Song Lei, Wang Lai, Li Fuqiang, Yukht Ada, Qin Minghui, Ruther Haley, Yang Mingjie, Chaux Aurelio, Shah Prediman K, Sharifi Behrooz G
Oppenheimer Atherosclerosis Research Center, Cedars Sinai Heart Institute, Los Angeles, California.
Oppenheimer Atherosclerosis Research Center, Cedars Sinai Heart Institute, Los Angeles, California.
J Am Coll Cardiol. 2017 Sep 26;70(13):1601-1615. doi: 10.1016/j.jacc.2017.07.789.
Tenascin-C (TNC) is a highly conserved matricellular protein with a distinct expression pattern during development and disease. Remodeling of the left ventricle (LV) in response to pressure overload leads to the re-expression of the fetal gene program.
The aim of this study was to investigate the function of TNC in cardiac hypertrophy in response to pressure overload.
Pressure overload was induced in TNC knockout and wild-type mice by constricting their abdominal aorta or by infusion of angiotensin II. Echocardiography, immunostaining, flow cytometry, quantitative real-time polymerase chain reaction, and reciprocal bone marrow transplantation were used to evaluate the effect of TNC deficiency.
Echocardiographic analysis of pressure overloaded hearts revealed that all LV parameters (LV end-diastolic and -systolic dimensions, ejection fraction, and fractional shortening) deteriorated in TNC-deficient mice compared with their wild-type counterparts. Cardiomyocyte size and collagen accumulation were significantly greater in the absence of TNC. Mechanistically, TNC deficiency promoted rapid accumulation of the CCR2/Ly6C monocyte/macrophage subset into the myocardium in response to pressure overload. Further, echocardiographic and immunohistochemical analyses of recipient hearts showed that expression of TNC in the bone marrow, but not the myocardium, protected the myocardium against excessive remodeling of the pressure-overloaded heart.
TNC deficiency further impaired cardiac function in response to pressure overload and exacerbated fibrosis by enhancing inflammation. In addition, expression of TNC in the bone marrow, but not the myocardium, protected the myocardium against excessive remodeling in response to mild pressure overload.
腱生蛋白-C(TNC)是一种高度保守的基质细胞蛋白,在发育和疾病过程中具有独特的表达模式。左心室(LV)对压力过载的重塑会导致胎儿基因程序的重新表达。
本研究旨在探讨TNC在压力过载引起的心脏肥大中的作用。
通过缩窄腹主动脉或输注血管紧张素II,在TNC基因敲除小鼠和野生型小鼠中诱导压力过载。采用超声心动图、免疫染色、流式细胞术、定量实时聚合酶链反应和相互骨髓移植来评估TNC缺乏的影响。
对压力过载心脏的超声心动图分析显示,与野生型小鼠相比,TNC缺陷小鼠的所有左心室参数(左心室舒张末期和收缩末期内径、射血分数和缩短分数)均恶化。在缺乏TNC的情况下,心肌细胞大小和胶原蛋白积累明显增加。机制上,TNC缺乏促进了CCR2/Ly6C单核细胞/巨噬细胞亚群在压力过载时迅速积聚到心肌中。此外,对受体心脏的超声心动图和免疫组织化学分析表明,骨髓而非心肌中的TNC表达可保护心肌免受压力过载心脏的过度重塑。
TNC缺乏会进一步损害压力过载时的心脏功能,并通过增强炎症反应加剧纤维化。此外,骨髓而非心肌中的TNC表达可保护心肌免受轻度压力过载引起的过度重塑。