ATI-2341 TFA 通过介导骨髓间充质干细胞的分化促进受损子宫内膜的修复

IF 0.7 4区 材料科学 Q3 Materials Science Materials Express Pub Date : 2024-01-01 DOI:10.1166/mex.2024.2576
Shiying Guo, Hong Chen, Ying Xu, Doudou Ding, Aihua Chen
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引用次数: 0

摘要

宫腔内粘连(IUA)是子宫内膜病变的常见并发症。本研究探讨了CXCR4的功能选择性异位调节剂ATI-2341在IUA中的作用及其与骨髓间充质干细胞(BMSCs)的相互作用。建立子宫内膜损伤模型后,用 ATI-2341 TFA(100 ng/mL)处理大鼠骨髓间充质干细胞。用 BMSCs 和雌激素处理或未经处理的 IUA 大鼠子宫内膜组织作为对照。检查子宫内膜厚度,并用 MTT 法检测子宫内膜 BMSC 的增殖情况。通过 Western 印迹分析测定 MMP-9、TIMP-1、CK 和 VIM 的水平。与雌激素处理(0.467±0.029 ng/mL)和对照处理相比,使用 ATI-2341 TFA 处理后,MMP-9(0.346±0.036 ng/mL)水平明显下降。携带 ATI-2341 TFA 和雌激素的 BMSCs 均诱导 TIMP-1 表达增加(0.734±0.034 ng/mL,0.618±0.035 ng/mL),并促进子宫内膜生长,ATI-2341 TFA 组子宫内膜更厚(294.21±59.97 μm)。处理后 48 h 和 72 h,ATI-2341 TFA 组和雌激素组的细胞增殖率均增加(P <0.05),且 ATI-2341 TFA 处理后增殖率更高。ATI-2341 TFA100 ng/mL组和雌激素组的细胞角蛋白呈显著阳性,而波形蛋白呈阴性。总之,ATI-2341 TFA 能促进 BMSCs 向子宫内膜上皮细胞分化,增强受损子宫内膜的修复,缓解 IUA。这些发现可能为基于 BMSC 的子宫内膜疾病治疗奠定了基础。
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ATI-2341 TFA promotes repair of damaged endometrium by mediating the differentiation of bone marrow mesenchymal stem cells
Intrauterine adhesion (IUA) is a common complication in endometrial disorder. This study investigated the role of ATI-2341, a functionally selective allosteric regulator of CXCR4 in IUAs, and its interaction with bone marrow-derived mesenchymal stem cells (BMSCs). Following establishment of endometrial injury model, rats BMSCs were treated with ATI-2341 TFA (100 ng/mL). Endometrial tissues of rats with IUA were treated with BMSCs and estrogen, or untreated which was taken as controls. The endometrium thickness was examined and endometrial BMSC proliferation was detected by MTT assay. Levels of MMP-9, TIMP-1, CK, and VIM were determined by Western blot analysis. Treatment with ATI-2341 TFA resulted in significantly decreased level of MMP-9 (0.346±0.036 ng/mL), compared with estrogen treatment (0.467±0.029 ng/mL) and control treatment. Both BMSCs carrying ATI-2341 TFA and estrogen induced increased expression of TIMP-1 (0.734±0.034 ng/mL, 0.618±0.035 ng/mL) and enhanced endometrim growth with thicker endometrium in ATI-2341 TFA group (294.21±59.97 μm). 48 h and 72 h after treatment, ATI-2341 TFA group and estrogen group exhibited increased proliferation rate (P <0.05), and higher rate appeared upon ATI-2341 TFA treatment. Cells in ATI-2341 TFA100 ng/mL and estrogen group were greatly positive for keratin and negative for vimentin. Collectively, ATI-2341 TFA promotes the differentiation of BMSCs into endometrial epithelial cells, enhances repair of damaged endometrium, and alleviate IUA. These findings might underlie a foundation for BMSC-based treatment for endometrial disorder.
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Materials Express
Materials Express NANOSCIENCE & NANOTECHNOLOGY-MATERIALS SCIENCE, MULTIDISCIPLINARY
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