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Genetic modification of smooth muscle cells to enhance mechanical properties of tissue engineered constructs

机译:平滑肌细胞增强组织工程构建体力学性能的遗传修饰

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A number of strategies have been investigated to enhance the mechanical stability of engineered tissues. In this report, we utilized lysyl oxidase (LO) to enzymatically crosslink extracellular matrix (ECM) proteins, particularly collagen and elastin, to enhance the mechanical integrity of the ECM and thereby impart mechanical strength to the engineered tissue. Vascular smooth muscle cells (VSMCs) were liposomally transfected with the LO gene. Western analysis confirmed increased LO expression. Increased LO activity was demonstrated as increased levels of desmosine, a product of LO crosslinking, in the ECM. The mechanical effects of altered crosslink densities within tissue engineered constructs were demonstrated in a VSMC-populated collagen gel model. Smooth muscle cells transfected with lysyl oxidase were seeded in collagen gels; the tensile strength and elastic modulus in these constructs increased by approximately twofold compared to constructs seeded with mock transfected VSMCs. Compositional analysis of the ECM deposited by the transformed cells showed similar collagen and elastin levels, and cell proliferation was similar as well. Thus, increased mechanical properties were attributed to ECM crosslinking.
机译:许多策略进行了研究,以提高工程组织的机械稳定性。在本报告中,我们利用赖氨酰氧化(LO)酶促交联的细胞外基质(ECM)蛋白质,特别是胶原和弹性蛋白,以增强ECM的机械完整性,并由此赋予机械强度的工程化组织。血管平滑肌细胞(VSMCs)与LO基因的脂质体转染。西方分析证实增加LO表达。增加LO活性证明是增加锁链素的水平,LO交联的产物,在ECM中。组织工程化构建体中改变的交联密度的机械效应在VSMC-填充胶原凝胶模型进行了论证。用赖氨酰氧化染平滑肌细胞在胶原凝胶接种;拉伸强度和弹性模量在这些构建体增加了大约两倍相比于用模拟转染的VSMC接种构建体。由转化的细胞沉积在ECM的组成分析显示类似的胶原蛋白和弹性蛋白的水平,和细胞增殖是以及类似。因此,增加的机械性能归因于ECM交联。

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