Ritter Michael C, Jesudason Rajiv, Majumdar Arnab, Stamenovic Dimitrije, Buczek-Thomas Jo Ann, Stone Phillip J, Nugent Matthew A, Suki Béla
Department of Biomedical Engineering, Boston University, 44 Cummington Street, Boston, MA 02215, USA.
Proc Natl Acad Sci U S A. 2009 Jan 27;106(4):1081-6. doi: 10.1073/pnas.0808414106. Epub 2009 Jan 14.
Mechanical failure of soft tissues is characteristic of life-threatening diseases, including capillary stress failure, pulmonary emphysema, and vessel wall aneurysms. Failure occurs when mechanical forces are sufficiently high to rupture the enzymatically weakened extracellular matrix (ECM). Elastin, an important structural ECM protein, is known to stretch beyond 200% strain before failing. However, ECM constructs and native vessel walls composed primarily of elastin and proteoglycans (PGs) have been found to fail at much lower strains. In this study, we hypothesized that PGs significantly contribute to tissue failure. To test this, we developed a zipper network model (ZNM), in which springs representing elastin are organized into long wavy fibers in a zipper-like formation and placed within a network of springs mimicking PGs. Elastin and PG springs possessed distinct mechanical and failure properties. Simulations using the ZNM showed that the failure of PGs alone reduces the global failure strain of the ECM well below that of elastin, and hence, digestion of elastin does not influence the failure strain. Network analysis suggested that whereas PGs drive the failure process and define the failure strain, elastin determines the peak and failure stresses. Predictions of the ZNM were experimentally confirmed by measuring the failure properties of engineered elastin-rich ECM constructs before and after digestion with trypsin, which cleaves the core protein of PGs without affecting elastin. This study reveals a role for PGs in the failure properties of engineered and native ECM with implications for the design of engineered tissues.
软组织的机械性衰竭是危及生命的疾病的特征,包括毛细血管应力衰竭、肺气肿和血管壁动脉瘤。当机械力足够高以破裂酶促弱化的细胞外基质(ECM)时,就会发生衰竭。弹性蛋白是一种重要的结构性ECM蛋白,已知在失效前可拉伸超过200%的应变。然而,已发现主要由弹性蛋白和蛋白聚糖(PGs)组成的ECM构建体和天然血管壁在低得多的应变下就会失效。在本研究中,我们假设PGs对组织衰竭有显著贡献。为了验证这一点,我们开发了一种拉链网络模型(ZNM),其中代表弹性蛋白的弹簧被组织成拉链状排列的长波浪纤维,并置于模拟PGs的弹簧网络内。弹性蛋白和PG弹簧具有不同的机械和失效特性。使用ZNM进行的模拟表明,仅PGs的失效就会使ECM的整体失效应变远低于弹性蛋白的失效应变,因此,弹性蛋白的消化不会影响失效应变。网络分析表明,虽然PGs驱动失效过程并定义失效应变,但弹性蛋白决定峰值和失效应力。通过测量富含弹性蛋白的工程化ECM构建体在用胰蛋白酶消化前后的失效特性,实验证实了ZNM的预测,胰蛋白酶可切割PGs的核心蛋白而不影响弹性蛋白。本研究揭示了PGs在工程化和天然ECM的失效特性中的作用,这对工程组织的设计具有重要意义。