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内源性逆转录病毒驱动灵长类和啮齿类胎盘谱系特异性调控进化。

Endogenous Retroviruses Drive Lineage-Specific Regulatory Evolution across Primate and Rodent Placentae.

机构信息

The Eunice Kennedy Shriver National Institutes of Child Health and Human Development, NIH, Bethesda, MD, USA.

Institute of Comparative Medicine, College of Veterinary Medicine, Yangzhou University, Yangzhou, Jiangsu, China.

出版信息

Mol Biol Evol. 2021 Oct 27;38(11):4992-5004. doi: 10.1093/molbev/msab223.

Abstract

In mammals, the placenta mediates maternal-fetal nutrient and waste exchange and acts in an immunomodulatory way to facilitate maternal-fetal tolerance. The placenta is highly diverse across mammalian species, yet the molecular mechanisms that distinguish the placenta of human from other mammals are not fully understood. Using an interspecies transcriptomic comparison of human, macaque, and mouse late-gestation placentae, we identified hundreds of genes with lineage-specific expression-including dozens that are placentally enriched and potentially related to pregnancy. We further annotated the enhancers for different human tissues using epigenomic data and demonstrate that the placenta and chorion are unique in that their enhancers display the least conservation. We identified numerous lineage-specific human placental enhancers and found they highly overlap with specific families of endogenous retroviruses (ERVs), including MER21A, MER41A/B, and MER39B that were previously linked to immune response and placental function. Among these ERV families, we further demonstrate that MER41A/B insertions create dozens of lineage-specific serum response factor-binding loci in human, including one adjacent to FBN2, a placenta-specific gene with increased expression in humans that produces the peptide hormone placensin to stimulate glucose secretion and trophoblast invasion. Overall, our results demonstrate the prevalence of lineage-specific placental enhancers which are frequently associated with ERV insertions and likely facilitate the lineage-specific evolution of the mammalian placenta.

摘要

在哺乳动物中,胎盘介导母体-胎儿的营养物质和废物交换,并以免疫调节的方式促进母体-胎儿的耐受。胎盘在哺乳动物中具有高度的多样性,但区分人类胎盘与其他哺乳动物胎盘的分子机制尚未完全理解。我们通过对人类、猕猴和小鼠晚期胎盘的种间转录组比较,鉴定出数百个具有谱系特异性表达的基因,其中包括几十种胎盘特异性高且可能与妊娠有关的基因。我们进一步利用不同人类组织的表观基因组数据对这些基因的增强子进行注释,并证明胎盘和绒毛膜在其增强子的保守性方面是独特的。我们鉴定了许多谱系特异性的人类胎盘增强子,并发现它们与内源性逆转录病毒(ERVs)的特定家族高度重叠,包括以前与免疫反应和胎盘功能相关的 MER21A、MER41A/B 和 MER39B。在这些 ERV 家族中,我们进一步证明 MER41A/B 的插入在人类中创建了数十个谱系特异性的血清反应因子结合位点,其中一个位于 FBN2 附近,FBN2 是一种胎盘特异性基因,在人类中表达增加,产生肽激素 placensin 以刺激葡萄糖分泌和滋养层侵袭。总的来说,我们的研究结果表明,谱系特异性胎盘增强子普遍存在,并且经常与 ERV 插入相关,可能促进了哺乳动物胎盘的谱系特异性进化。

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