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TFAP2C是子宫内滋养层细胞侵袭和深层血绒毛膜胎盘形成的关键调节因子。

TFAP2C is a key regulator of intrauterine trophoblast cell invasion and deep hemochorial placentation.

作者信息

Dominguez Esteban M, Moreno-Irusta Ayelen, Scott Regan L, Iqbal Khursheed, Soares Michael J

机构信息

Institute for Reproductive and Developmental Sciences, Department of Pathology & Laboratory Medicine, and.

Department of Obstetrics and Gynecology, University of Kansas Medical Center, Kansas City, Kansas, USA.

出版信息

JCI Insight. 2024 Dec 3;10(2):e186471. doi: 10.1172/jci.insight.186471.

Abstract

Transcription factor AP-2 gamma (TFAP2C) has been identified as a key regulator of the trophoblast cell lineage and hemochorial placentation. The rat possesses deep placentation characterized by extensive intrauterine trophoblast cell invasion, which resembles human placentation. Tfap2c is expressed in multiple trophoblast cell lineages, including invasive trophoblast cells situated within the uterine-placental interface of the rat placentation site. Global genome editing was used to explore the biology of Tfap2c in rat placenta development. Homozygous global disruption of Tfap2c resulted in prenatal lethality. Heterozygous global disruption of Tfap2c was associated with diminished invasive trophoblast cell infiltration into the uterus. The role of TFAP2C in the invasive trophoblast cell lineage was explored using Cre-lox conditional mutagenesis. Invasive trophoblast cell-specific disruption of Tfap2c resulted in inhibition of intrauterine trophoblast cell invasion and intrauterine and postnatal growth restriction. The invasive trophoblast cell lineage was not impaired following conditional monoallelic disruption of Tfap2c. In summary, TFAP2C contributes to the progression of distinct stages of placental development. TFAP2C is a driver of early events in trophoblast cell development and reappears later in gestation as an essential regulator of the invasive trophoblast cell lineage. A subset of TFAP2C actions on trophoblast cells are dependent on gene dosage.

摘要

转录因子AP-2γ(TFAP2C)已被确定为滋养层细胞谱系和血绒毛膜胎盘形成的关键调节因子。大鼠具有深度胎盘形成,其特征是广泛的子宫内滋养层细胞侵袭,这类似于人类胎盘形成。Tfap2c在多个滋养层细胞谱系中表达,包括位于大鼠胎盘部位子宫-胎盘界面的侵袭性滋养层细胞。利用全基因组编辑来探索Tfap2c在大鼠胎盘发育中的生物学特性。Tfap2c的纯合全基因组破坏导致产前致死。Tfap2c的杂合全基因组破坏与侵袭性滋养层细胞向子宫内的浸润减少有关。使用Cre-lox条件诱变来探索TFAP2C在侵袭性滋养层细胞谱系中的作用。Tfap2c的侵袭性滋养层细胞特异性破坏导致子宫内滋养层细胞侵袭受到抑制以及子宫内和出生后生长受限。Tfap2c的条件单等位基因破坏后,侵袭性滋养层细胞谱系未受损。总之,TFAP2C有助于胎盘发育不同阶段的进展。TFAP2C是滋养层细胞发育早期事件的驱动因素,在妊娠后期再次出现,作为侵袭性滋养层细胞谱系的重要调节因子。TFAP2C对滋养层细胞的一部分作用取决于基因剂量。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/806f/11790029/f06fda117daf/jciinsight-10-186471-g082.jpg

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