孕期0.9时母体适度整体营养减少对胎狒狒肾线粒体基因表达的影响。
Effects of moderate global maternal nutrient reduction on fetal baboon renal mitochondrial gene expression at 0.9 gestation.
作者信息
Pereira Susana P, Oliveira Paulo J, Tavares Ludgero C, Moreno António J, Cox Laura A, Nathanielsz Peter W, Nijland Mark J
机构信息
Center for Neuroscience and Cell Biology, University of Coimbra, Coimbra, Portugal; Department of Life Sciences, School of Sciences and Technology, University of Coimbra, Coimbra, Portugal; Center for Pregnancy and Newborn Research, University of Texas Health Science Center, San Antonio, Texas; and.
Center for Neuroscience and Cell Biology, University of Coimbra, Coimbra, Portugal;
出版信息
Am J Physiol Renal Physiol. 2015 Jun 1;308(11):F1217-28. doi: 10.1152/ajprenal.00419.2014. Epub 2015 Mar 11.
Early life malnutrition results in structural alterations in the kidney, predisposing offspring to later life renal dysfunction. Kidneys of adults who were growth restricted at birth have substantial variations in nephron endowment. Animal models have indicated renal structural and functional consequences in offspring exposed to suboptimal intrauterine nutrition. Mitochondrial bioenergetics play a key role in renal energy metabolism, growth, and function. We hypothesized that moderate maternal nutrient reduction (MNR) would adversely impact fetal renal mitochondrial expression in a well-established nonhuman primate model that produces intrauterine growth reduction at term. Female baboons were fed normal chow diet or 70% of control diet (MNR). Fetal kidneys were harvested at cesarean section at 0.9 gestation (165 days gestation). Human Mitochondrial Energy Metabolism and Human Mitochondria Pathway PCR Arrays were used to analyze mitochondrially relevant mRNA expression. In situ protein content was detected by immunohistochemistry. Despite the smaller overall size, the fetal kidney weight-to-body weight ratio was not affected. We demonstrated fetal sex-specific differential mRNA expression encoding mitochondrial metabolite transport and dynamics proteins. MNR-related differential gene expression was more evident in female fetuses, with 16 transcripts significantly altered, including 14 downregulated and 2 upregulated transcripts. MNR impacted 10 transcripts in male fetuses, with 7 downregulated and 3 upregulated transcripts. The alteration in mRNA levels was accompanied by a decrease in mitochondrial protein cytochrome c oxidase subunit VIc. In conclusion, transcripts encoding fetal renal mitochondrial energy metabolism proteins are nutrition sensitive in a sex-dependent manner. We speculate that these differences lead to decreased mitochondrial fitness that contributes to renal dysfunction in later life.
早期生活营养不良会导致肾脏结构改变,使后代在以后的生活中易患肾功能障碍。出生时生长受限的成年人的肾脏在肾单位数量上有很大差异。动物模型表明,暴露于非最佳宫内营养的后代会出现肾脏结构和功能方面的后果。线粒体生物能量学在肾脏能量代谢、生长和功能中起关键作用。我们假设,在一个成熟的非人灵长类动物模型中,适度的母体营养减少(MNR)会对胎儿肾脏线粒体表达产生不利影响,该模型会导致足月时宫内生长受限。雌性狒狒被喂食正常食物或对照饮食的70%(MNR)。在妊娠0.9期(妊娠165天)剖宫产时采集胎儿肾脏。使用人类线粒体能量代谢和人类线粒体途径PCR阵列分析与线粒体相关的mRNA表达。通过免疫组织化学检测原位蛋白质含量。尽管总体尺寸较小,但胎儿肾脏重量与体重之比不受影响。我们证明了编码线粒体代谢物转运和动力学蛋白的胎儿性别特异性差异mRNA表达。MNR相关的差异基因表达在雌性胎儿中更明显,有16个转录本显著改变,包括14个下调和2个上调转录本。MNR影响雄性胎儿中的10个转录本,有7个下调和3个上调转录本。mRNA水平的改变伴随着线粒体蛋白细胞色素c氧化酶亚基VIc的减少。总之,编码胎儿肾脏线粒体能量代谢蛋白的转录本对营养敏感,且具有性别依赖性。我们推测,这些差异导致线粒体适应性下降,这会导致以后生活中的肾功能障碍。
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