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A pair of co-opted retroviral envelope syncytin genes is required for formation of the two-layered murine placental syncytiotrophoblast.一对共转导的逆转录病毒包膜基因syncytin 对于形成双层鼠胎盘合胞滋养层是必需的。
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The captured retroviral envelope syncytin-A and syncytin-B genes are conserved in the Spalacidae together with hemotrichorial placentation.捕获的逆转录病毒包膜蛋白合胞素-A和合胞素-B基因在竹鼠科中与血绒毛膜胎盘一起保守存在。
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Syncytin-A knockout mice demonstrate the critical role in placentation of a fusogenic, endogenous retrovirus-derived, envelope gene.合胞素A基因敲除小鼠证明了一种融合性、内源性逆转录病毒衍生的包膜基因在胎盘形成中的关键作用。
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An endogenous retroviral envelope syncytin and its cognate receptor identified in the viviparous placental lizard.在胎生的有胎盘蜥蜴中鉴定出一种内源性逆转录病毒包膜蛋白 syncytin 及其同源受体。
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Syncytin-A and syncytin-B, two fusogenic placenta-specific murine envelope genes of retroviral origin conserved in Muridae.合胞素-A和合胞素-B,鼠科中两个起源于逆转录病毒的、具有融合活性的胎盘特异性鼠类包膜基因,在鼠科中保守存在。
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本文引用的文献

1
Slc20a1 and Slc20a2 regulate neuronal plasticity and cognition independently of their phosphate transport ability.Slc20a1 和 Slc20a2 通过独立于其磷酸盐转运能力调节神经元可塑性和认知。
Cell Death Dis. 2024 Jan 9;15(1):20. doi: 10.1038/s41419-023-06292-z.
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SLC20a1/PiT-1 is required for chorioallantoic placental morphogenesis.绒毛尿囊胎盘形态发生需要SLC20a1/PiT-1。
Vasc Biol. 2023 Apr 19;5(1). doi: 10.1530/VB-22-0018. Print 2023 Apr 1.
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Universal and cross-cancer prognostic biomarkers for predicting survival risk of cancer patients from expression profile of apoptotic pathway genes.从凋亡通路基因表达谱预测癌症患者生存风险的通用和跨癌预后生物标志物。
Proteomics. 2022 Feb;22(3):e2000311. doi: 10.1002/pmic.202000311. Epub 2021 Oct 28.
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Highly accurate protein structure prediction with AlphaFold.利用 AlphaFold 进行高精度蛋白质结构预测。
Nature. 2021 Aug;596(7873):583-589. doi: 10.1038/s41586-021-03819-2. Epub 2021 Jul 15.
5
Structure of the sodium-dependent phosphate transporter reveals insights into human solute carrier SLC20.钠依赖性磷酸盐转运体的结构揭示了对人类溶质载体SLC20的见解。
Sci Adv. 2020 Aug 7;6(32):eabb4024. doi: 10.1126/sciadv.abb4024. eCollection 2020 Aug.
6
Extracellular phosphate sensing in mammals: what do we know?哺乳动物细胞外磷酸盐感应:我们了解多少?
J Mol Endocrinol. 2020 Oct;65(3):R53-R63. doi: 10.1530/JME-20-0121.
7
PiT1/Slc20a1 Is Required for Endoplasmic Reticulum Homeostasis, Chondrocyte Survival, and Skeletal Development.PiT1/Slc20a1 对于内质网稳态、软骨细胞存活和骨骼发育是必需的。
J Bone Miner Res. 2019 Feb;34(2):387-398. doi: 10.1002/jbmr.3609. Epub 2018 Nov 20.
8
SWISS-MODEL: homology modelling of protein structures and complexes.SWISS-MODEL:蛋白质结构和复合物的同源建模。
Nucleic Acids Res. 2018 Jul 2;46(W1):W296-W303. doi: 10.1093/nar/gky427.
9
Transmission, Evolution, and Endogenization: Lessons Learned from Recent Retroviral Invasions.传播、进化和内源性化:从最近的逆转录病毒入侵中吸取的教训。
Microbiol Mol Biol Rev. 2017 Dec 13;82(1). doi: 10.1128/MMBR.00044-17. Print 2018 Mar.
10
Phosphate (P)-regulated heterodimerization of the high-affinity sodium-dependent P transporters PiT1/Slc20a1 and PiT2/Slc20a2 underlies extracellular P sensing independently of P uptake.磷酸盐(P)调节高亲和力钠依赖性 P 转运体 PiT1/Slc20a1 和 PiT2/Slc20a2 的异二聚化,是细胞外 P 感应的基础,而与 P 摄取无关。
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钠依赖性磷酸盐转运蛋白 PiT1/SLC20A1 作为内源性逆转录病毒 envelope syncytin-B 的受体,参与了小鼠胎盘的形成。

Sodium-dependent phosphate transporter PiT1/SLC20A1 as the receptor for the endogenous retroviral envelope syncytin-B involved in mouse placenta formation.

机构信息

Viroxis, Institut Gustave Roussy, Villejuif, France.

Unité Physiologie et Pathologie Moléculaires des Rétrovirus Endogènes et Infectieux, CNRS UMR 9196, Institut Gustave Roussy, Université Paris-Saclay, Villejuif, France.

