Abstract
Background and Hypothesis: The pathogenesis of Bronchopulmonary Dysplasia (BPD) is multifactorial leading to inflammation. In BPD, Endothelial-Monocyte Activating Polypeptide II (EMAP II, encoded by Aimp1), a moonlighting pro-inflammatory cytokine, is initially found in bronchiolar club cells followed by intra-alveolar GAL-3+ macrophages. Sustained EMAP II mimics BPD, invoking inflammation, alveolar simplification, and macrophage recruitment. Targeted ablation of EMAP II in the recruited macrophages may dampen innate immune response. 
 Experimental Design: Gender-matched, aged-matched littermate mice with myeloid-cell specific ablation of Aimp1 (Lyz2-Cre;Aimp1flox/flox, denoted as Aimp1Δ/Δ) or without (control) were subjected to lipopolysaccharide (LPS)-endotoxemia. Survival rates of co-housed or singly housed mice were measured over 72 hours following a lethal dose (15 mg/kg). Clinical scores (0-6) based on the integrity of their locomotion, fur, and eyes were assigned every 2 hours. Blood and bone marrow smears, average bodyweights, spleen-weights to bodyweights and liver-weights to bodyweights were analyzed. 
 Results: There were no baseline differences in bodyweight, spleen weight:bodyweight, liver weight:bodyweight (p-val = 0.42, 0.46, 0.64). Representative bone marrow and blood smears showed no notable difference. Aimp1[Symbol]/[Symbol] male mice co-housed (dose 15 mg/kg) but not singly housed survived longer than their littermates (median survival: hours); Aimp1[Symbol]/[Symbol] female mice showed a survival advantage (median survival: hours) with lower clinical scores than their littermates. The kinetics of NFKBIA/I[Symbol]B degradation was similar between Aimp1[Symbol]/[Symbol] and control peritoneal macrophages in response to LPS, although there was a higher basal amount in Aimp1[Symbol]/[Symbol]. 
 Conclusion and Potential Impact: Aimp1/EMAP II does play a positive feedback role in innate immunity, potentially in a metabolically and gender-specific role of Aimp1 which remain to be explored.
Highlights
Background and HypothesisThe pathogenesis of Bronchopulmonary Dysplasia (BPD) is multifactorial leading to inflammation
The kinetics of NFKBIA/IkB degradation was similar between Aimp1D/D and control peritoneal macrophages in response to LPS, there was a higher basal amount in Aimp1D/D
Impact: Aimp1/EMAP II does play a positive feedback role in innate immunity, potentially in a metabolically and genderspecific role of Aimp1 which remain to be explored
Summary
Background and HypothesisThe pathogenesis of Bronchopulmonary Dysplasia (BPD) is multifactorial leading to inflammation. Kirsten Zborek1, Daniel Lee2,3,4, Adam Pajakowski2, Jacob Slack4, Joseph Park4, June Park4, Margaret Schwarz2,3,4 Indiana University School of Medicine1, Indiana University School of Medicine2, Department of Pediatrics, Department of Cellular and Integrative Physiology3
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