NOX4 promotes Kupffer cell inflammatory response via ROS-NLRP3 to aggravate liver inflammatory injury in acute liver injury

Liping Zhai; Hongyan Pei; Yi Yang; Yu Zhu; Shuiliang Ruan

doi:doi:10.18632/aging.204173

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Research Paper Volume 14, Issue 17 pp 6905—6916

NOX4 promotes Kupffer cell inflammatory response via ROS-NLRP3 to aggravate liver inflammatory injury in acute liver injury

Figure 3. Suppressing NOX4 inhibits inflammatory response and injury in KCs. (A, B) Results of FCM assay (n = 3). The cell apoptosis level in L/N + GKT group significantly decreased, lower than that in L/N group. ^*P < 0.05, compared with Con group; ^#P < 0.05, compared with L/N group. (C) IF staining (n = 3). GKT suppressed NLRP3 inflammasome activation. The expression levels of NLRP3 and ASC evidently decreased, lower than those in L/N group. (D) ROS detection by DCFH-DA probe (n = 3). GKT inhibited ROS expression, and the number of positive cells markedly decreased, lower than that in L/N group.