfunction and Middle-Ear Dysfunction
4.6. Clinical Implications
4.7. Strengths
4.8. Limitations
4.9. Future Research
5. Conclusions
Supplementary Materials
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Acknowledgments
Conflicts of Interest
Abbreviations
| Abbreviation | Definition |
| AOM | Acute otitis media |
| AR | Allergic rhinitis |
| CI | Confidence interval |
| ENT | Ear, nose, and throat |
| ETD | Eustachian tube dysfunction |
| ETDQ-7 | Eustachian Tube Dysfunction Questionnaire-7 |
| IgE | Immunoglobulin E |
| MEP | Middle-ear pressure |
| NHANES | National Health and Nutrition Examination Survey |
| OME | Otitis media with effusion |
| OR | Odds ratio |
| PRISMA | Preferred Reporting Items for Systematic Reviews and Meta-Analyses |
| SPT | Skin-prick test |
| URTI | Upper respiratory tract infection |
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| Study | Country | Design | Population | Exposure | Outcome | Assessment/Diagnostic Method | Role in Synthesis |
|---|---|---|---|---|---|---|---|
| Pau and Ng, 2016 [9] | Hong Kong | Cross-sectional | Children aged 4–12 years | Allergic rhinitis | OME | Pneumatic otoscopy and portable tympanometry | Primary AR/rhinitis–OME meta-analysis |
| Fasunla et al., 2017 [10] | Nigeria | Case–control | Children aged 2–7 years | Allergic rhinitis | OME | AR diagnosed by symptoms and nasal cytology; OME by Jerger tympanometric patterns | Primary AR/rhinitis–OME meta-analysis |
| Sharifian et al., 2019 [11] | Iran | Case–control | 37 children with OME and 52 controls | Allergic rhinitis | OME | OME diagnosed by otoscopy and/or type B tympanogram; AR by clinical assessment and allergy testing where indicated | Primary AR/rhinitis–OME meta-analysis |
| Caffarelli et al., 1998 [12] | Italy | Case–control | 172 children with OME and 200 controls | Allergic rhinitis/atopic symptoms | OME | OME by otoscopy and type B/C tympanograms; allergic disorders assessed by questionnaire, clinical examination, and skin-prick testing | Primary AR/rhinitis–OME meta-analysis |
| Yeo et al., 2007 [13] | South Korea | Prospective case–control | 123 children with chronic OME and 141 controls | Allergic rhinitis | Chronic OME | OME by otoscopy and tympanometry; AR by history, examination, skin testing and/or MAST-CLA | Primary AR/rhinitis–OME meta-analysis |
| Kayhan et al., 2002 [14] | Turkey | Case–control | 22 children with OME and 21 controls | Allergic rhinitis | OME | OME by physical examination and tympanometry; AR by symptoms, IgE, skin-prick testing and nasal smear | Primary AR/rhinitis–OME meta-analysis |
| Adekanye et al., 2024 [15] | Nigeria | Community cross-sectional | 320 children aged 1–10 years | Clinically defined allergic rhinitis | OME | AR by rhinological symptoms plus allergy/family/asthma history; OME by otoscopy and tympanometry | Expanded sensitivity analysis |
| Kreiner-Møller et al., 2012 [18] | Denmark | Prospective birth cohort | COPSAC children assessed at 6 years | Allergic rhinitis | OME | AR defined by symptoms, sensitization and relevant exposure; OME by otoscopy and tympanometry | Adjusted-OR/narrative sensitivity |
| Chantzi et al., 2006 [16] | Greece | Case–control | 88 children with OME and 80 controls, aged 1–7 years | IgE sensitization | OME | OME by symptoms, otoscopy and tympanometry; sensitization by SPT and/or CAP-FEIA | Atopy/IgE–OME meta-analysis |
| Martines et al., 2010 [17] | Italy | School cross-sectional screening | 310 primary school children aged 5–6 years | Atopy by SPT | OME | OME by pneumatic otoscopy, type B/C tympanogram, absent acoustic reflex and conductive hearing loss | Atopy/IgE–OME meta-analysis |
| Ma et al., 2020 [19] | China | Prospective controlled cross-sectional study with treatment follow-up | 59 adults with house dust mite allergic rhinitis and 59 controls | House dust mite allergic rhinitis | ETD/middle-ear dysfunction | ETDQ-7, tympanography, nasal endoscopy and tubomanometry | ETD narrative synthesis |
