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Macrophage CARD9 mediates cardiac injury following myocardial infarction through regulation of lipocalin 2 expression 被引量:1

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摘要 Immune cell infiltration in response to myocyte death regulates extracellular matrix remodeling and scar formation after myocardial infarction(MI).Caspase-recruitment domain family member 9(CARD9)acts as an adapter that mediates the transduction of pro-inflammatory signaling cascades in innate immunity;however,its role in cardiac injury and repair post-MI remains unclear.We found that Card9 was one of the most upregulated Card genes in the ischemic myocardium of mice.CARD9 expression increased considerably 1 day post-MI and declined by day 7 post-MI.Moreover,CARD9 was mainly expressed in F4/80-positive macrophages.Card9 knockout(KO)led to left ventricular function improvement and infarct scar size reduction in mice 28 days post-MI.Additionally,Card9 KO suppressed cardiomyocyte apoptosis in the border region and attenuated matrix metalloproteinase(MMP)expression.RNA sequencing revealed that Card9 KO significantly suppressed lipocalin 2(Lcn2)expression post-MI.Both LCN2 and the receptor solute carrier family 22 member 17(SL22A17)were detected in macrophages.Subsequently,we demonstrated that Card9 overexpression increased LCN2 expression,while Card9 KO inhibited necrotic cell-induced LCN2 upregulation in macrophages,likely through NF-κB.Lcn2 KO showed beneficial effects post-MI,and recombinant LCN2 diminished the protective effects of Card9 KO in vivo.Lcn2 KO reduced MMP9 post-MI,and Lcn2 overexpression increased Mmp9 expression in macrophages.Slc22a17 knockdown in macrophages reduced MMP9 release with recombinant LCN2 treatment.In conclusion,our results demonstrate that macrophage CARD9 mediates the deterioration of cardiac function and adverse remodeling post-MI via LCN2.
出处 《Signal Transduction and Targeted Therapy》 SCIE CSCD 2023年第11期5383-5393,共11页 信号转导与靶向治疗(英文)
基金 National Natural Science Foundation of China(grant numbers 81300120,81770250 to Y.L 81790622 and 81430050 to J.D.) Bejing Natural Science Foundation(grant number Z200026 to C.Z.).
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