出版信息

J Virol. 2024 Oct 22;98(10):e0091524. doi: 10.1128/jvi.00915-24. Epub 2024 Sep 17.

DOI:10.1128/jvi.00915-24
PMID:39287391
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11495048/
Abstract

are envelope genes of retroviral origin that play a critical role in the formation of a syncytial structure at the fetomaternal interface their fusogenic activity. The mouse placenta is unique among placental mammals since the fetomaternal interface comprises two syncytiotrophoblast layers (ST-I and ST-II) instead of one observed in all other hemochorial placentae. Each layer specifically expresses a distinct mouse syncytin, namely syncytin-A (SynA) for ST-I and syncytin-B (SynB) for ST-II, which have been shown to be essential to placentogenesis and embryonic development. The cellular receptor for SynA has been identified as the membrane protein LY6E and is not the receptor for SynB. Here, by combining a cell-cell fusion assay with the screening of a human ORFeome-derived expression library, we identified the transmembrane multipass sodium-dependent phosphate transporter 1 PiT1/SLC20A1 as the receptor for SynB. Transfection of cells with the cloned receptor, but not the closely related PiT2/SLC20A2, leads to their fusion with cells expressing SynB, with no cross-reactive fusion activity with SynA. The interaction between the two partners was further demonstrated by immunoprecipitation. PiT1/PiT2 chimera and truncation experiments identified the PiT1 N-terminus as the major determinant for SynB-mediated fusion. RT-qPCR analysis of PiT1 expression on a panel of mouse adult and fetal tissues revealed a concomitant increase of PiT1 and SynB specifically in the developing placenta. Finally, electron microscopy analysis of the placenta of PiT1 null embryo before they die (E11.5) disclosed default of ST-II formation with lack of syncytialization, as previously observed in cognate SynB null placenta, and consistent with the present identification of PiT1 as the SynB partner.IMPORTANCESyncytins are envelope genes of endogenous retroviruses, coopted for a physiological function in placentation. They are fusogenic proteins that mediate cell-cell fusion by interacting with receptors present on the partner cells. Here, by devising an fusion assay that enables the screening of an ORFeome-derived expression library, we identified the long-sought receptor for syncytin-B (SynB), a mouse syncytin responsible for syncytiotrophoblast formation at the fetomaternal interface of the mouse placenta. This protein - PiT1/SLC20A1 - is a multipass transmembrane protein, also known as the receptor for a series of infectious retroviruses. Its profile of expression is consistent with a role in both ancestral endogenization of a SynB founder retrovirus and present-day mouse placenta formation, with evidence-in PiT1 knockout mice-of unfused cells at the level of the cognate placental syncytiotrophoblast layer.

摘要

逆转录病毒起源的 envelope 基因在形成胎儿-母体界面的合胞体结构中起着关键作用,其融合活性。鼠胎盘在胎盘哺乳动物中是独一无二的,因为胎儿-母体界面由两层合胞滋养层(ST-I 和 ST-II)组成,而不是所有其他绒毛膜胎盘中观察到的一层。每一层都特异性表达一种独特的小鼠 syncytin,即合胞滋养层 I 的 syncytin-A(SynA)和合胞滋养层 II 的 syncytin-B(SynB),它们被证明对胎盘发生和胚胎发育至关重要。SynA 的细胞受体已被鉴定为膜蛋白 LY6E,而不是 SynB 的受体。在这里,我们通过将细胞-细胞融合测定法与人类 ORFeome 衍生表达文库的筛选相结合,鉴定出跨膜多跨钠离子依赖性磷酸盐转运蛋白 1 PiT1/SLC20A1 作为 SynB 的受体。用克隆受体转染细胞,但不是密切相关的 PiT2/SLC20A2,导致它们与表达 SynB 的细胞融合,与 SynA 没有交叉反应性融合活性。两个伙伴之间的相互作用通过免疫沉淀进一步证明。PiT1/PiT2 嵌合体和截断实验确定了 PiT1 N 端是 SynB 介导融合的主要决定因素。对一系列小鼠成体和胎儿组织中 PiT1 表达的 RT-qPCR 分析显示,PiT1 和 SynB 特异性地在发育中的胎盘同时增加。最后,PiT1 缺失胚胎(E11.5)胎盘的电子显微镜分析显示,ST-II 形成缺失,没有合胞化,这与先前在同源 SynB 缺失胎盘观察到的情况一致,并且与目前鉴定的 PiT1 作为 SynB 伙伴一致。重要的是,Syncytins 是内源性逆转录病毒的包膜基因,被内源性病毒感染。它们是融合蛋白,通过与伴侣细胞上存在的受体相互作用介导细胞-细胞融合。在这里,我们通过设计一种融合测定法,使 ORFeome 衍生表达文库的筛选成为可能,鉴定出了长期以来寻找的 syncytin-B(SynB)的受体,一种小鼠 syncytin,负责形成小鼠胎盘胎儿-母体界面的合胞滋养层。这种蛋白质 PiT1/SLC20A1 是一种多跨膜蛋白,也被称为一系列传染性逆转录病毒的受体。它的表达谱与 SynB 始祖逆转录病毒的内源性以及目前的小鼠胎盘形成一致,在 PiT1 敲除小鼠中,合胞滋养层层的同源性证据表明存在未融合的细胞。