丙氨酰-谷氨酰胺通过 DPP4-SIRT1 通路抑制哮喘小鼠气道上皮细胞的上皮-间质转化

IF 2.5 4区医学 Q3 ALLERGY

International Archives of Allergy and Immunology Pub Date : 2024-11-07 DOI:10.1159/000541681

Kai Ding, Xiaowen He, Donglu Liang, Lanling Xu, Bo Xiao, Lixia Hou, Feiqian Xue, Guiming Zhou, Libing Ma

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引用次数: 0

摘要

简介丙氨酰-谷氨酰胺（Ala-Gln）是一种在各种组织损伤中具有保护作用的化合物。然而，它在哮喘相关肺损伤中的作用仍未得到充分探索。本研究探讨了 Ala-Gln 在小鼠模型中调节 sDPP4 诱导的气道上皮-间质转化和卵清蛋白（OVA）诱导的哮喘的机制：方法：使用 OVA 在雌性 C57BL/6 J 小鼠中建立哮喘模型。方法：使用 OVA 在雌性 C57BL/6 J 小鼠中建立哮喘模型，并分别从小鼠脾脏和支气管中分离出 CD4+ T 细胞和支气管上皮细胞（BECs）。干预措施包括重组 sCD26/sDPP4 蛋白、Ala-Gln 和 EX527（一种 SIRT1 抑制剂）。流式细胞术用于评估 Th17 和 Treg 细胞群。用 Ala-Gln、EX527 和布地奈德（BUD）治疗小鼠。使用苏木精-伊红和马森染色法评估肺组织的组织病理学变化。白细胞计数用血液分析仪测量。分析了 DPP4、IL-17、SIRT1、SMAD2/3、N-adherin、E-cadherin、MMP9 和 α-SMA 蛋白的表达水平：结果：用重组 sCD26/sDPP4 处理 BECs 会导致 E-cadherin 表达减少，α-SMA、MMP9 和 N-cadherin 水平升高，而 Ala-Gln 可减轻这些影响。Ala-Gln 还能防止 BECs 中 SIRT1 表达的减少以及重组 sCD26/sDPP4 诱导的 Th17 细胞分化的增加。与 Ala-Gln 同时服用 EX527 可逆转这些变化，并通过 SIRT1 信号增强 SMAD2/3 的磷酸化。单用 BUD 可减轻支气管组织的炎症和纤维化，降低支气管周围淋巴结中 Th17/Treg 的比例。结论：Ala-Gln能抑制支气管细胞癌细胞的生长：结论：Ala-Gln可通过SIRT1途径抑制重组sCD26/sDPP4介导的BEC纤维化和Th17细胞分化。结论：Ala-Gln 可通过 SIRT1 通路抑制重组 CD26/sDPP4 介导的 BEC 纤维化和 Th17 细胞分化。Ala-Gln 与 BUD 联用可增强对 OVA 诱导的小鼠哮喘的疗效，从而改善 DPP4 水平升高的哮喘患者的治疗效果。

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Alanyl-Glutamine Inhibits the Epithelial-Mesenchymal Transition of Airway Epithelial Cells in Asthmatic Mice via DPP4-SIRT1 Pathway.

Introduction: Alanyl-glutamine (Ala-Gln) is a compound known for its protective effects in various tissue injuries. However, its role in asthma-related lung injuries remains underexplored. This study investigates the mechanisms by which Ala-Gln modulates sDPP4-induced airway epithelial-mesenchymal transition and ovalbumin (OVA)-induced asthma in a mouse model.

Methods: An asthma model was established in female C57BL/6 J mice by using OVA. CD4+ T cells and bronchial epithelial cells (BECs) were isolated from the spleen and bronchi of the mice, respectively. Interventions included recombinant sCD26/sDPP4 protein, Ala-Gln, and EX527 (a SIRT1 inhibitor). Flow cytometry was used to assess Th17 and Treg cell populations. Mice were treated with Ala-Gln, EX527, and budesonide (BUD). Histopathological changes in lung tissues were evaluated using hematoxylin-eosin and Masson staining. White blood cell counts were measured with a hematology analyzer. The expression levels of DPP4, IL-17, SIRT1, SMAD2/3, N-cadherin, E-cadherin, MMP9, and α-SMA proteins were analyzed.

Results: Treatment with recombinant sCD26/sDPP4 resulted in decreased E-cadherin expression in BECs and increased levels of α-SMA, MMP9, and N-cadherin, effects that were mitigated by Ala-Gln. Ala-Gln also prevented the reduction in SIRT1 expression in BECs and the increase in Th17 cell differentiation induced by recombinant sCD26/sDPP4. EX527 administration alongside Ala-Gln reversed these changes and enhanced the phosphorylation of SMAD2/3 through SIRT1 signaling. BUD alone reduced inflammation and fibrosis in bronchial tissue and lowered the Th17/Treg ratio in peribronchial lymph nodes. The therapeutic effect of BUD was further improved with concurrent Ala-Gln treatment.

Conclusion: Ala-Gln can inhibit BEC fibrosis and Th17 cell differentiation mediated by recombinant sCD26/sDPP4 through the SIRT1 pathway. Combined with BUD, Ala-Gln enhanced therapeutic efficacy in OVA-induced asthma in mice, which could offer improved outcomes for asthmatic patients with elevated DPP4 levels.

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来源期刊

International Archives of Allergy and Immunology 医学-过敏

CiteScore

5.60

自引率

3.60%

发文量

105

审稿时长

2 months

期刊介绍： ''International Archives of Allergy and Immunology'' provides a forum for basic and clinical research in modern molecular and cellular allergology and immunology. Appearing monthly, the journal publishes original work in the fields of allergy, immunopathology, immunogenetics, immunopharmacology, immunoendocrinology, tumor immunology, mucosal immunity, transplantation and immunology of infectious and connective tissue diseases.