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Autophagy and apoptosis: parent-of-origin genome-dependent mechanisms of cellular self-destruction

机译:自噬和细胞凋亡:起源于父母的基因组依赖的细胞自我毁灭的机制。

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摘要

Functional genomic imprinting is necessary for the transfer of maternal resources to mammalian embryos. Imprint-free embryos are unable to establish a viable placental vascular network necessary for the transfer of resources such as nutrients and oxygen. How the parental origin of inherited genes influences cellular response to resource limitation is currently not well understood. Because such limitations are initially realized by the placenta, we studied how maternal and paternal genomes influence the cellular self-destruction responses of this organ specifically. Here, we show that cellular autophagy is prevalent in androgenetic (i.e. having only a paternal genome) placentae, while apoptosis is prevalent in parthenogenetic (i.e. having only a maternal genome) placentae. Our findings indicate that the parental origin of inherited genes determines the placenta's cellular death pathway: autophagy for androgenotes and apoptosis for parthenogenotes. The difference in time of arrest between androgenotes and parthenogenotes can be attributed, at least in part, to their placentae's selective use of these two cell death pathways. We anticipate our findings to be a starting point for general studies on the parent-of-origin regulation of autophagy. Furthermore, our work opens the door to new studies on the involvement of autophagy in pathologies of pregnancy in which the restricted transfer of maternal resources is diagnosed.
机译:功能基因组印迹是将母体资源转移到哺乳动物胚胎所必需的。无印迹的胚胎无法建立可行的胎盘血管网络,这是营养和氧气等资源转移所必需的。遗传基因的父母起源如何影响细胞对资源限制的反应目前尚不清楚。因为这种限制最初是由胎盘实现的,所以我们研究了母本和父本基因组如何特别影响该器官的细胞自我破坏反应。在这里,我们表明细胞自噬在雄激素(仅具有父本基因组)胎盘中普遍存在,而凋亡在孤雌生殖(即仅具有母体基因组)胎盘中普遍存在。我们的发现表明,遗传基因的亲本起源决定了胎盘的细胞死亡途径:雄激素的自噬和孤雌生殖的细胞凋亡。雌雄同体和孤雌生殖之间停滞时间的差异至少可以部分归因于它们的胎盘对这两种细胞死亡途径的选择性使用。我们预计我们的发现将成为有关自噬的母体调节的一般研究的起点。此外,我们的工作为自噬参与妊娠病理学的新研究打开了大门,在这些病理学中,诊断为母体资源转移受限。

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