IL-28A/IL-10Rβ axis promotes angiogenesis via eNOS/AKT signaling and AP-1/NF-κB/MMP-2 network by regulating HSP70-1 expression.

Journal of advanced research Pub Date : 2024-08-09 DOI:10.1016/j.jare.2024.08.013

Jun-Hui Song, Byungdoo Hwang, Sung Lyea Park, Hoon Kim, Soontag Jung, Changsun Choi, Hwan Myung Lee, Seok-Joong Yun, Yung Hyun Choi, Eun-Jong Cha, Cam Patterson, Wun-Jae Kim, Sung-Kwon Moon

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引用次数: 0

Abstract

Introduction: Angiogenesis plays a significant role in the development of tumor progression and inflammatory diseases. The role of IL-28A in angiogenesis and its precise regulatory mechanisms remain rarely elucidated.

Objectives: We report the novel regulatory role of IL-28A in physiological angiogenesis. The study aimed to elucidate the regulatory mechanisms involved in IL-28A-mediated angiogenesis and identify key genes associated with IL-28A-induced angiogenic responses.

Methods: To know the effect of IL-28A on angiogenesis, HUVECs were applied to perform proliferation, migration, invasion, tube formation, immunoblot, and EMSA. Gene expression changes in HUVECs following IL-28A treatment were analyzed by NGS. The functional role of HSP70-1 and IL-10Rβ in IL-28A-induced angiogenic responses was evaluated using PCR and siRNA knockdown. Animal studies were conducted by aortic ring ex vivo assays, Matrigel plug in vivo assays, and immunochemistry using HSP70-1 knockout and transgenic mice models. The efficacy of IL-28A in angiogenesis was confirmed in a hind-limb ischemia model.

Results: Autocrine/paracrine actions in HUVECs regulated IL-28A protein expression. Exogenous IL-28A increased the proliferation of HUVECs via eNOS/AKT and ERK1/2 signaling. IL-28A treatment promoted migration, invasion, and capillary tube formation of HUVECs through induction of the AP-1/NF-κB/MMP-2 network, which was associated with eNOS/AKT and ERK1/2 signaling. The efficacy of IL-28A-induced angiogenic potential was confirmed by aortic ring and Matrigel plug assay. HSP70-1 was identified as an IL-28A-mediated angiogenic effector gene using bioinformatics. Knockdown of HSP70-1 abolished angiogenic responses and eNOS/AKT signaling in IL-28A-treated HUVECs. IL-28A-induced microvessel sprouting formation was testified in HSP70-1-deficient and HSP70-1 transgenic mice. Flow recovery in hind-limb ischemia mice was accelerated by IL-28A injection. Finally, ablation of the IL-10Rβ gene impeded the angiogenic responses and eNOS/AKT signaling stimulated by IL-28A in HUVECs.

Conclusion: HSP70-1 drives the progression of angiogenesis by the IL-28A/IL-10Rβ axis via eNOS/AKT signaling and the AP-1/NF-κB/MMP-2 network.

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IL-28A/IL-10Rβ 轴通过调节 HSP70-1 的表达，通过 eNOS/AKT 信号和 AP-1/NF-κB/MMP-2 网络促进血管生成。

导言：血管生成在肿瘤进展和炎症性疾病的发展中起着重要作用。IL-28A在血管生成中的作用及其精确调控机制仍很少被阐明：我们报告了IL-28A在生理性血管生成中的新型调控作用。研究旨在阐明IL-28A介导的血管生成的调控机制，并确定与IL-28A诱导的血管生成反应相关的关键基因：为了了解IL-28A对血管生成的影响，应用HUVECs进行增殖、迁移、侵袭、管形成、免疫印迹和EMSA。通过 NGS 分析了 IL-28A 处理后 HUVECs 的基因表达变化。利用 PCR 和 siRNA 敲除技术评估了 HSP70-1 和 IL-10Rβ 在 IL-28A 诱导的血管生成反应中的功能作用。通过主动脉环体外试验、Matrigel塞体内试验以及使用HSP70-1基因敲除和转基因小鼠模型的免疫化学方法进行了动物实验。在后肢缺血模型中证实了IL-28A对血管生成的功效：结果：HUVECs的自分泌/旁分泌作用调节了IL-28A蛋白的表达。外源性 IL-28A 通过 eNOS/AKT 和 ERK1/2 信号传导增加了 HUVECs 的增殖。IL-28A通过诱导AP-1/NF-κB/MMP-2网络促进了HUVECs的迁移、侵袭和毛细血管管的形成，这与eNOS/AKT和ERK1/2信号有关。主动脉环和 Matrigel 栓实验证实了 IL-28A 诱导血管生成潜能的功效。利用生物信息学方法确定了HSP70-1是IL-28A介导的血管生成效应基因。敲除HSP70-1可消除IL-28A处理的HUVECs的血管生成反应和eNOS/AKT信号传导。在HSP70-1缺陷小鼠和HSP70-1转基因小鼠中，IL-28A诱导的微血管发芽形成得到了验证。注射 IL-28A 加快了后肢缺血小鼠的血流恢复。最后，IL-10Rβ基因的消减阻碍了IL-28A刺激HUVECs的血管生成反应和eNOS/AKT信号转导：结论：HSP70-1通过eNOS/AKT信号和AP-1/NF-κB/MMP-2网络驱动IL-28A/IL-10Rβ轴促进血管生成。

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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Journal of advanced research

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