Role of Transcription Factor, LIM Homeobox 9 (LHX9) in Inflammatory Response by PGE2 and Thrombin in SERPINA1-Silencing Endometrial Stromal Cells

IF 3 3区生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY

Molecular Reproduction and Development Pub Date : 2025-08-13 DOI:10.1002/mrd.70046

Kazuya Kusama, Misuzu Ashihara, Moana Okita, Kanoko Yoshida, Masumi Suzuki, Kaito Suzuki, Rena Hosokawa, Mikihiro Yoshie, Junya Kojima, Yumi Mizuno, Masanori Ono, Hirotaka Nishi, Takeshi Kajihara, Kazuhiro Tamura

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引用次数: 0

Abstract

Endometriosis is hypothesized to result from retrograde menstruation where cell debris including endometrial stromal cells (ESCs) travel through the fallopian tubes. This chronic inflammatory disease is characterized by inflammatory and fibrotic endometrial tissue. We have previously observed reduced expression of the anti-inflammatory factor SERPINA1 in endometriosis-like lesions in a mouse model implanted with human ESCs. Additionally, pro-inflammatory factors present in peritoneal hemorrhage exacerbated inflammation in these grafts, partly through prostaglandin (PG) E2 and thrombin. However, it remains unclear whether the reduction of SERPINA1, in combination with PGE2 and thrombin, synergistically influences the expression of inflammatory factors in endometriosis lesions and the underlying mechanisms. We analyzed RNA sequencing data from ESCs treated with SERPINA1 siRNA and PGE2/thrombin, comparing them to data sets derived from ESCs subjected to either SERPINA1 knockdown or PGE2/thrombin treatment. Comparative analysis identified 49 transcripts that were upregulated under both conditions and enriched for transcription regulatory genes, including SNAI1, HDAC5, PBX1, SOX4, EPAS1, LHX9, and MAFK. Silencing SNAI1, HDAC5, SOX4, EPAS1, or LHX9 suppressed IL6, CXCL8, and IL1B expression, which had been upregulated by SERPINA1 siRNA and PGE2/thrombin. Among these genes, LHX9 expression was significantly elevated in ectopic lesions, predominantly localized to stromal and glandular epithelial cells, with more pronounced expression during the secretory phase. LHX9 levels were also increased in endometriotic lesions compared to the normal endometrium. In conclusion, reduced SERPINA1 expression in ectopic ESCs, combined with PGE2/thrombin, induces inflammatory cytokine expression linked to LHX9. Pharmacological targeting of LHX9 may present a promising therapeutic strategy for mitigating chronic inflammation in endometriotic lesions.

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转录因子LIM Homeobox 9 （LHX9）在serpina1沉默子宫内膜基质细胞PGE2和凝血酶炎症反应中的作用

子宫内膜异位症被认为是由月经逆行引起的，包括子宫内膜基质细胞（ESCs）在内的细胞碎片穿过输卵管。这种慢性炎症性疾病的特点是炎症和纤维化的子宫内膜组织。我们之前观察到，在植入人类ESCs的小鼠模型中，抗炎因子SERPINA1在子宫内膜异位症样病变中的表达降低。此外，腹膜出血中存在的促炎因子部分通过前列腺素（PG） E2和凝血酶加剧了移植物的炎症。然而，SERPINA1的降低是否与PGE2和凝血酶协同影响子宫内膜异位症病变中炎症因子的表达及其潜在机制尚不清楚。我们分析了SERPINA1 siRNA和PGE2/凝血酶处理的ESCs的RNA测序数据，并将其与SERPINA1敲低或PGE2/凝血酶处理的ESCs的数据集进行了比较。对比分析发现，49个转录本在两种条件下均上调，且转录调控基因富集，包括SNAI1、HDAC5、PBX1、SOX4、EPAS1、LHX9和MAFK。沉默SNAI1、HDAC5、SOX4、EPAS1或LHX9可抑制被SERPINA1 siRNA和PGE2/凝血酶上调的IL6、CXCL8和IL1B的表达。在这些基因中，LHX9在异位病变中表达显著升高，主要局限于间质和腺上皮细胞，在分泌期表达更为明显。与正常子宫内膜相比，子宫内膜异位症病变中的LHX9水平也有所升高。综上所述，在异位ESCs中，SERPINA1表达的降低，结合PGE2/凝血酶，可诱导与LHX9相关的炎症细胞因子表达。LHX9的药理靶向可能是减轻子宫内膜异位症病变慢性炎症的一种有希望的治疗策略。

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来源期刊

Molecular Reproduction and Development 生物-发育生物学

CiteScore

5.20

自引率

0.00%

发文量

审稿时长

6-12 weeks

期刊介绍： Molecular Reproduction and Development takes an integrated, systems-biology approach to understand the dynamic continuum of cellular, reproductive, and developmental processes. This journal fosters dialogue among diverse disciplines through primary research communications and educational forums, with the philosophy that fundamental findings within the life sciences result from a convergence of disciplines. Increasingly, readers of the Journal need to be informed of diverse, yet integrated, topics impinging on their areas of interest. This requires an expansion in thinking towards non-traditional, interdisciplinary experimental design and data analysis.