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Synergy of Atopy and Airway Dysbiosis Promotes IL-5 Expression and Asthma Persistence in Children
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  • Łukasz Dobrakowski,
  • Piotr Lacwik,
  • Marta Mucha,
  • Błażej Rychlik ,
  • Andrzej Błauż ,
  • Michał Seweryn,
  • Dominik Strapagiel,
  • Joanna Majak,
  • Wojciech Feleszko,
  • Adam Antczak,
  • Piotr Kuna,
  • Paweł Majak
Łukasz Dobrakowski
Uniwersytet Medyczny w Lodzi
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Piotr Lacwik
Uniwersytet Jana Kochanowskiego w Kielcach Collegium Medicum

Corresponding Author:[email protected]

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Marta Mucha
Uniwersytet Medyczny w Lodzi
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Błażej Rychlik
Uniwersytet Lodzki
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Andrzej Błauż
Uniwersytet Lodzki
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Michał Seweryn
Uniwersytet Lodzki
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Dominik Strapagiel
Uniwersytet Lodzki
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Joanna Majak
Regional Center of Occupational Medicine
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Wojciech Feleszko
Warszawski Uniwersytet Medyczny
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Adam Antczak
Uniwersytet Medyczny w Lodzi
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Piotr Kuna
Uniwersytet Medyczny w Lodzi
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Paweł Majak
Uniwersytet Medyczny w Lodzi
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Abstract

Background: Recent studies increasingly suggest that airway microbiome plays a critical role in respiratory health and disease, including the potential influence on the development and persistence of asthma in children. This study aims to evaluate the clinical, immunological, and microbiological factors contributing to the persistence of asthma from preschool to school age. Methods: 183 children aged 4-8 years with chronic rhinosinusitis were enrolled in the study, including 82 children (62%) with asthma. Nasopharynx swabs were collected for microbiome analysis using next-generation sequencing methods, and nasal mucosa samples were taken to analyze mRNA expressions of predefined cytokines and innate lymphoid cells (ILCs). Out of the initial cohort, 117 children, including 74 with asthma, remained under observation for the next five years to assess asthma persistence Results: After 5 years asthma persisted in 23% (17 of 74) of patients. A multivariate model of logistic regression analysis revealed that asthma persistence was independently associated with atopy (OR=8.5, 95%CI: 1.7-43) and reduced biodiversity in the upper airway microbiome (OR=6.0, 95%CI: 1.7-22). Additionally, higher nasal expression of TSLP which correlated with IL-5 was observed in children with reduced biodiversity. In children with both atopy and reduced biodiversity higher nasal expression of IL-5 was detected, with the highest risk of persistent asthma. Conclusion: Reduced biodiversity concomitant with atopy is associated with increased risk of asthma persistence. This interaction is associated with higher nasal expression of IL-5. These findings identify new potential targets for the prevention of persistent asthma in children