| Adams et al., 2023 [20] | USA | NHANES cross-sectional | Adolescents aged 12–19 years | Allergic and non-allergic rhinitis | ETD-related history and tympanometry | Serum IgE, rhinitis classification, tympanometry and otologic history | ETD narrative synthesis |
| Alles et al., 2001 [21] | United Kingdom | Referral-clinic observational study | 209 children aged 3–8 years with chronic/recurrent OME | Atopic disorders/allergic rhinitis | Chronic/recurrent OME | Allergy history, examination, nasal smear and SPT | Qualitative synthesis only |
| Bemanian et al., 2020 [22] | Iran | Prospective cross-sectional/treatment-response study | 122 children with adenoid hypertrophy and/or OME | Atopy/allergic symptoms | AHT and OME symptoms | OME by otoscopy, audiometry and tympanometry; allergy assessment by symptoms, IgE and SPT in selected patients | Qualitative synthesis only |
| Kaymakçı et al., 2015 [23] | Turkey | Prospective controlled study | 33 atopic adults and 30 non-atopic controls | Atopy | Abnormal tympanometry/mastoid pneumatization | Atopy by SPT; tympanometry and 3D temporal CT mastoid volume measurement | Secondary qualitative ETD/middle-ear dysfunction synthesis |
| Norhafizah et al., 2020 [24] | Malaysia | Observational study | Children with OME | Allergic rhinitis | OME | Otologic and audiologic assessment as reported | Qualitative synthesis only |
| Hurst, 1996 [25] | USA | Mechanistic/clinical observational study | Patients with persistent OME | Atopy/allergy | OME and middle-ear inflammation | Skin testing, effusion markers and mucosal biopsy assessment | Mechanistic qualitative synthesis |
| Boedts et al., 1984 [26] | Belgium | Mechanistic observational study | Patients with OME/secretory otitis media | Atopic allergy/IgE | Middle-ear effusion | IgE assessment in effusion and serum | Mechanistic qualitative synthesis |
| Knight et al., 1992 [27] | USA | Seasonal exposure study | Patients with seasonal allergic rhinitis | Seasonal allergic rhinitis/pollen exposure | ETD/middle-ear pressure | Eustachian tube function and middle-ear pressure assessment | ETD qualitative synthesis |
| Osur et al., 1989 [28] | USA | Small seasonal exposure study | Children with ragweed hay fever | Ragweed allergic rhinitis | ETD | Eustachian tube obstruction/function assessment | ETD qualitative synthesis |
| Tomonaga et al., 1988 [29] | Japan | Clinical observational study | Children with OME, nasal allergy, and community controls | Nasal allergy diagnosed using clinical examination and multiple allergy tests | OME, tympanometric abnormalities, and Eustachian tube function | Otoscopy, audiometry, tympanometry, allergy testing, and Eustachian tube function tests | Narrative synthesis only; overlapping 1987 report excluded |
| Study | Analysis | Exposure | Outcome | a | b | c | d | OR | 95% CI | Weight RE (%) | Use/Caveat |
|---|---|---|---|---|---|---|---|---|---|---|---|
| Pau & Ng 2016 [9] | Primary AR/rhinitis–OME | Allergic rhinitis | OME | 12 | 147 | 3 | 182 | 4.95 | 1.37–17.88 | 14.7 | Patient-level full text |
| Fasunla et al., 2017 [10] | Primary AR/rhinitis–OME | Allergic rhinitis | OME | 39 | 47 | 8 | 78 | 8.09 | 3.48–18.79 | 19.7 | Patient-level full text |
| Sharifian et al., 2019 [11] | Primary AR/rhinitis–OME | Allergic rhinitis | OME | 9 | 3 | 28 | 49 | 5.25 | 1.31–21.01 | 13.6 | Case–control full text |
| Caffarelli et al., 1998 [12] | Primary AR/rhinitis–OME | Allergic rhinitis/rhinitis symptoms | OME | 28 | 11 | 144 | 189 | 3.34 | 1.61–6.94 | 21.1 | SPT positivity not pooled as AR |
| Yeo et al., 2007 [13] | Primary AR/rhinitis–OME | Allergic rhinitis | Chronic OME | 35 | 34 | 88 | 107 | 1.25 | 0.72–2.17 | 23.2 | Counts explicitly reported; non-significant study-level association. |
| Kayhan et al., 2002 [14] | Primary AR/rhinitis–OME | Allergic rhinitis | OME | 5 | 1 | 17 | 20 | 5.88 | 0.62–55.38 | 7.6 | Small study |
| Pooled random-effects | Primary AR/rhinitis–OME | - | - | - | - | - | - | 3.73 | 1.79–7.74 | - | I2 = 69.7%; p < 0.001 |
