Differential regulation of interferon signaling pathways in CD4+ t cells of the low type-2 obesity-associated asthma phenotype

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Abstract

In the era of personalized medicine, insights into the molecular mechanisms that differ-entially contribute to disease phenotypes, such as asthma phenotypes including obesity-associated asthma, are urgently needed. Peripheral blood was drawn from 10 obese, non-atopic asthmatic adults with a high body mass index (BMI; 36.67 ± 6.90); 10 non-obese, non-atopic asthmatic adults with normal BMI (23.88 ± 2.73); and 10 healthy controls with normal BMI (23.62 ± 3.74). All asthmatic patients were considered to represent a low type-2 asthma phenotype according to selective clinical parameters. RNA sequencing (RNA-Seq) was conducted on peripheral blood CD4+ T cells. Thou-sands of differentially expressed genes were identified in both asthma groups compared with heathy controls. The expression of interferon (IFN)-stimulated genes associated with IFN-related signaling pathways was specifically affected in obese asthmatics, while the gap junction and G pro-tein-coupled receptor (GPCR) ligand binding pathways were enriched in both asthma groups. Fur-thermore, obesity gene markers were also upregulated in CD4+ T cells from obese asthmatics compared with the two other groups. Additionally, the enriched genes of the three abovementioned pathways showed a unique correlation pattern with various laboratory and clinical parameters. The specific activation of IFN-related signaling and viral infection pathways might provide a novel view of the molecular mechanisms associated with the development of the low type-2 obesity-associated asthma phenotype, which is a step ahead in the development of new stratified therapeutic ap-proaches.

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Alhamdan, F., Marsh, L. M., Pedersen, F., Alhamwe, B. A., Thölken, C., Pfefferle, P. I., … Garn, H. (2021). Differential regulation of interferon signaling pathways in CD4+ t cells of the low type-2 obesity-associated asthma phenotype. International Journal of Molecular Sciences, 22(18). https://doi.org/10.3390/ijms221810144

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