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胎儿和新生儿膈肌中蛋白水解信号和抗氧化能力的个体发生。

Ontogeny of proteolytic signaling and antioxidant capacity in fetal and neonatal diaphragm.

机构信息

Centre for Neonatal Research and Education, The University of Western Australia, Crawley 6009, Western Australia, Australia.

出版信息

Anat Rec (Hoboken). 2012 May;295(5):864-71. doi: 10.1002/ar.22436. Epub 2012 Mar 7.

Abstract

Although upregulation of protein degradation pathways contributes to the development of muscle weakness in response to muscle injury and inflammation in the adult diaphragm, less is known about the preterm diaphragm. Muscle development during the antenatal and early postnatal periods normally results in net growth. However, the structural and functional immaturity of the preterm diaphragm may predispose it to injury and inflammation induced by adverse antenatal and postnatal exposures. Characterization of the ontogeny of diaphragm protein degradation pathways in early life is essential to recognize altered signaling pathways under pathologic conditions in preterm babies. We assessed the relative role of the major proteolytic pathways and antioxidant capacity during muscle maturation in ovine fetuses and lambs from 75 days to 200 days postconceptual age. Gene expression and protein content of calpain and caspase 3 exhibited a similar profile with advancing gestation, increasing from 75 days to 100 days/128 days and subsequently decreasing gradually toward the end of gestation. In contrast, ubiquitin conjugating and ligase genes did not change during gestation. All proteolytic genes examined (except Ubiquitin) were upregulated rapidly after delivery, with a similar developmental trend observed in calpain II protein content as well as calpain protease activity. In contrast, antioxidant gene expression demonstrated a steady increase from 75 days gestation to 24 hr after birth, followed by a significant reduction at 7 weeks of postnatal age (P ≤ 0.002). The proteolytic signaling and antioxidant capacity patterns reflect the adaptive process to metabolic change and muscle maturity with development.

摘要

虽然蛋白降解途径的上调导致成年膈肌在肌肉损伤和炎症反应时出现肌肉无力,但人们对早产儿膈肌知之甚少。产前和产后早期的肌肉发育通常导致净生长。然而,早产儿膈肌的结构和功能不成熟可能使其容易受到不利的产前和产后暴露引起的损伤和炎症。在病理条件下,识别早产儿信号通路的改变,明确早期生命膈肌蛋白降解途径的发育特征是至关重要的。我们评估了在绵羊胎儿和羔羊从 75 天到 200 天妊娠龄的肌肉成熟过程中,主要蛋白水解途径和抗氧化能力的相对作用。钙蛋白酶和半胱天冬酶 3 的基因表达和蛋白含量随胎龄的增加呈现相似的特征,从 75 天增加到 100 天/128 天,随后逐渐减少到妊娠末期。相比之下,泛素连接酶和连接酶基因在整个妊娠过程中没有变化。所有检查的蛋白水解基因(除泛素外)在分娩后迅速上调,钙蛋白酶 II 蛋白含量和钙蛋白酶活性也观察到相似的发育趋势。相比之下,抗氧化基因表达从 75 天妊娠到出生后 24 小时持续增加,然后在出生后 7 周时显著减少(P ≤ 0.002)。蛋白水解信号和抗氧化能力模式反映了与发育相关的代谢变化和肌肉成熟的适应过程。

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