CD36是一种基质金属蛋白酶-9底物,在心脏重构过程中刺激中性粒细胞凋亡和清除

K. DeLeon-Pennell, Yuan Tian, Bai Zhang, Courtney A. Cates, R. Iyer, Presley L. Cannon, Punit Shah, P. Aiyetan, G. Halade, Yonggang Ma, Elizabeth R. Flynn, Zhen Zhang, Yu-Fang Jin, Hui Zhang, M. Lindsey
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引用次数: 68

摘要

背景:心肌梗死后,左心室经历伤口愈合反应,包括中性粒细胞和巨噬细胞的强大浸润,以促进死亡肌细胞的清除以及细胞外基质的周转。基质金属蛋白酶(MMP)-9是调控心肌梗死后左室重构的关键酶。方法和结果:糖蛋白组学分析野生型和MMP-9缺失小鼠(每组8只)的梗死区域结果显示,在541个n -糖基化蛋白中,有45个蛋白在MMP-9缺失的情况下上调或下调2倍以上(均P<0.05)。软骨中间层蛋白和血小板糖蛋白4 (CD36)在MMP-9缺失小鼠中增加的倍数最高。免疫印迹法发现,在心肌梗死后的时间过程中,软骨中间层蛋白CD36而非软骨中间层蛋白稳定下降,这表明CD36是MMP-9的候选底物。体外和体内均证实MMP-9具有蛋白水解降解CD36的作用。用MMP-9或cd36阻断肽体外刺激心肌梗死后第7天的巨噬细胞可降低吞噬能力。双免疫荧光显示,与野生型组相比,MMP-9无效组伴有凋亡中性粒细胞的积累。用MMP-9体外刺激分离的中性粒细胞,通过降低caspase-9的表达,可以减少中性粒细胞的凋亡。结论-我们的数据揭示了MMP-9通过CD36降解调节巨噬细胞吞噬和中性粒细胞凋亡的新的细胞信号作用。
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CD36 Is a Matrix Metalloproteinase-9 Substrate That Stimulates Neutrophil Apoptosis and Removal During Cardiac Remodeling
Background—After myocardial infarction, the left ventricle undergoes a wound healing response that includes the robust infiltration of neutrophils and macrophages to facilitate removal of dead myocytes as well as turnover of the extracellular matrix. Matrix metalloproteinase (MMP)-9 is a key enzyme that regulates post-myocardial infarction left ventricular remodeling. Methods and Results—Infarct regions from wild-type and MMP-9 null mice (n=8 per group) analyzed by glycoproteomics showed that of 541 N-glycosylated proteins quantified, 45 proteins were at least 2-fold upregulated or downregulated with MMP-9 deletion (all P<0.05). Cartilage intermediate layer protein and platelet glycoprotein 4 (CD36) were identified as having the highest fold increase in MMP-9 null mice. By immunoblotting, CD36 but not cartilage intermediate layer protein decreased steadily during the time course post-myocardial infarction, which identified CD36 as a candidate MMP-9 substrate. MMP-9 was confirmed in vitro and in vivo to proteolytically degrade CD36. In vitro stimulation of day 7 post-myocardial infarction macrophages with MMP-9 or a CD36-blocking peptide reduced phagocytic capacity. Dual immunofluorescence revealed concomitant accumulation of apoptotic neutrophils in the MMP-9 null group compared with wild-type group. In vitro stimulation of isolated neutrophils with MMP-9 decreased neutrophil apoptosis, indicated by reduced caspase-9 expression. Conclusions—Our data reveal a new cell-signaling role for MMP-9 through CD36 degradation to regulate macrophage phagocytosis and neutrophil apoptosis.
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来源期刊
Circulation-Cardiovascular Genetics
Circulation-Cardiovascular Genetics CARDIAC & CARDIOVASCULAR SYSTEMS-GENETICS & HEREDITY
CiteScore
3.95
自引率
0.00%
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0
期刊介绍: Circulation: Genomic and Precision Medicine considers all types of original research articles, including studies conducted in human subjects, laboratory animals, in vitro, and in silico. Articles may include investigations of: clinical genetics as applied to the diagnosis and management of monogenic or oligogenic cardiovascular disorders; the molecular basis of complex cardiovascular disorders, including genome-wide association studies, exome and genome sequencing-based association studies, coding variant association studies, genetic linkage studies, epigenomics, transcriptomics, proteomics, metabolomics, and metagenomics; integration of electronic health record data or patient-generated data with any of the aforementioned approaches, including phenome-wide association studies, or with environmental or lifestyle factors; pharmacogenomics; regulation of gene expression; gene therapy and therapeutic genomic editing; systems biology approaches to the diagnosis and management of cardiovascular disorders; novel methods to perform any of the aforementioned studies; and novel applications of precision medicine. Above all, we seek studies with relevance to human cardiovascular biology and disease. Manuscripts are examined by the editorial staff and usually evaluated by expert reviewers assigned by the editors. Both clinical and basic articles will also be subject to statistical review, when appropriate. Provisional or final acceptance is based on originality, scientific content, and topical balance of the journal. Decisions are communicated by email, generally within six weeks. The editors will not discuss a decision about a manuscript over the phone. All rebuttals must be submitted in writing to the editorial office.
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