父本长期补充叶酸可诱导鸡获得性发育和代谢变化的跨代遗传

Shengru Wu, W. Guo, Xinyi Li, Yanli Liu, Yulong Li, Xinyu Lei, Junhu Yao, Xiaojun Yang
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引用次数: 20

摘要

越来越多的证据表明,父亲的饮食可以导致后代的代谢变化,但在鸟类中明确的机制尚不清楚。在本研究中,我们终生给种鸡饲喂5种不同的饲粮,分别含有0、0.25、1.25、2.50和5.00 mg kg - 1叶酸。父本补充叶酸(FS)有利于肉鸡子代的生长和器官发育。最重要的是,根据生化和代谢组学分析,父亲FS对种鸡和肉鸡后代的脂质和葡萄糖代谢有影响。我们进一步对肝脏和精子的信使RNA (mRNA)、长链非编码RNA (lncRNA)和微RNA (miRNA)进行了全局分析。在种鸡和肉鸡后代中,参与糖酵解或糖异生途径和PPAR信号通路的关键基因,包括PEPCK、ANGPTL4和THRSP,受到肝脏和精子mirna和lncrna差异表达的调控。此外,ANGPTL4的表达也可以通过竞争内源性RNA (ceRNA)机制受到精子中差异表达的mirna和lncrna的调控。综上所述,该模型表明,父本叶酸可以跨代调节肉鸡后代的脂质和糖代谢,其表观遗传传递可能涉及精子mirna和lncrna的改变。
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Paternal chronic folate supplementation induced the transgenerational inheritance of acquired developmental and metabolic changes in chickens
Increasing evidence indicates that paternal diet can result in metabolic changes in offspring, but the definite mechanism remains unclear in birds. Here, we fed breeder cocks five different diets containing 0, 0.25, 1.25, 2.50 and 5.00 mg kg−1 folate throughout life. Paternal folate supplementation (FS) was beneficial to the growth and organ development of broiler offspring. Most importantly, the lipid and glucose metabolism of breeder cocks and broiler offspring were affected by paternal FS, according to biochemical and metabolomic analyses. We further employed global analyses of hepatic and spermatozoal messenger RNA (mRNA), long non-coding RNA (lncRNA) and micro RNA (miRNA). Some key genes involved in the glycolysis or gluconeogenesis pathway and the PPAR signalling pathway, including PEPCK, ANGPTL4 and THRSP, were regulated by differentially expressed hepatic and spermatozoal miRNAs and lncRNAs in breeder cocks and broiler offspring. Moreover, the expression of ANGPTL4 could also be regulated by differentially expressed miRNAs and lncRNAs in spermatozoa via competitive endogenous RNA (ceRNA) mechanisms. Overall, this model suggests that paternal folate could transgenerationally regulate lipid and glucose metabolism in broiler offspring and the epigenetic transmission may involve altered spermatozoal miRNAs and lncRNAs.
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