| Adekanye et al., 2024 [15] | Expanded sensitivity AR/rhinitis–OME | Clinically defined allergic rhinitis | OME | 12 | 33 | 32 | 243 | 2.76 | 1.30–5.88 | - | Added in expanded sensitivity; adjusted association not significant |
| Pooled random-effects incl. Adekanye | Expanded sensitivity AR/rhinitis–OME | - | - | - | - | - | - | 3.46 | 1.92–6.23 | - | I2 = 63.7%; p < 0.001 |
| Chantzi et al., 2006 [16] | Exploratory atopy/IgE–OME | IgE sensitization | OME | 28 | 12 | 60 | 68 | 2.64 | 1.24–5.66 | 49.7 | SPT and/or CAP-FEIA; adjusted OR 2.52 |
| Martines et al., 2010 [17] | Exploratory atopy/IgE–OME | Atopy by SPT | OME | 24 | 32 | 16 | 238 | 11.16 | 5.36–23.20 | 50.3 | School screening; objective OME criteria |
| Pooled random-effects | Exploratory atopy/IgE–OME | - | - | - | - | - | - | 5.45 | 1.33–22.35 | - | I2 = 86.0%; p = 0.018 |
| Study | JBI Appraisal Tool | Key Methodological Limitations | Overall Risk of Bias |
|---|---|---|---|
| Pau and Ng, 2016 [9] | JBI Analytical Cross-Sectional | Allergic rhinitis was assessed mainly using clinical symptoms and questionnaire-based criteria; no multivariable adjustment was performed. | Moderate |
| Fasunla et al., 2017 [10] | JBI Case–Control | Cases and controls were recruited from different source settings; no adjusted analysis for relevant confounders was reported. | Moderate |
| Sharifian et al., 2019 [11] | JBI Case–Control | Small, selected sample; allergy testing was not uniformly applied to all participants; no multivariable adjustment was performed. | High |
| Caffarelli et al., 1998 [12] | JBI Case–Control | Referral-clinic cases and school-based controls differed in source population and age distribution; no adjusted analysis was reported. | Moderate-to-high |
| Yeo et al., 2007 [13] | JBI Case–Control | Chronic OME cases were referral-based and selected for ventilation tube insertion; no multivariable adjustment was performed. | Moderate |
| Kayhan et al., 2002 [14] | JBI Case–Control | Very small sample; allergy testing was applied selectively; methodological reporting and control of confounding were limited. | High |
| Adekanye et al., 2024 [15] | JBI Analytical Cross-Sectional | Allergic rhinitis was defined using symptom- and history-based criteria without objective sensitization testing; the adjusted association was not statistically significant. | Moderate |
| Chantzi et al., 2006 [16] | JBI Case–Control | Controls were hospital-based, although groups were matched, exposure and outcome assessment were objective, and multivariable adjustment was performed. | Low |
| Martines et al., 2010 [17] | JBI Analytical Cross-Sectional | Atopy and OME were objectively assessed, but no adjustment for relevant confounders was reported. | Moderate |
| Kreiner-Møller et al., 2012 [18] | JBI Analytical Cross-Sectional analysis within a prospective birth cohort | The cohort included children born to mothers with asthma, which may limit generalizability; some participants had missing or inconclusive OME assessments. | Low |
| Study | AR/Atopy Definition and Objective Assessment | OME Definition and Assessment | Estimate Used | Main Potential Source of Heterogeneity |
|---|---|---|---|---|
| Pau and Ng, 2016 [9] | AR identified from compatible nasal symptoms using the ARIR questionnaire; no systematic SPT or specific-IgE confirmation. | Pneumatic otoscopy and portable tympanometry. | Crude 2 × 2 estimate. | Symptom/questionnaire-based AR definition and no multivariable adjustment. |
| Fasunla et al., 2017 [10] | Watery rhinorrhea plus ≥ 1 additional nasal symptom for ≥3–4 weeks; nasal cytology with ≥5 eosinophils/high-power field; no systematic SPT or specific IgE. | Jerger tympanometry; type B and C patterns considered compatible with OME. | Crude 2 × 2 estimate. | Broader OME definition including type C and AR confirmation based on nasal eosinophilia rather than allergen-specific testing. |
| Sharifian et al., 2019 [11] | Clinical AR diagnosis; SPT in all OME cases but only in controls suspected of AR; total IgE, blood eosinophils, and nasal cytology also assessed. | Otoscopy and/or type B tympanogram; persistent/recurrent OME or ventilation-tube candidates. | Crude 2 × 2 estimate. | Differential allergy testing and selection of more severe OME cases. |
