Department of Cardiology, the Second Xiangya Hospital, Central South University, Changsha, Hunan, China.
Cell Death Dis. 2020 Nov 26;11(11):1014. doi: 10.1038/s41419-020-03211-4.
The prognostic impact of extracellular matrix (ECM) modulation and its regulatory mechanism post-acute myocardial infarction (AMI), require further clarification. Herein, we explore the predictive role of legumain-which showed the ability in ECM degradation-in an AMI patient cohort and investigate the underlying mechanisms. A total of 212 AMI patients and 323 healthy controls were enrolled in the study. Moreover, AMI was induced in mice by permanent ligation of the left anterior descending artery and fibroblasts were adopted for mechanism analysis. Based on the cut-off value for the receiver-operating characteristics curve, AMI patients were stratified into low (n = 168) and high (n = 44) plasma legumain concentration (PLG) groups. However, PLG was significantly higher in AMI patients than that in the healthy controls (median 5.9 μg/L [interquartile range: 4.2-9.3 μg/L] vs. median 4.4 μg/L [interquartile range: 3.2-6.1 μg/L], P < 0.001). All-cause mortality was significantly higher in the high PLG group compared to that in the low PLG group (median follow-up period, 39.2 months; 31.8% vs. 12.5%; P = 0.002). Multivariate Cox regression analysis showed that high PLG was associated with increased all-cause mortality after adjusting for clinical confounders (HR = 3.1, 95% confidence interval (CI) = 1.4-7.0, P = 0.005). In accordance with the clinical observations, legumain concentration was also increased in peripheral blood, and infarcted cardiac tissue from experimental AMI mice. Pharmacological blockade of legumain with RR-11a, improved cardiac function, decreased cardiac rupture rate, and attenuated left chamber dilation and wall thinning post-AMI. Hence, plasma legumain concentration is of prognostic value in AMI patients. Moreover, legumain aggravates cardiac remodelling through promoting ECM degradation which occurs, at least partially, via activation of the MMP-2 pathway.
细胞外基质 (ECM) 调节的预后影响及其在急性心肌梗死 (AMI) 后的调节机制,需要进一步阐明。在此,我们研究了组织蛋白酶 L(一种具有 ECM 降解能力的酶)在 AMI 患者队列中的预测作用,并探讨了其潜在机制。共纳入 212 例 AMI 患者和 323 例健康对照者。此外,通过结扎左前降支诱导小鼠 AMI,并采用成纤维细胞进行机制分析。基于受试者工作特征曲线的截断值,将 AMI 患者分为低(n = 168)和高(n = 44)血浆组织蛋白酶 L 浓度(PLG)组。然而,AMI 患者的 PLG 显著高于健康对照组(中位数 5.9μg/L [四分位距:4.2-9.3μg/L] 比中位数 4.4μg/L [四分位距:3.2-6.1μg/L],P < 0.001)。高 PLG 组的全因死亡率明显高于低 PLG 组(中位随访时间 39.2 个月;31.8%比 12.5%;P = 0.002)。多变量 Cox 回归分析显示,在校正临床混杂因素后,高 PLG 与全因死亡率增加相关(HR = 3.1,95%置信区间 [CI] = 1.4-7.0,P = 0.005)。与临床观察一致,实验性 AMI 小鼠的外周血和梗死心肌组织中组织蛋白酶 L 浓度也升高。用 RR-11a 抑制组织蛋白酶 L 可改善心功能,降低心脏破裂率,并减轻 AMI 后左心室扩张和壁变薄。因此,PLG 浓度对 AMI 患者具有预后价值。此外,组织蛋白酶 L 通过促进 ECM 降解加重心肌重构,至少部分通过激活 MMP-2 途径。
