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Transcriptional profiling of liver during the critical embryo-to-hatchling transition period in the chicken (Gallus gallus)

机译:肝脏临界胚胎到孵化期间肝脏转录分析(Gallus Gallus)

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Although hatching is perhaps the most abrupt and profound metabolic challenge that a chicken must undergo; there have been no attempts to functionally map the metabolic pathways induced in liver during the embryo-to-hatchling transition. Furthermore, we know very little about the metabolic and regulatory factors that regulate lipid metabolism in late embryos or newly-hatched chicks. In the present study, we examined hepatic transcriptomes of 12 embryos and 12 hatchling chicks during the peri-hatch period-or the metabolic switch from chorioallantoic to pulmonary respiration. Initial hierarchical clustering revealed two distinct, albeit opposing, patterns of hepatic gene expression. Cluster A genes are largely lipolytic and highly expressed in embryos. While, Cluster B genes are lipogenic/thermogenic and mainly controlled by the lipogenic transcription factor THRSPA. Using pairwise comparisons of embryo and hatchling ages, we found 1272 genes that were differentially expressed between embryos and hatchling chicks, including 24 transcription factors and 284 genes that regulate lipid metabolism. The three most differentially-expressed transcripts found in liver of embryos were MOGAT1, DIO3 and PDK4, whereas THRSPA, FASN and DIO2 were highest in hatchlings. An unusual finding was the "ectopic" and extremely high differentially expression of seven feather keratin transcripts in liver of 16?day embryos, which coincides with engorgement of liver with yolk lipids. Gene interaction networks show several transcription factors, transcriptional co-activators/co-inhibitors and their downstream genes that exert a 'ying-yang' action on lipid metabolism during the embryo-to-hatching transition. These upstream regulators include ligand-activated transcription factors, sirtuins and Kruppel-like factors. Our genome-wide transcriptional analysis has greatly expanded the hepatic repertoire of regulatory and metabolic genes involved in the embryo-to-hatchling transition. New knowledge was gained on interactive transcriptional networks and metabolic pathways that enable the abrupt switch from ectothermy (embryo) to endothermy (hatchling) in the chicken. Several transcription factors and their coactivators/co-inhibitors appear to exert opposing actions on lipid metabolism, leading to the predominance of lipolysis in embryos and lipogenesis in hatchlings. Our analysis of hepatic transcriptomes has enabled discovery of opposing, interconnected and interdependent transcriptional regulators that provide precise ying-yang or homeorhetic regulation of lipid metabolism during the critical embryo-to-hatchling transition.
机译:虽然孵化也许是鸡肉必须经历的最突然和深刻的代谢挑战;在胚胎到孵化过渡期间没有尝试用作肝脏诱导的代谢途径。此外,我们对调节晚期胚胎或新孵化的小鸡中的脂质代谢的代谢和调节因素很少。在本研究中,我们在Peri孵化周期期间检查了12个胚胎和12个孵化雏鸡的肝转录组,或来自Chorioallantic至肺呼吸的代谢切换。初始分层聚类揭示了两个不同的,虽然反对,但肝基因表达模式。簇基因在很大程度上是脂溶解的并且在胚胎中高度表达。虽然,簇B基因是脂肪生/热原,主要由脂肪转录因子THRSPA控制。使用胚胎和孵化年龄的成对比较,我们发现1272个基因在胚胎和孵化雏鸡之间差异表达,包括24种转录因子和调节脂质代谢的284个基因。在胚胎的肝脏中发现的三种最差异表达的转录物是Mogat1,DiO3和PDK4,而Thrspa,FasN和DiO2在孵出中最高。一种不寻常的发现是16?日胚胎肝脏中七个羽毛角蛋白转录物的“异位”和极高的差异表达,这与蛋黄脂质的肝脏结合恰逢肝脏。基因相互作用网络显示出几种转录因子,转录共激活剂/共抑制剂及其下游基因,在胚胎到阴影过程中施加对脂质代谢的“ying yang”作用。这些上游调节剂包括配体活化的转录因子,SIRTUINS和KRUPPEL样因子。我们的基因组转录分析极大地扩展了胚胎和代谢基因的肝脏曲目,参与胚胎到孵化过渡。在交互式转录网络和代谢途径上获得了新知识,使得能够从卵巢(胚胎)突然切换到鸡肉中吸收(孵化)。几种转录因子及其共催光剂/共同抑制剂似乎对脂质代谢产生相反的作用,导致孵化丛林中胚胎和脂肪生成的脂肪分解优势。我们对肝脏转录瘤的分析使得能够发现对抗,相互依赖的和相互依存的转录调节剂,其提供精确的ying yang或在临界胚胎到孵化过渡期间脂质代谢的家用调节。

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