Myeloid-specific knockout of Notch-1 inhibits MyD88- and TRIF-mediated TLR signaling pathways by regulating oxidative stress-SHP2 axis, thus restraining aneurysm progression

Yu Li; Ailin Guo; Jianlei Liu; Lijuan Tang; Lide Su; Zonghong Liu

doi:doi:10.18632/aging.205392

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Research Paper Volume 16, Issue 2 pp 1182—1191

Myeloid-specific knockout of Notch-1 inhibits MyD88- and TRIF-mediated TLR signaling pathways by regulating oxidative stress-SHP2 axis, thus restraining aneurysm progression

Figure 5. Notch-1 deficiency inhibited the activation of MyD88/TRIF/NF-κB signals. (A) Macrophages’ deficiency of Notch-1 inhibited the phosphorylated-MyD88, TRIF, and NF-κB and there statistical data; (B) Notch-1 cKO decreased the expression of IFN-γ, IL-1β, TNF-α expression in AAA tested by western blot. N = 6, ^*P < 0.05, ^**P < 0.01, apoE-KO/Notch-1^MAC-KO group vs. apoE-KO/Notch-1^WT group.