Department of Immunology, School of Laboratory Medicine, Bengbu Medical College, Bengbu, China.
Anhui Provincial Key Laboratory of Infection and Immunity, Bengbu Medical College, Bengbu, China.
Front Immunol. 2020 Jul 21;11:1585. doi: 10.3389/fimmu.2020.01585. eCollection 2020.
To maintain alveolar gas exchange, the alveolar surface has to limit unnecessary inflammatory responses. This involves crosstalk between alveolar epithelial cells (AECs) and alveolar macrophages (AMs) in response to damaging factors. We recently showed that insulin-like growth factor (IGF)-1 regulates the phagocytosis of AECs. AMs secrete IGF-1 into the bronchoalveolar lavage fluid (BALF) in response to inflammatory stimuli. However, whether AECs regulate the production of IGF-1 by AMs in response to inflammatory signals remains unclear, as well as the role of IGF-1 in controlling the alveolar balance in the crosstalk between AMs and AECs under inflammatory conditions. In this study, we demonstrated that IGF-1 was upregulated in BALF and lung tissues of acute lung injury (ALI) mice, and that the increased IGF-1 was mainly derived from AMs. experiments showed that the production and secretion of IGF-1 by AMs as well as the expression of TGF-β were increased in LPS-stimulated AEC-conditioned medium (AEC-CM). Pharmacological blocking of TGF-β in AECs and addition of TGF-β neutralizing antibody to AEC-CM suggested that this AEC-derived cytokine mediates the increased production and secretion of IGF-1 from AMs. Blocking TGF-β synthesis or treatment with TGF-β neutralizing antibody attenuated the increase of IGF-1 in BALF in ALI mice. TGF-β induced the production of IGF-1 by AMs through the PI3K/Akt signaling pathway. IGF-1 prevented LPS-induced p38 MAPK activation and the expression of the inflammatory factors MCP-1, TNF-α, and IL-1β in AECs. However, IGF-1 upregulated PPARγ to increase the phagocytosis of apoptotic cells by AECs. Intratracheal instillation of IGF-1 decreased the number of polymorphonuclear neutrophils in BALF of ALI model mice, reduced alveolar congestion and edema, and suppressed inflammatory cell infiltration in lung tissues. These results elucidated a mechanism by which AECs used TGF-β to regulate IGF-1 production from AMs to attenuate endogenous inflammatory signals during alveolar inflammation.
为了维持肺泡气体交换,肺泡表面必须限制不必要的炎症反应。这涉及到肺泡上皮细胞 (AECs) 和肺泡巨噬细胞 (AMs) 之间的相互作用,以应对损伤因子。我们最近表明,胰岛素样生长因子 (IGF)-1 调节 AEC 的吞噬作用。AMs 在受到炎症刺激时将 IGF-1 分泌到支气管肺泡灌洗液 (BALF) 中。然而,AEC 是否在炎症信号下通过 TGF-β 调节 AM 产生 IGF-1 以及 IGF-1 在控制炎症条件下 AM 和 AEC 之间相互作用中的肺泡平衡中的作用仍不清楚。在这项研究中,我们证明了 IGF-1 在急性肺损伤 (ALI) 小鼠的 BALF 和肺组织中上调,并且增加的 IGF-1 主要来自 AM。实验表明,LPS 刺激的 AEC 条件培养基 (AEC-CM) 中 AM 的 IGF-1 产生和分泌以及 TGF-β 的表达增加。在 AEC 中阻断 TGF-β 和向 AEC-CM 中添加 TGF-β 中和抗体表明,这种 AEC 衍生的细胞因子介导 AM 中 IGF-1 的产生和分泌增加。阻断 TGF-β 合成或用 TGF-β 中和抗体治疗可减轻 ALI 小鼠 BALF 中 IGF-1 的增加。TGF-β 通过 PI3K/Akt 信号通路诱导 AM 产生 IGF-1。IGF-1 可防止 LPS 诱导的 p38 MAPK 激活和 AEC 中炎症因子 MCP-1、TNF-α 和 IL-1β 的表达。然而,IGF-1 上调 PPARγ 以增加 AEC 对凋亡细胞的吞噬作用。气管内滴注 IGF-1 可减少 ALI 模型小鼠 BALF 中的多形核白细胞数量,减轻肺泡充血和水肿,并抑制肺组织中的炎症细胞浸润。这些结果阐明了一种机制,即 AEC 通过 TGF-β 调节 AM 产生 IGF-1,以减轻肺泡炎症过程中的内源性炎症信号。
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