TIG1 triggers placental senescence in preeclampsia through LMNA/p53 axis activation

IF 3 2区医学 Q2 DEVELOPMENTAL BIOLOGY

Placenta Pub Date : 2025-02-01 DOI:10.1016/j.placenta.2024.12.023

Yanxuan Xiao , Maliang Tao , Jiexing He , Jiaqi Li , Qiuyu Huang , Yiqi Yu , Mingze Gao , Qian Chen , Zhijian Wang

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Abstract

Introduction

The mechanism behind abnormal placental aging in preeclampsia (PE) is unclear. Although TIG1 is widely expressed in the human placenta, its function hasn't been well understood. Our previous study found a significant elevation of TIG1 in the placentas of PE patients. In this study, we focused on the molecular mechanism by which TIG1 functions in PE.

Methods

TIG1 expression of placentas from PE patients and L-NAME mice were analyzed using qRT-PCR, Western blot, and immunohistochemistry. TIG1-overexpressed HTR-8/SVneo cells were constructed for transcriptomic sequencing. Senescence in the placenta was evaluated by biomarkers of p16, p21, and p53. TIG1 binding proteins were identified via co-immunoprecipitation. A co-culture system of HTR-8/SVneo and human endometrial stromal cells was developed to study the change in trophoblasts’ function.

Results

TIG1 expression was significantly increased in the PE placentas. Elevated expression of TIG1 was associated with abnormal senescence of trophoblasts. TIG1 induced trophoblasts’ senescence by regulating LMNA/p53 axis. The senescence of trophoblasts can be manifested as reduced invasion ability in the co-culture system.

Discussion

Our study indicated that TIG1 was crucial in the development of PE by causing the senescence of trophoblasts and reducing their invasiveness, offering insights into the molecular mechanisms of placental dysfunction in PE.

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TIG1通过LMNA/p53轴激活引发子痫前期胎盘衰老。

导读：子痫前期（PE）胎盘异常老化的机制尚不清楚。虽然TIG1在人胎盘中广泛表达，但其功能尚不清楚。我们之前的研究发现PE患者胎盘中TIG1显著升高。在本研究中，我们重点研究了TIG1在PE中的作用的分子机制。方法：采用qRT-PCR、Western blot和免疫组织化学方法分析PE患者和L-NAME小鼠胎盘中TIG1的表达。构建tig1过表达的HTR-8/SVneo细胞进行转录组测序。通过p16、p21和p53的生物标志物来评估胎盘的衰老。通过共免疫沉淀法鉴定TIG1结合蛋白。建立HTR-8/SVneo与人子宫内膜基质细胞共培养体系，研究滋养细胞功能的变化。结果：TIG1在PE胎盘中表达明显升高。TIG1表达升高与滋养细胞异常衰老有关。TIG1通过调控LMNA/p53轴诱导滋养细胞衰老。滋养细胞的衰老表现为在共培养体系中侵袭能力的降低。讨论：我们的研究表明，TIG1通过引起滋养细胞衰老和降低其侵袭性，在PE的发展中起着至关重要的作用，为PE胎盘功能障碍的分子机制提供了新的见解。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Placenta 医学-发育生物学

CiteScore

6.30

自引率

10.50%

发文量

391

审稿时长

78 days

期刊介绍： Placenta publishes high-quality original articles and invited topical reviews on all aspects of human and animal placentation, and the interactions between the mother, the placenta and fetal development. Topics covered include evolution, development, genetics and epigenetics, stem cells, metabolism, transport, immunology, pathology, pharmacology, cell and molecular biology, and developmental programming. The Editors welcome studies on implantation and the endometrium, comparative placentation, the uterine and umbilical circulations, the relationship between fetal and placental development, clinical aspects of altered placental development or function, the placental membranes, the influence of paternal factors on placental development or function, and the assessment of biomarkers of placental disorders.

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