转移相关肺腺癌转录本1在抗磷脂抗体阳性所致复发性自然流产小鼠中诱导甲基化CpG结合域蛋白4。
Metastasis-associated lung adenocarcinoma transcript 1 induces methyl-CpG-binding domain protein 4 in mice with recurrent spontaneous abortion caused by anti-phospholipid antibody positivity.
作者信息
Han Yongmei, Wang Ying, Zhang Chenyu, Li Yanru, Guo Jing, Tian Chao
机构信息
College of Integrated Traditional Chinese and Western Medicine, Henan University of Traditional Chinese Medicine, Zhengzhou, 450046, Henan, PR China.
Reproductive Center, Nanyang First People's Hospital, Nanyang, 473000, Henan, PR China.
出版信息
Placenta. 2023 Jun;137:38-48. doi: 10.1016/j.placenta.2023.04.008. Epub 2023 Apr 8.
INTRODUCTION
Antiphospholipid syndrome is an autoimmune disease characterized by pregnancy-related morbidity, related to persistent positivity of antiphospholipid antibodies (APL). One of the characteristics of pregnancy-related morbidity in patients with antiphospholipid syndrome is recurrent spontaneous abortion (RSA). This study aimed to examine the mechanism through which metastasis-associated lung adenocarcinoma transcript 1 (MALAT1) regulates methyl-CpG-binding domain protein 4 (MBD4) expression in APL-positive RSA.
METHODS
Clinical samples were subjected to microarray analysis to filter differentially expressed genes. RSA mice with APL positivity were generated, followed by adenoviral vector injection to artificially upregulate MALAT1. The effects of MALAT1 on the biological behavior of trophoblast cells were assessed. The downstream mechanism of MALAT1 was analyzed using subcellular fractionation and bioinformatics prediction, and the relationship between MALAT1 and CREB binding protein (CREBBP) or MBD4 was investigated in trophoblast cells.
RESULTS
MALAT1 was downregulated in APL-positive RSA patients. MALAT1 was predominantly localized in the nucleus and recruited CREBBP to mediate the MBD4 transcription. In the APL-positive RSA mice overexpressing MALAT1, the expression of soluble Fms-related tyrosine kinase 1 and anticardiolipin antibody and the embryonic resorption rate were decreased, indicating that MALAT1 reduced the occurrence of RSA in mice. Moreover, MALAT1 enhanced proliferation, migration, and invasion of trophoblast cells through recruiting CREBBP to promote MBD4 expression. Silencing of CREBBP or MBD4 increased embryonic resorption rate in RSA mice overexpressing MALAT1.
DISCUSSION
MALAT1 suppresses APL-positive RSA by promoting MBD4 transcription through recruitment of CREBBP to the MBD4 promoter region.
引言
抗磷脂综合征是一种自身免疫性疾病,其特征为与抗磷脂抗体(APL)持续阳性相关的妊娠相关并发症。抗磷脂综合征患者妊娠相关并发症的特征之一是复发性自然流产(RSA)。本研究旨在探讨转移相关肺腺癌转录本1(MALAT1)在APL阳性RSA中调节甲基-CpG结合域蛋白4(MBD4)表达的机制。
方法
对临床样本进行微阵列分析以筛选差异表达基因。构建APL阳性的RSA小鼠模型,随后注射腺病毒载体以人工上调MALAT1。评估MALAT1对滋养层细胞生物学行为的影响。采用亚细胞分级分离和生物信息学预测分析MALAT1的下游机制,并在滋养层细胞中研究MALAT1与CREB结合蛋白(CREBBP)或MBD4之间的关系。
结果
MALAT1在APL阳性RSA患者中表达下调。MALAT1主要定位于细胞核,并募集CREBBP以介导MBD4转录。在过表达MALAT1的APL阳性RSA小鼠中,可溶性Fms相关酪氨酸激酶1和抗心磷脂抗体的表达以及胚胎吸收率降低,表明MALAT1减少了小鼠RSA的发生。此外,MALAT1通过募集CREBBP促进MBD4表达,增强了滋养层细胞的增殖、迁移和侵袭能力。沉默CREBBP或MBD4可增加过表达MALAT1的RSA小鼠的胚胎吸收率。
讨论
MALAT1通过募集CREBBP至MBD4启动子区域促进MBD4转录,从而抑制APL阳性RSA。
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