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心脏基质和整合素的年龄相关变化。

Age-associated changes in cardiac matrix and integrins.

作者信息

Burgess M L, McCrea J C, Hedrick H L

机构信息

Department of Health Sciences, Laboratory of Cardiovascular Biology, Boston University, 635 Commonwealth Avenue, Boston, MA 02215, USA.

出版信息

Mech Ageing Dev. 2001 Oct;122(15):1739-56. doi: 10.1016/s0047-6374(01)00296-2.

Abstract

The progressive shift from young age to senescence is characterized by structural and functional changes in the cardiac extracellular matrix (ECM), which supports and aligns myocytes and blood vessels, and maintains myocardial mass, structure and function. As cardiac function declines with advancing age, ECM collagen and fibronectin influence diastolic stiffness. ECM binding to membrane-bound receptors, or integrins, directly links ECM to cardiac muscle and fibroblast cells, affording it the permissive role to modulate heart function. To better understand the ECM structure-function relationship in the old heart, we studied the relative protein content of these ECM proteins and integrins across three age groups. Old Balb-c mice (20 months) exhibit biventricular, cardiac hypertrophy, and greater left ventricular (LV) collagen, fibronectin, alpha 1 and alpha 5 integrin protein than middle-aged (12 months) or young (2 months) LV (P<0.05). beta1 integrin protein content is lower in old LV (P<0.05). These data show that advancing age is associated with greater collagen, fibronectin, alpha 1 and alpha 5 integrin content, suggesting that these matrix proteins undergo coordinated regulation in the aging heart. The differential integrin and ECM protein content suggests that there is regulatory signaling to the fibroblasts, which maintain the cardiac ECM.

摘要

从年轻到衰老的渐进转变的特征是心脏细胞外基质(ECM)的结构和功能变化,心脏细胞外基质支撑并排列心肌细胞和血管,并维持心肌质量、结构和功能。随着心脏功能随着年龄增长而下降,ECM胶原蛋白和纤连蛋白会影响舒张期硬度。ECM与膜结合受体或整合素的结合直接将ECM与心肌细胞和成纤维细胞联系起来,使其具有调节心脏功能的许可作用。为了更好地理解老年心脏中ECM的结构-功能关系,我们研究了这三种ECM蛋白和整合素在三个年龄组中的相对蛋白含量。老年Balb-c小鼠(20个月)表现出双心室心肌肥大,且左心室(LV)胶原蛋白、纤连蛋白、α1和α5整合素蛋白含量高于中年(12个月)或年轻(2个月)的左心室(P<0.05)。老年左心室中β1整合素蛋白含量较低(P<0.05)。这些数据表明,年龄增长与胶原蛋白、纤连蛋白、α1和α5整合素含量增加有关,这表明这些基质蛋白在衰老心脏中受到协同调节。整合素和ECM蛋白含量的差异表明,存在对维持心脏ECM的成纤维细胞的调节信号。

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