| Caffarelli et al., 1998 [12] | Rhinitis and atopic symptoms assessed by questionnaire and clinical examination; SPT performed in all participants. | Clinical glue ear plus type B or C tympanograms; controls had type A and no OME history. | Crude estimate for clinical rhinitis; SPT positivity not pooled as AR. | Referral cases versus school controls, age imbalance, and inclusion of type C tympanograms. |
| Yeo et al., 2007 [13] | Compatible nasal symptoms plus positive MAST-CLA and/or skin testing; nasal provocation performed in the AR group. | Chronic OME by otoscopy and type B or C tympanometry; cases underwent ventilation-tube insertion. | Crude 2 × 2 estimate. | Selected surgical chronic-OME cohort, inclusion of type C, and no confounder adjustment. |
| Kayhan et al., 2002 [14] | AR based on rhinitis symptoms, total IgE, SPT, and nasal smear; SPT/smear used only in children with raised IgE or recurrent symptoms. | Physical examination and tympanometry. | Crude 2 × 2 estimate. | Selective allergy work-up, very small sample, and limited reporting. |
| Adekanye et al., 2024 [15] | At least two nasal/ocular symptoms plus personal/family allergy history or asthma; no SPT or specific-IgE confirmation. | Otoscopy and tympanometry in a community sample. | Crude estimate in sensitivity analysis; adjusted OR interpreted narratively. | Broad symptom/history-based AR definition; association weakened after adjustment for age and sex. |
| Chantzi et al., 2006 [16] | Primary exposure was IgE sensitization; respiratory allergy symptoms used standardized definitions; SPT and/or CAP-FEIA performed. | Symptoms, otoscopy, and type B or C tympanometry; duration > 1 month or recurrent OME. | Crude 2 × 2 estimate pooled; adjusted OR interpreted narratively. | Objective sensitization but broader type B/C OME definition and hospital-based controls. |
| Martines et al., 2010 [17] | Atopy defined by positive SPT during school screening. | Persistent effusion ≥ 3 months plus pneumatic otoscopy, type B/C tympanogram, absent acoustic reflex, and conductive hearing loss > 25 dB. | Crude 2 × 2 estimate. | Strict composite OME definition but no adjustment for confounders. |
| Kreiner-Møller et al., 2012 [18] | AR required symptoms, specific-IgE sensitization, and relevant allergen exposure; non-allergic rhinitis and asymptomatic sensitization analyzed separately. | Otoscopy plus type B or C2 tympanogram (<−200 dPa); children with tubes classified as OME. | Adjusted OR used for narrative sensitivity interpretation. | Most specific AR definition and extensive adjustment, but high-risk birth cohort and broader OME classification including C2/tubes. |
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Petre, A.-M.; Costin, R.; Anghel, I. Allergic Rhinitis and Allergic Sensitization in Pediatric Otitis Media with Effusion: A Systematic Review and Meta-Analysis with Narrative Synthesis of Eustachian Tube Dysfunction. Children 2026, 13, 892. https://doi.org/10.3390/children13070892
Petre A-M, Costin R, Anghel I. Allergic Rhinitis and Allergic Sensitization in Pediatric Otitis Media with Effusion: A Systematic Review and Meta-Analysis with Narrative Synthesis of Eustachian Tube Dysfunction. Children. 2026; 13(7):892. https://doi.org/10.3390/children13070892
Chicago/Turabian StylePetre, Alina-Mihaela, Romeo Costin, and Ion Anghel. 2026. "Allergic Rhinitis and Allergic Sensitization in Pediatric Otitis Media with Effusion: A Systematic Review and Meta-Analysis with Narrative Synthesis of Eustachian Tube Dysfunction" Children 13, no. 7: 892. https://doi.org/10.3390/children13070892
APA StylePetre, A.-M., Costin, R., & Anghel, I. (2026). Allergic Rhinitis and Allergic Sensitization in Pediatric Otitis Media with Effusion: A Systematic Review and Meta-Analysis with Narrative Synthesis of Eustachian Tube Dysfunction. Children, 13(7), 892. https://doi.org/10.3390/children13070892

