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首页> 外文期刊>American Journal of Physiology >Altered hemodynamics controls matrix metalloproteinase activity and tenascin-C expression in neonatal pig lung.
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Altered hemodynamics controls matrix metalloproteinase activity and tenascin-C expression in neonatal pig lung.

机译:改变的血流动力学控制着新生猪肺中的基质金属蛋白酶活性和腱生蛋白-C表达。

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摘要

Tenascin-C (TN-C) expression and matrix metalloproteinase (MMP) activity are induced within remodeling pulmonary arteries (PAs), where they promote cell growth. Because pulmonary vascular disease in children with congenital heart defects is commonly associated with changes in pulmonary hemodynamics, we hypothesized that changes in pulmonary blood flow regulate TN-C and MMPs. To test this, we ligated the left PAs of neonatal pigs. After 12 wk, we evaluated the levels of TN-C and MMPs in control and ligated lung tissue. Modifying pulmonary hemodynamics increased TN-C mRNA and protein expression, MMP activity, and the DNA-binding activity of Egr-1, a transcription factor that has been shown to activate TN-C expression. To link MMP-mediated remodeling of the extracellular matrix to increased TN-C expression and Egr-1 activity, porcine PA smooth muscle cells were cultivated either on denatured type I collagen, which supported TN-C expression and Egr-1 activity, or on native collagen, which had the opposite effect. These data provide a framework for understanding how changes in pulmonary blood flow in the neonate modify the tissue microenvironment and cell behavior.
机译:Tenascin-C(TN-C)表达和基质金属蛋白酶(MMP)活性在重塑肺动脉(PAs)内被诱导,从而促进细胞生长。由于先天性心脏缺陷患儿的肺血管疾病通常与肺血流动力学的变化有关,因此我们假设肺血流的变化会调节TN-C和MMP。为了测试这一点,我们结扎了新生猪的左PA。 12周后,我们评估了对照和结扎的肺组织中TN-C和MMP的水平。改变肺血流动力学可以增加TN-C mRNA和蛋白表达,MMP活性以及Egr-1的DNA结合活性,Egr-1是一种转录因子,已被证实可以激活TN-C表达。为了将MMP介导的细胞外基质重塑与增加的TN-C表达和Egr-1活性联系起来,在变性的I型胶原蛋白(支持TN-C表达和Egr-1活性)上或在天然胶原蛋白,其作用相反。这些数据为理解新生儿肺血流的变化如何改变组织微环境和细胞行为提供了框架。

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