Production of a p65 fl/fl /LysMCre mouse model with dysfunctional NF-κB signaling in bone marrow-derived macrophages.
Ahmet K KorkayaJeffrey FischerAnthony PeppersSean M CrossonManira RayamajhiEdward A MiaoAlbert S BaldwinJennifer W BradfordPublished in: Innate immunity (2023)
Here, we describe the production and characterization of a novel p65 fl/fl /LysMCre mouse model, which lacks canonical nuclear factor-kappaB member RelA/p65 (indicated as p65 hereafter) in bone marrow-derived macrophages. Cultured bone marrow-derived macrophages that lack p65 protein reveal NF-κB signaling deficiencies, a reduction in phagocytic ability, and reduced ability to produce nitrites. Despite abnormal bone marrow-derived macrophage function, p65 fl/fl /LysMCre mice do not exhibit differences in naïve systemic immune profiles or colony forming units and time to death following Salmonella infection as compared to controls. Additionally, p65 fl/fl /LysMCre mice, especially females, display splenomegaly, but no other obvious physical or behavioral differences as compared to control animals. As bone marrow-derived macrophages from this transgenic model are almost completely devoid of canonical nuclear factor-kappaB pathway member p65, this model has the potential for being very useful in investigating bone marrow-derived macrophage NF-kappaB signaling in diverse biological and biomedical studies.
Keyphrases
- nuclear factor
- toll like receptor
- mouse model
- mesenchymal stem cells
- signaling pathway
- escherichia coli
- lps induced
- adipose tissue
- type diabetes
- oxidative stress
- pi k akt
- immune response
- mental health
- metabolic syndrome
- endothelial cells
- gene expression
- single cell
- climate change
- dna methylation
- insulin resistance
- human health
- bone marrow
- binding protein
- amino acid