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机械力调节肺弹性蛋白中弹性蛋白酶的活性和结合位点的可及性。

Mechanical forces regulate elastase activity and binding site availability in lung elastin.

机构信息

Department of Biomedical Engineering, Boston University, Boston, Massachusetts, USA.

出版信息

Biophys J. 2010 Nov 3;99(9):3076-83. doi: 10.1016/j.bpj.2010.09.018.

Abstract

Many fundamental cellular and extracellular processes in the body are mediated by enzymes. At the single molecule level, enzyme activity is influenced by mechanical forces. However, the effects of mechanical forces on the kinetics of enzymatic reactions in complex tissues with intact extracellular matrix (ECM) have not been identified. Here we report that physiologically relevant macroscopic mechanical forces modify enzyme activity at the molecular level in the ECM of the lung parenchyma. Porcine pancreatic elastase (PPE), which binds to and digests elastin, was fluorescently conjugated (f-PPE) and fluorescent recovery after photobleach was used to evaluate the binding kinetics of f-PPE in the alveolar walls of normal mouse lungs. Fluorescent recovery after photobleach indicated that the dissociation rate constant (k(off)) for f-PPE was significantly larger in stretched than in relaxed alveolar walls with a linear relation between k(off) and macroscopic strain. Using a network model of the parenchyma, a linear relation was also found between k(off) and microscopic strain on elastin fibers. Further, the binding pattern of f-PPE suggested that binding sites on elastin unfold with strain. The increased overall reaction rate also resulted in stronger structural breakdown at the level of alveolar walls, as well as accelerated decay of stiffness and decreased failure stress of the ECM at the macroscopic scale. These results suggest an important role for the coupling between mechanical forces and enzyme activity in ECM breakdown and remodeling in development, and during diseases such as pulmonary emphysema or vascular aneurysm. Our findings may also have broader implications because in vivo, enzyme activity in nearly all cellular and extracellular processes takes place in the presence of mechanical forces.

摘要

体内许多基本的细胞和细胞外过程都是由酶介导的。在单分子水平上,酶活性受机械力的影响。然而,机械力对完整细胞外基质(ECM)的复杂组织中酶反应动力学的影响尚未确定。在这里,我们报告称,生理相关的宏观机械力在肺实质 ECM 的分子水平上改变了酶活性。弹性蛋白酶(PPE)与弹性蛋白结合并消化弹性蛋白,其被荧光偶联(f-PPE),荧光恢复后光漂白用于评估正常小鼠肺肺泡壁中 f-PPE 的结合动力学。荧光恢复后光漂白表明,f-PPE 的离解速率常数(k(off))在拉伸的肺泡壁中明显大于松弛的肺泡壁,k(off)与宏观应变之间存在线性关系。使用实质的网络模型,也发现 k(off)与弹性纤维上的微观应变之间存在线性关系。此外,f-PPE 的结合模式表明,弹性蛋白上的结合位点随应变而展开。总体反应速率的增加也导致肺泡壁水平的结构破坏更强,以及 ECM 在宏观尺度上的刚度衰减和失效应力降低。这些结果表明,机械力与酶活性之间的耦合在 ECM 破坏和重塑的发育过程中以及在肺气肿或血管动脉瘤等疾病中起着重要作用。我们的发现可能具有更广泛的意义,因为在体内,几乎所有细胞和细胞外过程中的酶活性都是在机械力的存在下发生的。

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