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Intrauterine growth restriction is associated with cardiac ultrastructural and gene expression changes related to the energetic metabolism in a rabbit model

机译:宫内生长受限与兔模型中心脏超微结构和基因表达的变化有关,与能量代谢有关

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Intrauterine growth restriction (IUGR) affects 7-10% of pregnancies and is associated with cardiovascular remodeling and dysfunction, which persists into adulthood. The underlying subcellular remodeling and cardiovascular programming events are still poorly documented. Cardiac muscle is central in the fetal adaptive mechanism to IUGR given its high energetic demands. The energetic homeostasis depends on the correct interaction of several molecular pathways and the adequate arrangement of intracellular energetic units (ICEUs), where mitochondria interact with the contractile machinery and the main cardiac ATPases to enable a quick and efficient energy transfer. We studied subcellular cardiac adaptations to IUGR in an experimental rabbit model. We evaluated the ultrastructure of ICEUs with transmission electron microscopy and observed an altered spatial arrangement in IUGR, with significant increases in cytosolic space between mitochondria and myofilaments. A global decrease of mitochondrial density was also observed. In addition, we conducted a global gene expression profile by advanced bioinformatics tools to assess the expression of genes involved in the cardiomyocyte energetic metabolism and identified four gene modules with a coordinated over-representation in IUGR: oxygen homeostasis (GO: 0032364), mitochondrial respiratory chain complex I (GO:0005747), oxidative phosphorylation (GO: 0006119), and NADH dehydrogenase activity (GO:0003954). These findings might contribute to changes in energetic homeostasis in IUGR. The potential persistence and role of these changes in long-term cardiovascular programming deserves further investigation.
机译:宫内生长受限(IUGR)影响7-10%的怀孕,并与心血管重塑和功能障碍有关,并一直持续到成年期。潜在的亚细胞重塑和心血管程序性事件仍鲜有文献报道。鉴于其较高的能量需求,心脏肌肉对IUGR的胎儿适应机制至关重要。高能动态平衡取决于几种分子途径的正确相互作用以及细胞内高能单元(ICEU)的适当排列,其中线粒体与收缩机制和主要心脏ATPase相互作用以实现快速有效的能量转移。我们在实验性兔子模型中研究了亚细胞对IUGR的心脏适应性。我们用透射电子显微镜评估了ICEUs的超微结构,并观察到IUGR的空间排列发生了改变,线粒体和肌丝之间的胞质空间显着增加。还观察到线粒体密度的总体下降。此外,我们通过先进的生物信息学工具进行了全球基因表达谱分析,以评估参与心肌细胞能量代谢的基因的表达,并确定了在IUGR中具有协调过度表达的四个基因模块:氧稳态(GO:0032364),线粒体呼吸链复合物I(GO:0005747),氧化磷酸化(GO:0006119)和NADH脱氢酶活性(GO:0003954)。这些发现可能有助于IUGR能量平衡的改变。这些变化在长期心血管计划中的潜在持久性和作用值得进一步研究。

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