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Genetic and Epigenetic Programming of Allergic Airway Inflammation

$618,598R01FY2015AINIH

Boston Children'S Hospital, Boston MA

Investigators

Linked publications, trials & patents

Abstract

DESCRIPTION (provided by applicant): The Interaction of environmental factors with asthma susceptibility genes plays a fundamental role in the genesis and persistence of the asthma epidemic. Particularly important in this process are allelic variants along the IL-4/IL-13/IL-4 receptor axis, which have been linked to distinct asthma phenotypes. Many of the mechanisms by which these alleles exert their functions are unclear, including the proximal signaling events involved, the consequent genetic and epigenetic responses underlying disease chronicity, and their interface with environmental influences in programming allergic diseases. By employing incisive genetic mouse models, we have established a causative link between Il4ra alleles and atopy and asthma. More recently, we have also established that a human polymorphism, IL-4RaQ576R, which associates with severe and fatal/near fatal asthma, enables a novel Stat6-independent pathway involving MAP kinases (MAPKs) that, in synergy with Stat6, promotes severe allergic airway inflammation and remodeling. Our recent studies reveal that IL-13- induced allergic airway inflammation associates with an epigenetic methylation signature that may contribute to inflammation, airway remodeling and disease chronicity. These signaling, genetic and epigenetic events are themselves subject to environmental influences, as revealed by preliminary studies showing synergy between the Il4raR576 allele and diesel exhaust particles (DEP) in allergic inflammation. Based on the above, we hypothesize that severe asthma-associated Il4raR576 allele mobilizes a mechanistically distinct signaling pathway that mediates the allele's exaggerated allergic inflammatory and tissue remodeling attributes. Furthermore, we hypothesize that Il4ra signaling imparts an epigenetic signature that contributes to airway remodeling and disease chronicity. Finally, we hypothesize that DEP act synergistically with Il4raR576 by mechanisms involving the oxidative stress response and the Notch pathway. These hypotheses will be validated using a combination of molecular, cellular and whole animal approaches. Our studies address fundamental attributes of gene/environment interaction in asthma, promise novel insights into disease pathogenesis and chronicity and new approaches to therapy.

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